ABCA1 p.Arg219Lys

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PMID: 22982414 [PubMed] Jiang M et al: "Meta-analysis on association between the ATP-binding cassette transporter A1 gene (ABCA1) and Alzheimer's disease."
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9 34 Conclusions: In summary, there was no significant association detected between ABCA1 R219K, I883M and 35 R1587K polymorphisms and risk for AD.
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28 In consideration of the extensive role of ABCA1 in the develop- 77 ment of AD, we carried out a comprehensive meta-analysis on all eligible 78 case-control studies to estimate the overall AD risk of ABCA1 R219K 79 (rs2230806), I883M (rs4149313) and R1587K (rs2230808) polymor- 80 phisms as well as to quantify the between-study heterogeneity and po- 81 tential bias.
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63 For the R219K 155 polymorphism, 12 studies were available, including a total of 5372 156 cases and 5180 controls. For the I883M polymorphism, 5 studies in- 157 volved a total of 2118 cases and 1852 controls. For the R1587K poly- 158 morphism, 6 studies involved a total of 2942 cases and 2720 controls.
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68 Association of R219K variant with AD 165 For AD risk and the R219K polymorphism of ABCA1, our meta- 166 analysis gave an overall OR of 1.03 (95% CI: 0.93-1.14; p=0.56) without 167 statistically significant between-study heterogeneity (Fig. 2).
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78 t1:3 Study Year Ethnicity Genotyping method No. of case/control Diagnostic criterion Outcome Mean age of onset Mean age of case/control Gender of case/control (% male) Polymorphism t1:4 Wollmer 2003 Swedish Pyrosequencing 169/166 NINCDS-ADRDA LOAD; EOAD 70.1 73.5/69.0 42.0/51.0 R219K t1:5 Li 2004 American RT-PCR 418/376 NINCDS-ADRDA LOAD 75.5 77.5/NA 43.0/44.0 R219K, I883M, R1587K t1:6 Katzov 2004 Swedish; English DASH 974/751 NINCDS-ADRDA LOAD; EOAD 70.8 76.6/75.4 40.2/44.1 R219K, I883M, R1587K t1:7 Shibata 2006 North American SNAPshot 218/195 NINCDS-ADRDA LOAD 75.0 NA/73.1 47.0/48.0 R219K, I883M, R1587K t1:8 Kölsch 2006 German RFLP 241/294 DSM IV LOAD; EOAD NA 73.2/71.8 28.5/45.6 R219K t1:9 Wahrle 2007 American MassArray 1225/1431 AD patients LOAD NA NA/NA NA/NA R219K t1:10 Chu 2007 Chinese MassArray 272/278 NINCDS-ADRDA LOAD NA 78.0/72.0 51.0/70.1 R219K, I883M, R1587K t1:11 Wang 2007 Chinese RFLP 168/215 NINCDS-ADRDA LOAD; EOAD 69.3 73.5/72.3 46.0/41.4 R219K t1:12 Sundar 2007 American Pyrosequencing 992/699 NINCDS-ADRDA LOAD 72.3 NA/75.3 34.0/38.0 R219K t1:13 Rodríguez-Rodríguez 2007 Spainish TaqMan 371/436 NINCDS-ADRDA LOAD 72.3 75.8/80.8 34.0/31.0 R219K, I883M, R1587K t1:14 Li 2008 Canadian Affymetrix genechip 691/682 DSM IV LOAD 80.2 NA/NA 100/100 R1587K t1:15 Khorshid 2010 Iranian RFLP 154/162 DSM IV LOAD NA 78.5/77.1 40.9/38.9 R219K t1:16 Sun 2012 Chinese RFLP 321/349 DSM IV LOAD; EOAD NA 70.0/68.5 38.0/35.8 R219K t1:17 NA: Not available, DASH: Dynamic Allele Specific Hybridization, LOAD: Late-onset Alzheimer disease, EOAD: Early-onset Alzheimer disease, DSM-IV: Diagnostic and Statistical Manual of t1:18 Mental Disorders IV.
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79 Fig. 2. Forest plot from the meta-analysis of Alzheimer's disease risk and ABCA1 R219K polymorphism (K versus R).
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80 3 182 The data on genotypes of the R219K polymorphism among cases 183 and controls stratified by APOE ε4-allele status were available in 5 184 (including 2131 cases and 2343 controls) studies.
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81 Using the dominant 185 genetic model, the APOE ε4-allele carrier with the risk allele of R219K 186 variant had no significantly increased AD risk compared to APOE 187 ε4-allele non-carrier with an OR of 1.04 [95% CI: 0.83-1.31; P(Z)= 188 0.73; P(Q)=0.26].
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83 Association of I883M variant with AD 190 Overall, the per-allele OR of the 883M variant for AD was 1.10 191 (95% CI: 0.96-1.26; p=0.16; Fig. 3), with corresponding results for 192 heterozygous and homozygous of 1.12 (95% CI: 0.94-1.33; p=0.22) 193 and 1.21 (95% CI: 0.80-1.82; p=0.89), respectively. In the stratified 194 analysis by ethnicity and sample size, no significant associations be- 195 tween the I883M polymorphism and AD risk were detected in all ge- 196 netic models (Table 3).
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86 Table 2 t2:1 t2:2 Main results of pooled ORs with CI for association of the R219K polymorphism and Alzheimer's disease risk in the meta-analysis.
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92 The statistical results still did not show publi- 210 cation bias in these studies for R219K (Begg test, P=0.67; Egger test, 211 P=0.83; Supplementary Fig. 4), I883M (Begg test, P=0.42; Egger 212 test, P=0.62; Supplementary Fig. 5) and R1587K (Begg test, P= 213 0.13; Egger test, P=0.49; Supplementary Fig. 6).
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114 This may indicate that the R219K genotype has 254 a minor effect on AD than that of the APOE ε4ε4 genotype.
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127 282 To conclude, this meta-analysis suggests that the R219K, I883M 283 and R1587K polymorphisms of ABCA1 are not associated with AD 284 susceptibility.
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30 In consideration of the extensive role of ABCA1 in the development of AD, we carried out a comprehensive meta-analysis on all eligible case-control studies to estimate the overall AD risk of ABCA1 R219K (rs2230806), I883M (rs4149313) and R1587K (rs2230808) polymorphisms as well as to quantify the between-study heterogeneity and potential bias.
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65 For the R219K polymorphism, 12 studies were available, including a total of 5372 cases and 5180 controls. For the I883M polymorphism, 5 studies involved a total of 2118 cases and 1852 controls. For the R1587K polymorphism, 6 studies involved a total of 2942 cases and 2720 controls.
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70 Association of R219K variant with AD For AD risk and the R219K polymorphism of ABCA1, our meta-analysis gave an overall OR of 1.03 (95% CI: 0.93-1.14; p=0.56) without statistically significant between-study heterogeneity (Fig. 2).
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82 The data on genotypes of the R219K polymorphism among cases and controls stratified by APOE b5;4-allele status were available in 5 (including 2131 cases and 2343 controls) studies.
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88 Table 2 Main results of pooled ORs with CI for association of the R219K polymorphism and Alzheimer's disease risk in the meta-analysis. Sub-group analysis No. of data sets No. of case/control K allele Heterozygous Homozygous OR (95% CI) P (Z) P (Q) I2 (%) OR (95% CI) P (Z) P (Q) I2 (%) OR (95% CI) P (Z) P (Q) I2 (%) Total 15 5372/5180 1.03 (0.93-1.14) 0.56 0.01 23 1.07 (0.98-1.17) 0.12 0.43 10 0.95 (0.77-1.17) 0.62 0.06 21 Ethnicity Caucasian 11 4897/4669 1.04 (0.96-1.14) 0.32 0.18 14 1.09 (1.00-1.19) 0.06 0.64 0 1.02 (0.83-1.25) 0.87 0.18 19 Asian 4 475/511 0.91 (0.72-1.16) 0.76 0.05 21 0.91 (0.61-1.36) 0.66 0.15 8 0.71 (0.38-1.30) 0.26 0.09 26 Onset type EOAD 2 244/293 1.06 (0.82-1.36) 0.68 0.55 5 1.16 (0.81-1.67) 0.42 0.93 0 1.02 (0.56-1.85) 0.95 0.53 0 LOAD 10 3340/2785 1.06 (0.96-1.17) 0.27 0.19 16 1.14 (1.00-1.31) 0.06 0.51 12 0.99 (0.78-1.27) 0.94 0.15 17 Mixed 4 1788/2102 0.92 (0.76-1.10) 0.35 0.06 33 0.92 (0.74-1.14) 0.44 0.17 19 0.85 (0.57-1.27) 0.43 0.07 22 APOE status b5;4 carriers 5 1099/552 1.09 (0.93-1.28) 0.30 0.59 0 1.37 (0.96-1.96) 0.08 0.90 0 0.96 (0.66-1.40) 0.84 0.66 0 b5;4 non-carriers 5 1032/1791 0.97 (0.79-1.20) 0.80 0.07 24 1.07 (0.77-1.50) 0.67 0.04 57 0.88 (0.61-1.27) 0.49 0.13 18 Sample size b300 8 1334/1608 0.98 (0.85-1.14) 0.82 0.10 13 1.00 (0.85-1.18) 0.97 0.37 2 0.93 (0.67-1.29) 0.66 0.16 6 ࣙ300 7 4038/3572 1.03 (0.91-1.17) 0.61 0.05 42 1.10 (1.00-1.22) 0.06 0.45 0 0.96 (0.71-1.30) 0.80 0.05 39 Fig. 3. Forest plot from the meta-analysis of Alzheimer's disease risk and ABCA1 I883M polymorphism (M versus I).
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113 This may indicate that the R219K genotype has a minor effect on AD than that of the APOE b5;4b5;4 genotype.
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126 To conclude, this meta-analysis suggests that the R219K, I883M and R1587K polymorphisms of ABCA1 are not associated with AD susceptibility.
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PMID: 22668585 [PubMed] Kolovou V et al: "Association of gender, ABCA1 gene polymorphisms and lipid profile in Greek young nurses."
No. Sentence Comment
2 We analyzed SNPs in chromosome 9 such as rs2230806 (R219K) in the position 107620867, rs2230808 (R1587K) in the position 106602625 and rs4149313 (I883M) in the position 106626574 according to gender and lipid profile of Greek nurses.
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6 However, only R219K genotype distribution bared borderline statistical significance (p = 0.08) between the two studied groups.
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7 Moreover, allele frequencies of R219K, R1587K and I88M polymorphisms did not differ according to gender.
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19 Several ABCA1 gene polymorphisms were identified such as rs2230806 (R219K) in the chromosomal position 107620867, rs2230808 (R1587K) in the chromosomal position 106602625 and rs4149313 (I883M) in the chromosomal position 106626574].
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34 DNA analysis and determination of blood lipids The ABCA1 gene polymorphisms (R219K, R1587K and I883M) were detected using polymerase chain reaction (PCR) and restricted fragment length polymorphism analysis (RFLP`s).
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36 The oligonucleotide primers used for R219K and R1587K polymorphisms were described by Saleheen D et al. [7] and Tupitsina TV et al. [8] respectively. The oligonucleotide primers used for I883M polymorphism were 5`-GAGAAGAGCCACCCTGGTT- CCAACCAGAAGAGGAT-3` and 5`- AGAAAGGCAG- GAGACATCGCTT -3 as described by Clee SM et al. [9].
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42 The Kruskal - Wallis H statistic was employed in order to detect differences in lipid levels according to three different polymorphisms of ABCA1 gene (R219K, R1587K and I883M).
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54 However, only R219K distribution bared borderline significance between the two groups studied (Table 2).
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55 A post hoc power calculation was conducted employing the calculated differences in the distribution of R219K polymorphism between men and women.
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58 Moreover, allele frequencies of R219K, R1587K and I88M polymorphisms did not differ according to gender (Table 2).
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65 R219K polymorphism One of the first study which evaluated the R219K polymorphism and lipid profile in man was published by Clee SM et al. [9].
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70 Since then, many other studies correlated the R219K variant with the lipid profile and risk for CAD in various populations and ethnicities [6,9-16].
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76 Table 2 Distribution of R219K, R1587K and I883M polymorphisms and allele frequencies according to sex Men(n = 87) Women(n = 360) P R219K RR 39 (17.3%) 186 (82.7%) 0.08* RK 45 (23.8%) 144 (76.2%) KK 3(9.4%) 29 (90.6%) R1587K RR 37 (17.5%) 174 (82.5%) 0.12* RK 45 (23.5%) 146 (76.5%) KK 5 (11.4%) 39 (88.6%) I883M II 64 (20.7%) 245 (79.3%) 0.66* IM 22 (17.2%) 106 (82.8%) MM 1 (12.5%) 7 (87.5 %) Allele frequencies for R219K polymorphism R allele frequency 0.71 0.72 0.85** K allele frequency 0.29 0.28 Allele frequencies for R1587K polymorphism R allele frequency 0.68 0.69 0.85** K allele frequency 0.32 0.31 Allele frequencies for I883M polymorphism I allele frequency 0.86 0.83 0.4** M allele frequency 0.17 0.14 Fisher`s exact test - **Test for equality of proportions.
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82 In our study, we do not find any association of the R219K variant with any parameter of the lipid profile.
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84 Noteworthy to mention is that the R219K distribution bared borderline statistical significance (p = 0.08) between two studied groups.
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92 In this study we found according to gender that blood lipid levels did not Table 3 Blood lipid levels according to ABCA1 polymorphisms in all subjects ALL SUBJECTS (n = 447) Genotype Median IQR P† R219K Total cholesterol (mg/dl) RR 199 [160 - 239] 0.74 RK 194 [158 - 241] KK 205 [160-244] Triglycerides (mg/dl) RR 98 [65 - 162] 0.66 RK 98 [63 - 170] KK 95 [69 - 140] HDL cholesterol (mg/dl) RR 66 [51 - 80] 0.94 RK 64 [52.5 - 84] KK 63 [50.5 - 85] LDL cholesterol (mg/dl) RR 106 [78 - 131] 0.18 RK 104 [71.5 - 131] KK 118 [92-147] Apo A1 (mg/dl) RR 139 [108 - 180] 0.09 RK 152 [106-187] KK 164 [115-202] R1587K Total cholesterol (mg/dl) RR 190 [145 - 238] 0.08 RK 203 [170 - 241] KK 199 [158 - 222] Triglycerides (mg/dl) RR 95 [60 - 167] 0.35 RK 103 [68 - 168] KK 85 [69-150] HDL cholesterol (mg/dl) RR 65 [51 - 81] 0.73 RK 65 [53 - 83] KK 62 [47 - 85] LDL cholesterol (mg/dl) RR 100 [66 - 122] 0.0025 RK 114 [84 -139] KK 88 [87 - 89] Apo A1 (mg/dl) RR 145 [104 - 185] 0.78 RK 148 [109 - 180] KK 147 [107 - 194] I883M Total cholesterol (mg/dl) II 198 [155 - 240] 0.74 IM 198 [164 - 238] MM 197 [175 - 253] Triglycerides (mg/dl) II 99 [65 - 163] 0.49 IM 91 [62 - 171] MM 170 [78 - 233] HDL cholesterol (mg/dl) II 65 [51 - 82] 0.83 IM 64 [52 - 82] MM 68 [55 - 95] LDL cholesterol (mg/dl) II 105 [74 - 130] 0.52 IM 108 [81 - 133] MM 117 [64 - 132] Table 3 Blood lipid levels according to ABCA1 polymorphisms in all subjects (Continued) Apo A1 (mg/dl) II 143 [104 - 182] 0.62 IM 148 [109 - 184] MM 153 [111 - 200] HDL: high density lipoprotein, LDL: low density lipoprotein, Apo A1: apolipoprotein A1.
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104 Hodoğlugil et al. [20] correlated the I883M variant with higher HDL-C concentration in both sexes.
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108 Although, this variant was common in Thai Table 4 Blood lipid levels according to ABCA1 polymorphisms in men MEN (n = 87) Genotype Median IQR P† R219K Total cholesterol (mg/dl) RR 199 [149 - 250] 0.86 RK 205 [164 - 258] KK 222 [122 - 240] Triglycerides (mg/dl) RR 125 [100 - 177] 0.58 RK 142 [97 - 196] KK 134 [50 - 163] HDL cholesterol (mg/dl) RR 61 [49 - 74] 0.28 RK 57 [46 - 81] KK 46 [45 - 48] LDL cholesterol (mg/dl) RR 109 [66 - 146] 0.84 RK 106 [76 - 150] KK 149 [67 - 159] Apo A1 (mg/dl) RR 112 [100 - 135] 0.58 RK 117 [95 - 168] KK 116 [81 - 180] R1587K Total cholesterol (mg/dl) RR 192 [146 - 273] 0.28 RK 206 [166 - 241] KK 122 [110 - 205] Triglycerides (mg/dl) RR 131 [79 - 199] 0.92 RK 131 [100 - 176] KK 153 [108 - 170] HDL cholesterol (mg/dl) RR 60 [51 - 74] 0.41 RK 58 [48 - 76] KK 45 [42 - 48] LDL cholesterol (mg/dl) RR 99 [70 - 150] 0.16 RK 119 [81 - 149] KK 67 [58-106] Apo A1 (mg/dl) RR 114 [94 - 156] 0.79 RK 116 [100 - 149] KK 100 [96 - 116] I883M Total cholesterol (mg/dl) II 201 [148 - 255] 0.27 IM 214 [180 - 241] MM 120 - Triglycerides (mg/dl) II 126 [84-177] 0.18 IM 169 [118 - 250] MM 152 - HDL cholesterol (mg/dl) II 59 [47 - 75] 0.44 IM 57 [48 - 78] MM 41 - LDL cholesterol (mg/dl) II 111 [70-148] 0.39 IM 105 [80 - 149] MM 49 - Table 4 Blood lipid levels according to ABCA1 polymorphisms in men (Continued) Apo A1 (mg/dl) II 110 [94 - 148] 0.14 IM 148 [107 - 169] MM 112 - HDL: high density lipoprotein, LDL: low density lipoprotein, Apo A1: apolipoprotein A1.
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114 However, there are some data from Delgado-Lista et al. [24] suggesting that the major allele homozygotes for ABCA1 gene polymorphisms i27943 (rs2575875) and R219K (rs2230806) have a lower postprandial response as compared to minor allele carriers.
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124 Authors` contributions VK participated in the development of hypothesis, drafting of the manuscript and carried out the genetic analysis, AM participated in the molecular Table 5 Blood lipid levels according to ABCA1 polymorphisms in women WOMEN (n = 360) Genotype Median IQR P† R219K Total cholesterol (mg/dl) RR 200 [160 - 238] 0.64 RK 193 [155 - 238] KK 204 [163 - 249] Triglycerides (mg/dl) RR 89 [57 - 152] 0.88 RK 87 [61 - 159] KK 94 [70 - 134] HDL cholesterol (mg/dl) RR 66 [52 - 82] 0.84 RK 65 [55 - 85] KK 66 [55 - 85] LDL cholesterol (mg/dl) RR 105 [79 - 127] 0.18 RK 104 [70 - 126] KK 117 [93 - 141] Apo A1 (mg/dl) RR 145 [111 - 187] 0.16 RK 155 [110 - 194] KK 164 [122 - 204] R1587K Total cholesterol (mg/dl) RR 189 [145 - 231] 0.09 RK 203 [172 - 240] KK 203 [163 - 224] Triglycerides (mg/dl) RR 87 [57 - 146] 0.61 RK 96 [61 - 160] KK 81 [69 - 136] HDL cholesterol (mg/dl) RR 66 [51 - 82] 0.82 RK 67 [55 - 84] KK 64 [52 - 86] LDL cholesterol (mg/dl) RR 100 [66 - 121] 0.0053 RK 112 [85 - 132] KK 106 [83 - 133] Apo A1 (mg/dl) RR 152 [109 - 189] 0.59 RK 155 [114 - 188] KK 153 [116 - 194] I883M Total cholesterol (mg/dl) II 198 [156 - 237] 0.54 IM 196 [160 - 238] MM 214 [181 - 273] Triglycerides (mg/dl) II 90 [61-155] 0.45 IM 86 [58 - 148] MM 188 [73 - 274] HDL cholesterol (mg/dl) II 66 [52-82.5] 0.61 IM 66 [53 - 83] MM 73 [60 - 111] LDL cholesterol (mg/dl) II 104 [74 - 125] 0.34 IM 109 [83 - 132] MM 124 [66 - 134] Table 5 Blood lipid levels according to ABCA1 polymorphisms in women (Continued) Apo A1 (mg/dl) II 154 [111-189] 0.86 IM 149 [110 - 188] MM 166 [110 - 226] HDL: high density lipoprotein, LDL: low density lipoprotein, Apo A1: apolipoprotein A1.
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157 Srinivasan SR, Li S, Chen W, Boerwinkle E, Berenson GS: R219K polymorphism of the ABCA1 gene and its modulation of the variations in serum high-density lipoprotein cholesterol and triglycerides related to age and adiposity in white versus black young adults.
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164 Zhao SP, Xiao ZJ, Li QZ, Nie S, Tan LM, Jiang B, Wu J: Relationship between ATP-binding cassette transporter 1 R219K genetic variation and blood lipids.
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170 Kitjaroentham A, Hananantachai H, Tungtrongchitr A, Pooudong S, Tungtrongchitr R: R219K polymorphism of ATP binding cassette transporter A1 related with low HDL in overweight/obese Thai males.
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18 ABCA1 protein is expressed in liver, macrophages, intestines, lungs etc. Several ABCA1 gene polymorphisms were identified such as rs2230806 (R219K) in the chromosomal position 107620867, rs2230808 (R1587K) in the chromosomal position 106602625 and rs4149313 (I883M) in the chromosomal position 106626574].
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31 DNA analysis and determination of blood lipids The ABCA1 gene polymorphisms (R219K, R1587K and I883M) were detected using polymerase chain reaction (PCR) and restricted fragment length polymorphism analysis (RFLP`s).
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33 The oligonucleotide primers used for R219K and R1587K polymorphisms were described by Saleheen D et al. [7] and Tupitsina TV et al. [8] respectively. The oligonucleotide primers used for I883M polymorphism were 5`-GAGAAGAGCCACCCTGGTTCCAACCAGAAGAGGAT-3` and 5`- AGAAAGGCAG- GAGACATCGCTT -3 as described by Clee SM et al. [9].
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39 The Kruskal - Wallis H statistic was employed in order to detect differences in lipid levels according to three different polymorphisms of ABCA1 gene (R219K, R1587K and I883M).
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51 However, only R219K distribution bared borderline significance between the two groups studied (Table 2).
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52 A post hoc power calculation was conducted employing the calculated differences in the distribution of R219K polymorphism between men and women.
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62 R219K polymorphism One of the first study which evaluated the R219K polymorphism and lipid profile in man was published by Clee SM et al. [9].
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67 Since then, many other studies correlated the R219K variant with the lipid profile and risk for CAD in various populations and ethnicities [6,9-16].
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73 Table 2 Distribution of R219K, R1587K and I883M polymorphisms and allele frequencies according to sex Men(n = 87) Women(n = 360) P R219K RR 39 (17.3%) 186 (82.7%) 0.08* RK 45 (23.8%) 144 (76.2%) KK 3(9.4%) 29 (90.6%) R1587K RR 37 (17.5%) 174 (82.5%) 0.12* RK 45 (23.5%) 146 (76.5%) KK 5 (11.4%) 39 (88.6%) I883M II 64 (20.7%) 245 (79.3%) 0.66* IM 22 (17.2%) 106 (82.8%) MM 1 (12.5%) 7 (87.5 %) Allele frequencies for R219K polymorphism R allele frequency 0.71 0.72 0.85** K allele frequency 0.29 0.28 Allele frequencies for R1587K polymorphism R allele frequency 0.68 0.69 0.85** K allele frequency 0.32 0.31 Allele frequencies for I883M polymorphism I allele frequency 0.86 0.83 0.4** M allele frequency 0.17 0.14 Fisher`s exact test - **Test for equality of proportions.
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79 In our study, we do not find any association of the R219K variant with any parameter of the lipid profile.
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81 Noteworthy to mention is that the R219K distribution bared borderline statistical significance (p = 0.08) between two studied groups.
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89 In this study we found according to gender that blood lipid levels did not Table 3 Blood lipid levels according to ABCA1 polymorphisms in all subjects ALL SUBJECTS (n = 447) Genotype Median IQR Pߤ R219K Total cholesterol (mg/dl) RR 199 [160 - 239] 0.74 RK 194 [158 - 241] KK 205 [160-244] Triglycerides (mg/dl) RR 98 [65 - 162] 0.66 RK 98 [63 - 170] KK 95 [69 - 140] HDL cholesterol (mg/dl) RR 66 [51 - 80] 0.94 RK 64 [52.5 - 84] KK 63 [50.5 - 85] LDL cholesterol (mg/dl) RR 106 [78 - 131] 0.18 RK 104 [71.5 - 131] KK 118 [92-147] Apo A1 (mg/dl) RR 139 [108 - 180] 0.09 RK 152 [106-187] KK 164 [115-202] R1587K Total cholesterol (mg/dl) RR 190 [145 - 238] 0.08 RK 203 [170 - 241] KK 199 [158 - 222] Triglycerides (mg/dl) RR 95 [60 - 167] 0.35 RK 103 [68 - 168] KK 85 [69-150] HDL cholesterol (mg/dl) RR 65 [51 - 81] 0.73 RK 65 [53 - 83] KK 62 [47 - 85] LDL cholesterol (mg/dl) RR 100 [66 - 122] 0.0025 RK 114 [84 -139] KK 88 [87 - 89] Apo A1 (mg/dl) RR 145 [104 - 185] 0.78 RK 148 [109 - 180] KK 147 [107 - 194] I883M Total cholesterol (mg/dl) II 198 [155 - 240] 0.74 IM 198 [164 - 238] MM 197 [175 - 253] Triglycerides (mg/dl) II 99 [65 - 163] 0.49 IM 91 [62 - 171] MM 170 [78 - 233] HDL cholesterol (mg/dl) II 65 [51 - 82] 0.83 IM 64 [52 - 82] MM 68 [55 - 95] LDL cholesterol (mg/dl) II 105 [74 - 130] 0.52 IM 108 [81 - 133] MM 117 [64 - 132] Table 3 Blood lipid levels according to ABCA1 polymorphisms in all subjects (Continued) Apo A1 (mg/dl) II 143 [104 - 182] 0.62 IM 148 [109 - 184] MM 153 [111 - 200] HDL: high density lipoprotein, LDL: low density lipoprotein, Apo A1: apolipoprotein A1.
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109 However, there are some data from Delgado-Lista et al. [24] suggesting that the major allele homozygotes for ABCA1 gene polymorphisms i27943 (rs2575875) and R219K (rs2230806) have a lower postprandial response as compared to minor allele carriers.
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119 Authors` contributions VK participated in the development of hypothesis, drafting of the manuscript and carried out the genetic analysis, AM participated in the molecular Table 5 Blood lipid levels according to ABCA1 polymorphisms in women WOMEN (n = 360) Genotype Median IQR Pߤ R219K Total cholesterol (mg/dl) RR 200 [160 - 238] 0.64 RK 193 [155 - 238] KK 204 [163 - 249] Triglycerides (mg/dl) RR 89 [57 - 152] 0.88 RK 87 [61 - 159] KK 94 [70 - 134] HDL cholesterol (mg/dl) RR 66 [52 - 82] 0.84 RK 65 [55 - 85] KK 66 [55 - 85] LDL cholesterol (mg/dl) RR 105 [79 - 127] 0.18 RK 104 [70 - 126] KK 117 [93 - 141] Apo A1 (mg/dl) RR 145 [111 - 187] 0.16 RK 155 [110 - 194] KK 164 [122 - 204] R1587K Total cholesterol (mg/dl) RR 189 [145 - 231] 0.09 RK 203 [172 - 240] KK 203 [163 - 224] Triglycerides (mg/dl) RR 87 [57 - 146] 0.61 RK 96 [61 - 160] KK 81 [69 - 136] HDL cholesterol (mg/dl) RR 66 [51 - 82] 0.82 RK 67 [55 - 84] KK 64 [52 - 86] LDL cholesterol (mg/dl) RR 100 [66 - 121] 0.0053 RK 112 [85 - 132] KK 106 [83 - 133] Apo A1 (mg/dl) RR 152 [109 - 189] 0.59 RK 155 [114 - 188] KK 153 [116 - 194] I883M Total cholesterol (mg/dl) II 198 [156 - 237] 0.54 IM 196 [160 - 238] MM 214 [181 - 273] Triglycerides (mg/dl) II 90 [61-155] 0.45 IM 86 [58 - 148] MM 188 [73 - 274] HDL cholesterol (mg/dl) II 66 [52-82.5] 0.61 IM 66 [53 - 83] MM 73 [60 - 111] LDL cholesterol (mg/dl) II 104 [74 - 125] 0.34 IM 109 [83 - 132] MM 124 [66 - 134] Table 5 Blood lipid levels according to ABCA1 polymorphisms in women (Continued) Apo A1 (mg/dl) II 154 [111-189] 0.86 IM 149 [110 - 188] MM 166 [110 - 226] HDL: high density lipoprotein, LDL: low density lipoprotein, Apo A1: apolipoprotein A1.
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151 Srinivasan SR, Li S, Chen W, Boerwinkle E, Berenson GS: R219K polymorphism of the ABCA1 gene and its modulation of the variations in serum high-density lipoprotein cholesterol and triglycerides related to age and adiposity in white versus black young adults.
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158 Zhao SP, Xiao ZJ, Li QZ, Nie S, Tan LM, Jiang B, Wu J: Relationship between ATP-binding cassette transporter 1 R219K genetic variation and blood lipids.
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PMID: 22377775 [PubMed] Sun YM et al: "The polymorphism of the ATP-binding cassette transporter 1 gene modulates Alzheimer disease risk in Chinese Han ethnic population."
No. Sentence Comment
3 Methods: We studied the role of R219K and V825I polymorphisms of ABCA1 in modulating the risk of AD in 321 AD patients and 349 comparisons of Chinese Han.
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4 Genotyping of R219K and V825I were performed by PCR-restriction fragment length polymorphism analysis.
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5 Results: The genotype distribution of R219K was different with more RK in total AD group (χ2 = 8.705, df = 2, p = 0.013), late-onset AD (LOAD) group (χ2 = 10.636, df = 2, p = 0.005), APOE non-ε4ε4 group (χ2 = 9.900, df = 2, p = 0.007), and female AD group (χ2 = 8.369, df = 2, p = 0.015).
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9 In R219K, age at onset (AAO) was significantly lower by 4.9 years on average in patients of KK genotype than those of RK in APOE ε4 carrying group and higher by 5.5 years in patients of KK genotype than those of RR in APOE ε4 noncarrying group.
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16 C 2012 American Association for Geriatric Psychiatry DOI: 10.1097/JGP.0b013e3182423b6a of R219K may relate to the development of AD in the east of China.
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22 But clinical investigation of its relationship to AD has commenced in these years and the results were controversial.19 Also, the investigation in Chinese ethnic Han people is rare.20 Here, we examined two single nucleotide polymorphisms (SNPs) in the coding regions of ABCA1: R219K (rs2230806) located in exon 7 with a G to A nucleotide change, which is most popular SNP in both CAD and AD examinations; V825I (rs2066715) located in exon 17 with a G to A as well, which associated with HDL-C and played an important role in CAD but was rarely reported in AD patients.21,22 We conducted a case-control study to investigate the genetic association of these two SNPs with AD in a population of Chinese Han in eastern China.
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36 Genotyping of R219K, V825I, and APOE Genomic DNA was extracted from the sodium citrate treated blood samples of both AD patients and comparisons by TIANamp blood DNA Kit (TIAN- GEN).
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37 The genotypes of R219K and V825I were the same as the previous report.23 The APOE genotypes were determined as described by Donohoe et al.24 Statistical Analysis Statistical analyses were performed using SPSS version 12.0 (SPSS Inc., Chicago, IL).
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48 Genotype and Allele Frequency Distribution R219K and V825I were under Hardy-Weinberg equilibrium in both AD and comparison groups (p > 0.20) (see Table, Supplemental Digital Content 1, http://links.lww.com/AJGP/A26, which demonstrates Hardy-Weinberg equilibrium of the two SNPs inAD patientsandcomparisongroup).
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50 The distribution of genotype in R219K was different in AD patients and comparisons (χ2 = 8.705, df = 2, p = 0.013).
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52 There was difference in genotype of R219K inLOAD group(χ2 = 10.636, df = 2, p= 0.005) but no difference in EOAD group (χ2 = 0.598, df = 2, p = 0.741).
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60 As shown in Table 3, logistic regression was used to further analyze the R219K genotype in total population, LOAD-comparison group, and APOE ε4ε4 noncarrying group.
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64 Influence of ABCA1 Polymorphisms on AAO and MMSE Score of AD As shown in Table 4, using ANOVA, we analyzed the effects of R219K and V825I genotypes on the AAO and MMSE scores of AD patients which were divided according to the onset age, gender, and APOE ε4 and ε4ε4 carrying status.
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65 When further using the post-hoc LSD multiple comparisons, in the R219K, we found that AAO was significantly lower by 4.9 years in patients of KK genotype than those of RK in APOE ε4 carrying group and higher by 5.5 years on average in patients of KK genotype than those of RR in APOE ε4 noncarrying group.
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68 R219K locates in the major extracellular loop in N-terminus of the ABCA1 protein, important for the cholesterol efflux.
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77 The R219K has been one of the most studied SNPs in both CAD and AD in recent years.
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78 In CAD, the 219K was depicted to associate with either increased HDL-C or reduced severity of atherosclerosis.30 However, the role of R219K polymorphism in AD remains controversial.
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80 Rodr´ıguez-Rodr´ıguez et al.31 found that RK + KK in R219K was significantly associated with AD and conferred a risk of 1.78 (p = 0.007) in 372 Spanish AD patients and 440 controls, the same as our results, and they also demonstrated the RK + KK genotypes increased risk in both EOAD and LOAD.
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82 Genotypes and Allele Frequencies of R219K and V825I Polymorphisms in ABCA1 Gene in AD Patients and Comparison Group Comparison Comparison R219K AD (%) Group (%) V825I AD (%) Group (%) Total, n 321 349 321 349 RR 93 (29.0) 125 (35.8) VV 92 (28.7) 109 (31.2) RK 180 (56.1) 156 (44.7) VI 158 (49.2) 170 (48.7) KK 48 (15.0) 68 (19.5) II 71 (22.1) 70 (20.1) χ2 (p) 8.705 (0.013)a 0.715 (0.699) R frequency 366 (57.0) 407 (58.2) V frequency 342 (53.3) 388 (55.6) K frequency 276 (43.0) 293 (41.8) I frequency 300 (46.7) 310 (44.4) χ2 (p) 0.183 (0.669) 0.724 (0.395) EOAD, n 124 149 124 149 RR 42 (33.9) 53 (35.6) VV 31 (25.0) 50 (33.6) RK 66 (53.2) 73 (49.0) VI 62 (50.0) 66 (44.3) KK 16 (12.9) 23 (15.4) II 31 (25.0) 33 (22.1) χ2 (p) 0.598 (0.741) 2.375 (0.305) R frequency 150 (60.5) 179 (60.1) V frequency 124 (50.0) 166 (55.7) K frequency 98 (39.5) 119 (39.9) I frequency 124 (50.0) 132 (44.3) χ2 (p) 0.1 (0.921) 1.769 (0.184) LOAD, n 197 200 197 200 RR 51 (25.9) 72 (36.0) VV 61 (31.0) 59 (29.5) RK 114 (57.9) 83 (41.5) VI 96 (48.7) 104 (52.0) KK 32 (16.2) 45 (22.5) II 40 (20.3) 37 (18.5) χ2 (p) 10.636 (0.005)b 0.448 (0.799) R frequency 216 (54.8) 227 (56.8) V frequency 218 (55.3) 222 (55.5) K frequency 178 (45.2) 173 (43.2) I frequency 176 (44.7) 178 (44.5) χ2 (p) 0.229 (0.584) 0.002 (0.962) Male, n 123 125 123 125 RR 41 (33.3) 42 (33.6) VV 31 (25.2) 41 (32.8) RK 66 (53.7) 58 (46.4) VI 64 (52.0) 60 (48.0) KK 16 (13.0) 25 (20.0) II 28 (22.8) 24 (19.2) χ2 (p) 2.488 (0.288) 1.81 (0.405) R frequency 148 (60.2) 142 (56.8) V frequency 126 (51.2) 142 (56.8) K frequency 98 (39.8) 108 (43.2) I frequency 120 (48.8) 108 (43.2) χ2 (p) 0.577 (0.447) 1.555 (0.212) Female, n 198 224 198 224 RR 52 (26.3) 83 (37.1) VV 61 (30.8) 68 (30.4) RK 114 (57.6) 98 (43.8) VI 94 (47.5) 110 (49.1) KK 32 (16.2) 43 (19.2) II 43 (21.7) 46 (20.5) χ2 (p) 8.369 (0.015)a 0.134 (0.935) R frequency 218 (55.1) 264 (58.9) V frequency 216 (54.5) 246 (54.9) K frequency 178 (44.9) 184 (41.1) I frequency 180 (45.5) 202 (45.1) χ2 (p) 1.291 (0.256) 0.11 (0.915) APOE ε4 carrying, n 150 143 150 143 RR 48 (32.0) 52 (36.4) VV 37 (24.7) 44 (30.8) RK 82 (54.7) 62 (43.4) VI 78 (52.0) 74 (51.7) KK 20 (13.3) 29 (20.3) II 35 (23.3) 25 (17.5) χ2 (p) 4.426 (0.109) 2.211 (0.331) R frequency 178 (59.3) 166 (58.0) V frequency 152 (50.7) 162 (56.6) K frequency 122 (40.7) 120 (42.0) I frequency 148 (49.3) 124 (43.4) χ2 (p) 0.101 (0.751) 2.103 (0.147) APOE ε4 noncarrying, n 171 206 171 206 RR 45 (26.3) 73 (35.4) VV 55 (32.2) 65 (31.6) RK 98 (57.3) 94 (45.6) VI 80 (46.8) 96 (46.6) KK 28 (16.4) 39 (18.9) II 36 (21.1) 45 (21.8) χ2 (p) 5.33 (0.070) 0.039 (0.981) R frequency 188 (55.0) 240 (58.3) V frequency 190 (55.6) 226 (54.9) K frequency 154 (45.0) 172 (41.7) I frequency 152 (44.4) 186 (45.1) χ2 (p) 0.82 (0.365) 0.037 (0.847) APOE ε4ε4 carrying, n 35 3 35 3 RR 11 (31.4) 1 (33.3) VV 7 (20.0) 1 (33.3) RK 17 (48.6) 2 (66.7) VI 20 (57.1) 1 (33.3) KK 7 (20.0) 0 (0.0) II 8 (22.9) 1 (33.3) (Continued ) TABLE 2.
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ABCA1 p.Arg219Lys 22377775:82:36
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83 (Continued ) Comparison Comparison R219K AD (%) Group (%) V825I AD (%) Group (%) χ2 (p) 0.656 (1.000)c 1.321 (0.577)c R frequency 39 (55.7) 4 (66.7) V frequency 34 (48.6) 3 (50.0) K frequency 31 (44.3) 2 (33.3) I frequency 36 (51.4) 3 (50.0) χ2 (p) (0.692)c (1.000)c APOE ε4ε4 noncarrying, n 286 346 286 346 RR 82 (28.7) 124 (35.8) VV 85 (29.7) 108 (31.2) RK 163 (57.0) 154 (44.5) VI 138 (48.3) 169 (48.8) KK 41 (14.3) 68 (19.7) II 63 (22.0) 69 (19.9) χ2 (p) 9.9 (0.007)b 0.452 (0.798) R frequency 327 (57.2) 402 (58.1) V frequency 308 (53.8) 385 (55.6) K frequency 245 (42.8) 290 (41.9) I frequency 264 (46.2) 307 (44.4) χ2 (p) 0.11 (0.741) 0.405 (0.525) Notes: For all the χ2 of genotypes, df = 2; for all the χ2 of allele frequencies, df = 1.
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86 Logistic Regression Analysis of R219K Polymorphism of ABCA1 Gene in AD Patients and Comparison Group R219K AD Comparison Group Wald p OR (95% CI) Total, n 321 (%) 349 (%) RR 93 (29.0) 125 (35.8) Reference RK 180 (56.1) 156 (44.7) 6.102 0.014a 1.546 (1.094-2.185) KK 48 (15.0) 68 (19.5) 0.062 0.804 0.943 (0.596-1.494) RK + KK 228 (71.1) 224 (64.2) 3.430 0.064 1.363 (0.982-1.892) LOAD, n 197 (%) 200 (%) RR 51 (25.9) 72 (36.0) Reference RK 114 (57.9) 83 (41.5) 7.746 0.005b 1.921 (1.213-3.041) KK 32 (16.2) 45 (22.5) 0.021 0.884 1.044 (0.583-1.871) RK + KK 146 (74.1) 128 (64.0) 4.750 0.029a 1.619 (1.050-2.497) APOE ε4ε4 noncarrying, n 286 (%) 346 (%) RR 82 (28.7) 124 (35.8) Reference RK 163 (57.0) 154 (44.5) 6.399 0.011a 1.586 (1.109-2.266) KK 41 (14.3) 68 (19.7) 0.175 0.675 0.903 (0.559-1.458) RK + KK 204 (71.3) 222 (64.2) 3.409 0.065 1.377 (0.981-1.933) Notes: For the Wald χ2 tests, df = 1.
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ABCA1 p.Arg219Lys 22377775:86:32
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92 Effects of Two Single Nucleotide Polymorphisms (R219K and V825I) of ABCA1 Gene on AAO and MMSE Score in AD Patients R219K V825I RR (%) RK (%) KK (%) F (p) VV (%)g VI (%) II (%) F (p) Total, n 93 (29.0) 180 (56.1) 48 (15.0) 92 (28.7) 158 (49.2) 71 (22.1) AAO 65.4 ± 10.42 67.8 ± 9.46 67.3 ± 9.36 1.813 (0.165) 68.4 ± 9.34 66.8 ± 9.84 65.6 ± 10.01 1.764 (0.173) MMSE 14.1 ± 6.44 14.4 ± 6.00 14.5 ± 6.25 0.113 (0.893) 14.8 ± 5.87 14.0 ± 6.31 14.4 ± 5.87 0.545 (0.580) EOAD, n 42 (33.9) 66 (53.2) 16 (12.9) 31 (25.0) 62 (50.0) 31 (25.0) AAO 55.5 ± 5.33 57.0 ± 4.97 55.7 ± 4.92 1.222 (0.298) 57.0 ± 5.20 56.3 ± 5.04 55.7 ± 5.19 0.470 (0.626) MMSE 13.6 ± 6.84 13.0 ± 6.63 14.3 ± 8.62 0.237 (0.790) 13.9 ± 7.38 12.2 ± 6.92 15.2 ± 6.21a 2.119 (0.125) LOAD, n 51 (25.9) 114 (57.9) 32 (16.2) 61 (40.0) 96 (48.7) 40 (20.3) AAO 73.5 ± 5.23 74 ± 4.57 73.1 ± 4.1 0.523 (0.594) 74.2 ± 4.11 73.6 ± 4.99 73.2 ± 4.70 0.628 (0.535) MMSE 14.4 ± 6.14 15.2 ± 5.48 14.6 ± 4.81 0.427 (0.653) 15.3 ± 5.37 15.2 ± 5.63 13.7 ± 5.58 1.179 (0.310) Male, n 41 (33.3) 66 (53.7) 16 (13.0) 31 (25.2) 64 (52.0) 28 (22.8) AAO 65.1 ± 9.65 67.2 ± 9.38 67.9 ± 9.81 0.850 (0.430) 68.0 ± 10.50 66.8 ± 9.04 64.7 ± 9.51 0.887 (0.415) MMSE 15.2 ± 6.27 16.1 ± 6.21 15.0 ± 5.72 0.404 (0.668) 16.7 ± 5.67 14.9 ± 6.49 16.4 ± 5.77 1.110 (0.333) Female, n 52 (26.3) 114 (57.6) 32 (16.1) 61 (30.8) 94 (47.5) 43 (21.7) AAO 65.7 ± 11.80 68.1 ± 9.53 67.0 ± 9.27 1.036 (0.357) 68.7 ± 8.78 66.9 ± 10.39 66.2 ± 10.38 0.960 (0.385) MMSE 13.2 ± 6.50 13.4 ± 5.67 14.2 ± 6.57 0.301 (0.740) 13.9 ± 6.03 13.4 ± 6.15 13.1 ± 5.63 0.255 (0.775) APOE ε4 carrying, n 48 (32.0) 82 (54.7) 20 (13.3) 37 (24.7) 78 (52.0) 35 (23.3) AAO 65.7 ± 9.95 67.8 ± 8.64 62.7 ± 8.85b 2.798 (0.064) 67.9 ± 8.92 65.7 ± 9.41 66.7 ± 9.14 0.742 (0.478) MMSE 13.8 ± 6.04 14.8 ± 5.69 14.5 ± 7.13 0.369 (0.692) 15.3 ± 6.15 13.7 ± 6.32 15.2 ± 4.86 1.212 (0.301) APOE ε4 noncarrying, n 45 (26.3) 98 (57.3) 28 (16.4) 55 (32.2) 80 (46.8) 36 (21.1) AAO 65.1 ± 11.01 67.8 ± 10.14 70.6 ± 8.37c 2.627 (0.075) 68.8 ± 9.68 68.0 ± 10.16 64.5 ± 10.79d 2.160 (0.119) MMSE 14.3 ± 6.90 14.1 ± 6.27 14.5 ± 5.68 0.036 (0.964) 14.6 ± 6.13 14.3 ± 6.34 13.4 ± 6.69 0.252 (0.778) APOE ε4ε4 carrying, n 11 (31.4) 17 (48.6) 7 (20.0) 7 (20.0) 20 (57.1) 8 (22.9) AAO 64.8 ± 9.67 66.5 ± 6.79 67.6 ± 7.41 0.283 (0.756) 65.0 ± 8.37 66.0 ± 7.70 67.6 ± 8.16 0.215 (0.807) MMSE 14.9 ± 6.99 14.4 ± 4.70 13.4 ± 5.29 0.162 (0.851) 13.9 ± 4.41 14.5 ± 6.43 15.0 ± 4.03 0.077 (0.926) APOE ε4ε4 noncarrying, n 82 (28.7) 163 (57.0) 41 (14.3) 85 (29.7) 138 (48.3) 63 (22.0) AAO 65.5 ± 10.57 67.9 ± 9.70 67.2 ± 9.73 1.597 (0.204) 68.7 ± 9.41 67.0 ± 10.12 65.3 ± 10.24e 2.132 (0.121) MMSE 13.9 ± 6.40 14.4 ± 6.13 14.7 ± 6.44 0.206 (0.814) 14.9 ± 6.24 13.9 ± 6.31 14.3 ± 6.08 0.667 (0.514) Notes: MMSE score and AAO were analyzed by ANOVA and post-hoc LSD multiple comparisons and were expressed in mean ± SD.
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98 If the function of R219K in ABCA1 is also related to age in the brain, the RR genotype may be assumed to become a protective factor in elder people.
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99 We found that the impact of RK and RK + KK in R219K polymorphism on LOAD but not on EOAD, which may be explained by the assumption shown earlier.
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106 Genotypes and allele frequencies of R219K showed no discrepancies in our study when stratified by APOE-ε4 allele carrying status, the same as the results of Wollmer et al.36 Other studies showed the association between R219K genotypes and the risk of AD in APOE-ε4 noncarriers,20,35 but seldom in APOE-ε4 carriers.
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107 Wahrle et al.34 investigated R219K polymorphisms in 1225 AD cases and 1431 controls, which analyzed subgroups on the basis of APOE genotype according to the large number of sample.
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108 They failed to show an effect of R219K SNP on risk of AD in either APOE ε4ε4 group or APOE non- ε4ε4 group.34 We did not find the difference in APOE ε4ε4 group and moreover the number of APOE ε4ε4 carrying subjects in our study was far smaller than theirs.
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109 But in our APOE non-ε4ε4 carrying subjects, there were significant discrepancies in R219K genotypes with more RK genotype in AD group, which was not showed in APOE ε4ε4 carriers.
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110 This may indicate the R219K RK genotype has a minor effect on AD than that of APOE ε4ε4 genotype.
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111 Wollmer et al.36 found that R219K K allele was associated with delayed AAO by 1.7 years in their late-onset, sporadic AD patients.
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113 The results indicated that R219K might affect the AD occurrence interacting with APOE ε4 allele, which needs further investigation.
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114 In summary, our data revealed that the RK heterozygosis of R219K in ABCA1 increased the risk of AD in Chinese Han ethnic population, particularly in LOAD, APOE ε4ε4 noncarriers, and females.
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PMID: 22584245 [PubMed] Kolovou G et al: "Cholesteryl Ester Transfer Protein and ATP-Binding Cassette Transporter A1 Genotype Alter the Atorvastatin and Simvastatin Efficacy: Time for Genotype-Guided Therapy?"
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4 Patients treated with atorvastatin (n ¼ 254) or simvastatin (n ¼ 332) were genotyped for CETP (TaqIB and I405V) and ABCA1 (R219K) genetic variants.
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8 The TaqIB and R219K (opposite to I405V) gene polymorphisms seem to modify the response to lipid-lowering therapy with simvastatin or atorvastatin treatment.
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11 Several ABCA1 gene polymorphisms were identified, including rs2230806 (R219K) which codes RR, RK, and KK genotypes.
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28 DNA Analysis and Determination of Blood Lipids and Glucose The CETP (TaqIB, I405V) polymorphisms were detected using polymerase chain reaction (PCR) and restricted fragment length polymorphism (RFLP) analysis as described previously.10,11 The R219K of ABCA1 gene polymorphism was detected using PCR and RFLPs.
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30 For R219K polymorphism, AAA- GACTTCAAGGACCCAGCTT and cctcacattccgaaagcatta oligonucleotide primers were used.12 The PCR was subjected to 95 C for 5 minutes, 30 cycles of 95 C for 30 seconds, 55 C for 30 seconds, 72 C for 30 seconds, and final extension to 72 C for 7 minutes, producing a fragment of 309 bp.
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ABCA1 p.Arg219Lys 22584245:30:4
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48 In the whole cohort, the genotype frequency of ABCA1 (R219K) polymorphism was 47% for RR, 43.8% for RK, and 9.2% for KK.
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53 ABCA1 (R219K).
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59 Discussion Gene frequencies for TaqIB, I405V, and R219K polymorphisms in our cohort were similar to those reported in other cau- casians13,14 and dyslipidemic populations.15,16 In previous studies, we evaluated the efficacy of atorvasta- tin8 and simvastatin7 according to CETP polymorphisms and found that the effectiveness in lipid lowering may be influenced by CETP polymorphism.
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80 C, HDL-C concentrations before and after statin therapy according to ABCA1 R219K genotypes in patients with baseline HDL-C <40 mg/ dL.
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PMID: 21643759 [PubMed] Li Y et al: "Quantitative assessment of the effect of ABCA1 R219K polymorphism on the risk of coronary heart disease."
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0 Quantitative assessment of the effect of ABCA1 R219K polymorphism on the risk of coronary heart disease Yang Li • Kefu Tang • Kejun Zhou • Zhiyun Wei • Zhen Zeng • Lin He • Chunling Wan Received: 19 November 2010 / Accepted: 21 May 2011 / Published online: 4 June 2011 Ó Springer Science+Business Media B.V. 2011 Abstract In the past decade, a number of case-control studies have been conducted to investigate the relationship between the ATP-binding cassette transporter A1 (ABCA1) R219K polymorphism and coronary heart disease (CHD).
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ABCA1 p.Arg219Lys 21643759:0:47
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13 In conclusion, our results indicate that the ABCA1 R219K polymorphism is a protective factor of CHD in Asians, but not in Caucasians.
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27 To date, many case-control studies have been carried out to investigate the relationship between ABCA1 R219K polymorphism and the risk of developing CHD, but the results were conflicting or inconclusive.
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29 In an attempt to clarify this inconsistency, we combined data from relevant published population-based association studies to quantify the overall genetic effect of the ABCA1 R219K polymorphism on the risk of CHD.
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33 Inclusion criteria For inclusion, studies had to meet all of the following criteria: (1) be a case-control or cohort study published in a peer-reviewed journal; (2) examine the associations between CHD and ABCA1 R219K polymorphisms; (3) have determined the ABCA1 R219K polymorphisms in both cases and controls; (4) be independent from other studies; and (5) present original data on genotype distribution or obtain from the authors.
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52 Meta-analysis results The meta-analysis of the R219K polymorphism included 20 studies with 9,437 cases and 16,270 controls.
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53 Figure 1 shows the results of all studies of the R219K polymorphism and CHD.
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60 Pooled OR is indicated by black diamonds Table 1 Summary estimates for the OR of ABCA1 R219K polymorphism in subgroup analyses Study population Studies, n OR (95% CI) P(Z)a P(Q)b I2 (%) P(Q)c All 20 0.80 (0.69-0.92) 0.001 \0.001 76 All in HWE 17 0.78 (0.66-0.92) 0.003 \0.001 79 Ethnicity 0.010 Caucasian 10 0.87 (0.73-1.04) 0.12 \0.001 77 Asian 8 0.69 (0.55-0.86) 0.0009 0.05 50 Other 2 0.70 (0.29-1.70) 0.43 Outcome 0.922 Coronary stenosis 12 0.78 (0.67-0.92) 0.002 0.03 49 Myocardial infarction 2 0.81 (0.67-0.98) 0.03 0.34 0 Combined 6 0.80 (0.59-1.08) 0.15 \0.001 90 Gender 0.381 Males 3 0.94 (0.80-1.09) 0.4 0.59 0 Femals 2 0.82 (0.41-1.63) 0.57 0.07 69 Combined 17 0.78 (0.66-0.92) 0.003 \0.001 78 HWE Hardy-Weinberg Equilibrium The OR was calculated using random effect model a Z test used to determine the significance of the overall OR b Cochran`s chi-square Q statistic test used to assess the heterogeneity in subgroups c Cochran`s chi-square Q statistic test used to assess the heterogeneity between subgroups Caucasians and the pooled OR was 0.87(95% CI 0.73-1.04; P(Z) = 0.12).
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65 Discussion This study represents the first application of meta-analysis to assess the risk for CHD in relation to the ABCA1 R219K polymorphism.
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79 One explanation about how ABCA1 R219K polymorphism modifies the risk of CHD is that ABCA1 may influence the plasma lipid levels.
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82 Only the R219K was significantly associated with HDL-C concentration and CAD risk [29].
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86 It is probable that the protective function of R219K polymorphism is not only explained by increased plasma HDL-C level.
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91 Another probable mechanism is that R219K polymorphism induces the activity of ABCA1 protein, which mediates cholesterol efflux from peripheral cells back to liver independent of plasma HDL-C levels.
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101 reported that R219K variant appeared to be more protective for smokers and ex-smokers than non-smokers in the premature CHD group.
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106 Our meta-analysis supports an association of ABCA1 R219K polymorphism with CHD in Asians.
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109 In subgroup analyses, evidence was obtained to suggest different risk effects of R219K between populations of Caucasians and Asians.
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51 Meta-analysis results The meta-analysis of the R219K polymorphism included 20 studies with 9,437 cases and 16,270 controls.
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59 Pooled OR is indicated by black diamonds Table 1 Summary estimates for the OR of ABCA1 R219K polymorphism in subgroup analyses Study population Studies, n OR (95% CI) P(Z)a P(Q)b I2 (%) P(Q)c All 20 0.80 (0.69-0.92) 0.001 \0.001 76 All in HWE 17 0.78 (0.66-0.92) 0.003 \0.001 79 Ethnicity 0.010 Caucasian 10 0.87 (0.73-1.04) 0.12 \0.001 77 Asian 8 0.69 (0.55-0.86) 0.0009 0.05 50 Other 2 0.70 (0.29-1.70) 0.43 Outcome 0.922 Coronary stenosis 12 0.78 (0.67-0.92) 0.002 0.03 49 Myocardial infarction 2 0.81 (0.67-0.98) 0.03 0.34 0 Combined 6 0.80 (0.59-1.08) 0.15 \0.001 90 Gender 0.381 Males 3 0.94 (0.80-1.09) 0.4 0.59 0 Femals 2 0.82 (0.41-1.63) 0.57 0.07 69 Combined 17 0.78 (0.66-0.92) 0.003 \0.001 78 HWE Hardy-Weinberg Equilibrium The OR was calculated using random effect model a Z test used to determine the significance of the overall OR b Cochran`s chi-square Q statistic test used to assess the heterogeneity in subgroups c Cochran`s chi-square Q statistic test used to assess the heterogeneity between subgroups Caucasians and the pooled OR was 0.87(95% CI 0.73-1.04; P(Z) = 0.12).
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64 Discussion This study represents the first application of meta-analysis to assess the risk for CHD in relation to the ABCA1 R219K polymorphism.
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78 One explanation about how ABCA1 R219K polymorphism modifies the risk of CHD is that ABCA1 may influence the plasma lipid levels.
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81 Only the R219K was significantly associated with HDL-C concentration and CAD risk [29].
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85 It is probable that the protective function of R219K polymorphism is not only explained by increased plasma HDL-C level.
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90 Another probable mechanism is that R219K polymorphism induces the activity of ABCA1 protein, which mediates cholesterol efflux from peripheral cells back to liver independent of plasma HDL-C levels.
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100 reported that R219K variant appeared to be more protective for smokers and ex-smokers than non-smokers in the premature CHD group.
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105 Our meta-analysis supports an association of ABCA1 R219K polymorphism with CHD in Asians.
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108 In subgroup analyses, evidence was obtained to suggest different risk effects of R219K between populations of Caucasians and Asians.
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PMID: 22090467 [PubMed] Guevara-Cruz M et al: "A dietary pattern including nopal, chia seed, soy protein, and oat reduces serum triglycerides and glucose intolerance in patients with metabolic syndrome."
No. Sentence Comment
93 Single nucleotide polymorphisms of the ABCA1 R230C (rs9282541), ABCA1 R219K (rs2230806), TCF7L2 (rs7903146), PPARG (rs1801282), and IRS1 (rs1801278) genes were determined using PCR-based TaqMan allele discrimination assays (ABI Prism 7900 HT Sequence Detection System, Applied Biosystems) (30).
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136 The number of participants with a specific genotype distribution (wild-type allele homozygote, variant heterozygote, variant homozygote) for each polymorphism was as follows: ABCA1 R230C (56, 11, 0,); ABCA1 R219K (37, 26, 4); TCF7L2 C/T (51,13,3); PPARG P12A (58 7,2,); and IRS1 G972R (59 7,1,).
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137 Allele frequencies (wild-type, variant) were as follows: ABCA1 R230C (91.8%, 8.2%); ABCA1 R219K (74.6%, 25.4%); TCF7L2 C/T (85.8%, 14.2%); PPARG P12A (91.8%, 8.2%); and IRS1 G972R (93.3%, 6.7%).
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138 Associations between ABCA1 R230C and anthropometric and biochemical variables.
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139 The decrease in BW in the participants in the DP group with the ABCA1 R230C variant was significantly greater (25.0 6 1.9 kg) than those with ABCA1 R230R variant (21.7 6 2 kg), and the increase in the serum adiponectin concentration in participants with the ABCA1 R230C variant (1.7 6 1.6 mg/L) was significantly greater than in those with the ABCA1 R230R variant (0.2 6 1.0 mg/L) after 2 mo.
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142 The ABCA1 R230C, ABCA1 R219K, TCF7L2 C/T, PPARG P12A, and IRS1 G972R polymorphisms were not related to the other clinical or biochemical variables or the dietary treatments (data not shown).
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171 Four additional polymorphisms, ABCA1 R219K, IRS-1 (Gly972Arg), PPARG (P12A), and TCF2L7, were examined in the current study because they are associated with decreased coronary heart disease, insulin resistance, weight loss, and diabetes; however, there was no relationship between the DP group, the presence of these polymorphisms, and the clinical and biochemical variables.
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95 Single nucleotide polymorphisms of the ABCA1 R230C (rs9282541), ABCA1 R219K (rs2230806), TCF7L2 (rs7903146), PPARG (rs1801282), and IRS1 (rs1801278) genes were determined using PCR-based TaqMan allele discrimination assays (ABI Prism 7900 HT Sequence Detection System, Applied Biosystems) (30).
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144 The ABCA1 R230C, ABCA1 R219K, TCF7L2 C/T, PPARG P12A, and IRS1 G972R polymorphisms were not related to the other clinical or biochemical variables or the dietary treatments (data not shown).
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173 Four additional polymorphisms, ABCA1 R219K, IRS-1 (Gly972Arg), PPARG (P12A), and TCF2L7, were examined in the current study because they are associated with decreased coronary heart disease, insulin resistance, weight loss, and diabetes; however, there was no relationship between the DP group, the presence of these polymorphisms, and the clinical and biochemical variables.
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PMID: 21839797 [PubMed] Ota M et al: "A polymorphism of the ABCA1 gene confers susceptibility to schizophrenia and related brain changes."
No. Sentence Comment
25 Previous studies have examined the association between polymorphisms of ABCA1, particularly the non-synonymous single nucleotide polymorphisms (SNPs) of rs2230806 (R219K), rs2066718 (V771M), and rs2230808 (R1587K) and risk for Alzheimer's disease.
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65 We found only four well-validated SNPs with a heterozygosity value of N0.10 in Asian populations: rs2230806 (R219K), rs2066718 (V771M), rs2066714 (I883M), and rs2230808 (R1587K).
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123 db SNP ID and aminoacid change Position⁎ Inter-SNP distance (bp) Gender Group N Genotype distribution (frequency) χ2 P Allele count (frequency) χ2 P HWE of Controls (df=1) R/R R/K K/K R K rs2230806 107620867 (-) All Schizophrenia 497 119 (0.24) 241 (0.48) 137 (0.28) 2.77 0.250 479 (0.48) 515 (0.52) 0.01 0.897 χ²=3.73 Arg219Lys exon 7 Controls 932 204 (0.22) 495 (0.53) 233 (0.25) 903 (0.48) 961 (0.52) P=0.053 M Schizophrenia 274 63 (0.23) 137 (0.50) 74 (0.27) 0.47 0.789 263 (0.48) 285 (0.52) 0.45 0.503 χ²=0.05 Controls 330 71 (0.22) 162 (0.49) 97 (0.29) 304 (0.46) 356 (0.54) P=0.827 F Schizophrenia 223 56 (0.25) 104 (0.47) 63 (0.28) 216 (0.48) 230 (0.52) χ²=6.81 Controls 602 133 (0.22) 333 (0.55) 136 (0.23) 599 (0.50) 605 (0.50) P=0.009 V/V V/M M/M V M rs2066718 107589255 31,612 All Schizophrenia 494 438 (0.89) 54 (0.11) 2 (0.00) 1.09 0.580 930 (0.94) 58 (0.06) 0.99 0.319 χ²=0.04 Val771Met exon 16 Controls 936 812 (0.87) 120 (0.13) 4 (0.00) 1744 (0.93) 128 (0.07) P=0.847 M Schizophrenia 273 242 (0.89) 29 (0.11) 2 (0.01) 1.70 0.428 513 (0.94) 33 (0.06) 0.50 0.480 χ²=0.30 Controls 333 287 (0.86) 45 (0.14) 1 (0.00) 619 (0.93) 47 (0.07) P=0.582 F Schizophrenia 221 196 (0.89) 25 (0.11) 0 (0.00) 1.32 0.518 417 (0.94) 25 (0.06) 0.60 0.437 χ²=0.03 Controls 603 525 (0.87) 75 (0.12) 3 (0.00) 1125 (0.93) 81 (0.07) P=0.856 I/I I/M M/M I M rs2066714 107586753 34,114 All Schizophrenia 487 208 (0.43) 212 (0.44) 67 (0.14) 3.86 0.145 628 (0.64) 346 (0.36) 1.75 0.186 χ²=0.91 Ile883Met exon 18 Controls 917 345 (0.38) 446 (0.49) 126 (0.14) 1136 (0.62) 698 (0.38) P=0.339 M Schizophrenia 266 115 (0.43) 116 (0.44) 35 (0.13) 3.23 0.199 346 (0.65) 186 (0.35) 0.87 0.335 χ²=2.40 Controls 330 122 (0.37) 168 (0.51) 40 (0.12) 412 (0.62) 248 (0.38) P=0.122 F Schizophrenia 221 93 (0.42) 96 (0.43) 32 (0.14) 1.23 0.542 282 (0.64) 160 (0.36) 0.62 0.430 χ²=0.002 Controls 587 223 (0.38) 278 (0.47) 86 (0.15) 724 (0.62) 450 (0.38) P=0.966 R/R R/K K/K R K rs2230808 107562804 58,063 All Schizophrenia 491 174 (0.35) 252 (0.51) 65 (0.13) 4.05 0.132 600 (0.61) 382 (0.39) 0.63 0.427 χ²=0.50 Arg1587Lys exon 35 Controls 923 367 (0.40) 422 (0.46) 134 (0.15) 1156 (0.63) 690 (0.37) P=0.478 M Schizophrenia 273 87 (0.32) 148 (0.54) 38 (0.14) 8.51 0.014 322 (0.59) 224 (0.41) 3.68 0.055 χ²=1.17 Controls 327 140 (0.43) 141 (0.43) 46 (0.14) 421 (0.64) 233 (0.36) P=0.278 F Schizophrenia 218 87 (0.40) 104 (0.48) 27 (0.12) 0.79 0.674 278 (0.64) 158 (0.36) 0.60 0.440 χ²=0.01 Controls 596 227 (0.38) 281 (0.47) 88 (0.15) 735 (0.62) 457 (0.38) P=0.945 HWE; Hardy-Weinberg equilibrium.
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ABCA1 p.Arg219Lys 21839797:123:349
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64 We found only four well-validated SNPs with a heterozygosity value of N0.10 in Asian populations: rs2230806 (R219K), rs2066718 (V771M), rs2066714 (I883M), and rs2230808 (R1587K).
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ABCA1 p.Arg219Lys 21839797:64:109
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122 db SNP ID and aminoacid change PositionÌe; Inter-SNP distance (bp) Gender Group N Genotype distribution (frequency) c7;2 P Allele count (frequency) c7;2 P HWE of Controls (df=1) R/R R/K K/K R K rs2230806 107620867 (-) All Schizophrenia 497 119 (0.24) 241 (0.48) 137 (0.28) 2.77 0.250 479 (0.48) 515 (0.52) 0.01 0.897 c7;&#b2;=3.73 Arg219Lys exon 7 Controls 932 204 (0.22) 495 (0.53) 233 (0.25) 903 (0.48) 961 (0.52) P=0.053 M Schizophrenia 274 63 (0.23) 137 (0.50) 74 (0.27) 0.47 0.789 263 (0.48) 285 (0.52) 0.45 0.503 c7;&#b2;=0.05 Controls 330 71 (0.22) 162 (0.49) 97 (0.29) 304 (0.46) 356 (0.54) P=0.827 F Schizophrenia 223 56 (0.25) 104 (0.47) 63 (0.28) 216 (0.48) 230 (0.52) c7;&#b2;=6.81 Controls 602 133 (0.22) 333 (0.55) 136 (0.23) 599 (0.50) 605 (0.50) P=0.009 V/V V/M M/M V M rs2066718 107589255 31,612 All Schizophrenia 494 438 (0.89) 54 (0.11) 2 (0.00) 1.09 0.580 930 (0.94) 58 (0.06) 0.99 0.319 c7;&#b2;=0.04 Val771Met exon 16 Controls 936 812 (0.87) 120 (0.13) 4 (0.00) 1744 (0.93) 128 (0.07) P=0.847 M Schizophrenia 273 242 (0.89) 29 (0.11) 2 (0.01) 1.70 0.428 513 (0.94) 33 (0.06) 0.50 0.480 c7;&#b2;=0.30 Controls 333 287 (0.86) 45 (0.14) 1 (0.00) 619 (0.93) 47 (0.07) P=0.582 F Schizophrenia 221 196 (0.89) 25 (0.11) 0 (0.00) 1.32 0.518 417 (0.94) 25 (0.06) 0.60 0.437 c7;&#b2;=0.03 Controls 603 525 (0.87) 75 (0.12) 3 (0.00) 1125 (0.93) 81 (0.07) P=0.856 I/I I/M M/M I M rs2066714 107586753 34,114 All Schizophrenia 487 208 (0.43) 212 (0.44) 67 (0.14) 3.86 0.145 628 (0.64) 346 (0.36) 1.75 0.186 c7;&#b2;=0.91 Ile883Met exon 18 Controls 917 345 (0.38) 446 (0.49) 126 (0.14) 1136 (0.62) 698 (0.38) P=0.339 M Schizophrenia 266 115 (0.43) 116 (0.44) 35 (0.13) 3.23 0.199 346 (0.65) 186 (0.35) 0.87 0.335 c7;&#b2;=2.40 Controls 330 122 (0.37) 168 (0.51) 40 (0.12) 412 (0.62) 248 (0.38) P=0.122 F Schizophrenia 221 93 (0.42) 96 (0.43) 32 (0.14) 1.23 0.542 282 (0.64) 160 (0.36) 0.62 0.430 c7;&#b2;=0.002 Controls 587 223 (0.38) 278 (0.47) 86 (0.15) 724 (0.62) 450 (0.38) P=0.966 R/R R/K K/K R K rs2230808 107562804 58,063 All Schizophrenia 491 174 (0.35) 252 (0.51) 65 (0.13) 4.05 0.132 600 (0.61) 382 (0.39) 0.63 0.427 c7;&#b2;=0.50 Arg1587Lys exon 35 Controls 923 367 (0.40) 422 (0.46) 134 (0.15) 1156 (0.63) 690 (0.37) P=0.478 M Schizophrenia 273 87 (0.32) 148 (0.54) 38 (0.14) 8.51 0.014 322 (0.59) 224 (0.41) 3.68 0.055 c7;&#b2;=1.17 Controls 327 140 (0.43) 141 (0.43) 46 (0.14) 421 (0.64) 233 (0.36) P=0.278 F Schizophrenia 218 87 (0.40) 104 (0.48) 27 (0.12) 0.79 0.674 278 (0.64) 158 (0.36) 0.60 0.440 c7;&#b2;=0.01 Controls 596 227 (0.38) 281 (0.47) 88 (0.15) 735 (0.62) 457 (0.38) P=0.945 HWE; Hardy-Weinberg equilibrium.
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ABCA1 p.Arg219Lys 21839797:122:344
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PMID: 21300560 [PubMed] Jiang Z et al: "Genetic variation of the ATP-binding cassette transporter A1 and susceptibility to coronary heart disease."
No. Sentence Comment
4 Overall, significantly decreased CHD risk was associated with 219 K allele of R219K polymorphism when all studies were pooled into the meta-analysis.
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ABCA1 p.Arg219Lys 21300560:4:78
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8 In conclusion, this meta-analysis suggests that K allele of ABCA1 R219K polymorphism is a protective factor associated with decreased CHD susceptibility, but these associations vary in different ethnic populations.
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ABCA1 p.Arg219Lys 21300560:8:66
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33 Among them, two common polymorphisms in the coding region, which lead to a arginine→lysine substitution at exon 7 (R219K, rs2230806) and isoleucine→methionine substitution in exon 18 (I883M, rs4149313) were studied widely for their association with CHD susceptibility [8,9].
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ABCA1 p.Arg219Lys 21300560:33:121
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35 In consideration of the extensive role of ABCA1 in the development of CHD, we carried out a comprehensive meta-analysis on all eligible case-control studies to estimate the overall CHD risk of ABCA1 R219K and I883M polymorphisms as well as to quantify the between-study heterogeneity and potential bias.
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ABCA1 p.Arg219Lys 21300560:35:199
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38 Literature search and data extraction Genetic association studies published before the end of November 2010 on CHD and the R219K and I883M polymorphisms in the ABCA1 were sought through a search of PubMed, Web of Science, EMBASE, and CNKI (Chinese National Knowledge Infrastructure) database without language restrictions.
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ABCA1 p.Arg219Lys 21300560:38:123
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49 The strength of association between R219K and I883M polymorphisms of ABCA1 and CHD risk was assessed by OR with the corresponding 95% confidence interval (CI).
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ABCA1 p.Arg219Lys 21300560:49:36
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69 For the R219K polymorphism, 27 studies involved a total of 12,960 cases and 26,834 controls.
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ABCA1 p.Arg219Lys 21300560:69:8
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75 of cases/ controls Mean age of cases/ controls Gender component in cases/controls (% male) Diagnostic criterion Outcome Definition of control Control source Genotyping method HWE for control Qi [15] 2010 R219K Chinese 173/389 60.0/61.0 70.3/57.9 ≥50% stenosis CAD CAD- HB RFLP Y Doosti [16] 2010 R219K Iranian 207/84 49.1/55.1 83.1/59.6 NA CAD CAD- HB RFLP N Shi [17] 2009 R219K Chinese 132/157 61.7/61.1 NA/NA NA CHD CAD- HB RFLP Y Wang [18] 2009 R219K Chinese 150/139 53.5/51.1 80.0/64.7 ≥50% stenosis CHD CHD- HB RFLP N Porchay-Baldérelli [8] 2009 R219K, I883M French 482/2647 68.0/65.2 79.7/71.8 NA CHD CHD- PB allele-specific PCR Y Li [19] 2009 R219K Chinese 365/246 63.0/61.0 66.4/45.9 ≥50% stenosis CHD Healthy PB RFLP Y Zhang [20] 2008 R219K Chinese 162/186 68.3/63.5 74.7/66.1 ≥50% stenosis CHD CHD- HB RFLP Y Ni [21] 2008 R219K Chinese 260/248 63.5/62.1 64.6/66.1 ≥50% stenosis CHD CHD- HB RFLP N Liu [22] 2008 R219K Chinese 71/155 58.0/57.0 52.1/55.5 NA CHD Healthy, CHD- HB, PB RFLP Y Frikke-Schmidt [9] 2008 R219K, I883M Danish 2039/15,851 NA/NA NA IHD IHD- PB TaqMan Y Wang [23] 2008 R219K Chinese 321/294 NA/NA NA/NA ≥50% stenosis CHD CHD- HB RFLP Y Balcerzyk [24] 2007 R219K Pole 178/180 43.8/35.0 65.7/71.1 ≥50% stenosis CAD CAD- PB RFLP Y Jensen [25] 2007 I883M American 259/930 62.0/54.3 0/0 WHO CHD CHD- PB Probe Y Tsai [26] 2007 I883M Chinese 205/201 62.9/51.9 78.0/51.0 ≥50% stenosis CAD CAD- PB RFLP Y Nebel [27] 2007 I883M German 1090/728 NA/NA NA/NA ≥70% stenosis CHD Healthy PB TaqMan Y Andrikovics [28] 2006 R219K, I883M German 150/193 53.4/35.3 68.4/48.2 ≥50% stenosis CHD CHD- PB Probe Y Wang [29] 2006 R219K Chinese 234/198 64.9/62.5 61.1/59.1 ≥50% stenosis CHD CHD- HB RFLP Y Martin [30] 2006 R219K, I883M Spanish 100/100 NA/NA 100/100 NA MI CHD- HB NA Y Li [31] 2005 R219K Chinese 394/417 60.1/59.4 59.8/59.5 ≥50% stenosis CHD Healthy PB RFLP Y Woll [32] 2005 R219K American 838/257 49.5/48.3 NA/NA NA CAD Healthy PB RFLP Y Sun [33] 2005 R219K, I883M Chinese 224/248 63.7/59.6 66.9/55.2 ≥50% stenosis CHD CHD- PB RFLP Y Whiting [34] 2004 R219K American 2468/834 65.0/59.0 60.0/46.0 ≥70% stenosis CAD CAD- HB RFLP Y Wang [35] 2004 R219K Chinese 222/278 62.4/62.2 54.9/50.7 NA CHD Healthy PB RFLP Y Tregouet [36] 2004 R219K, I883M British 750/722 56.3/57.3 67.0/NA NA MI CHD- PB BigDye Y Zhao [37] 2004 R219K Chinese 236/251 NA/NA NA/NA NA CHD Healthy PB RFLP Y Bertolini [38] 2004 R219K Italian 97/97 53.9/53.8 58.8/58.8 ≥50% stenosis CAD CAD- PB RFLP Y Harada [39] 2003 R219K, I883M Janpanese 273/137 NA/NA NA/NA ≥50% stenosis CAD CAD- HB Probe Y Tan [40] 2003 I883M Chinese, Malays, Indians 616/640 58.4/45.1 100/100 ≥50% stenosis CAD Healthy PB RFLP Y Cenarro [41] 2003 R219K Spanish 216/158 53.3/67.9 66.7/41.8 NA CHD CHD- HB RFLP Y Evans [42] 2003 R219K German 114/629 55.5/43.4 71.1/53.3 NA CHD CHD- HB Probe Y Brousseau [43] 2001 R219K, I883M American 1014/1013 64.0/53.0 100/100 ≥50% stenosis CHD CHD- PB Probe Y NA: not available; MI: myocardial infarction; CAD: coronary artery disease; IHD: ischemic heart disease; RFLP: restriction fragment length polymorphisms; Y: yes; N: no; PB: population based; HB: hospital based; WHO: world health organization.
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ABCA1 p.Arg219Lys 21300560:75:204
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ABCA1 p.Arg219Lys 21300560:75:2596
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80 Association of R219K variant with CHD Significant heterogeneity was present among the 27 studies of the R219K polymorphism (Pb0.05).
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ABCA1 p.Arg219Lys 21300560:80:15
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ABCA1 p.Arg219Lys 21300560:80:104
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86 However, significantly decreased CHD risk was found in two studies [38,41] conducted in familial hypercholesterolaemia (FH) subjects [K allele: OR=0.66, 95% CI: 0.51-0.87; dominant model: OR=0.57, 95% CI: 0.41-0.80; recessive model: OR=0.72, 95% CI: Fig. 2. Forest plot (random-effects model) of CHD associated with ABCA1 R219K polymorphism using dominant genetic model.
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ABCA1 p.Arg219Lys 21300560:86:322
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91 Table 2 Results of meta-analysis for ABCA1 R219K polymorphism and CHD risk. Sub-group analysis No.
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ABCA1 p.Arg219Lys 21300560:91:43
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100 No heterogeneity was present among the 7 studies of the R219K polymorphism (PN0.05 for all comparison).
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ABCA1 p.Arg219Lys 21300560:100:56
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121 Our results demonstrated that the K allele of the R219K polymorphism of ABCA1 is a protective factor for developing CHD.
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ABCA1 p.Arg219Lys 21300560:121:50
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125 In the stratified analysis by ethnicity, significant associations were found in East Asians and other population for R219K polymorphism in all genetic models; while no associations were detected among Caucasians for the polymorphism.
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ABCA1 p.Arg219Lys 21300560:125:117
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132 When analyses were restricted to FH subjects, the K allele of R219K polymorphism has a protective effect of CHD among Caucasian population.
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ABCA1 p.Arg219Lys 21300560:132:62
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134 Our results suggest that taking other loci than LDLR such as variant R219K of ABCA1 into consideration in CHD prediction would give a more reliable result for FH patients.
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ABCA1 p.Arg219Lys 21300560:134:69
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140 However, other studies failed to find an association between the R219K polymorphism and HDL [42,43,49].
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ABCA1 p.Arg219Lys 21300560:140:65
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148 Despite these limitations, this meta-analysis suggests that ABCA1 R219K polymorphism was significantly associated with decreased risk of CHD, particularly in East Asian population.
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ABCA1 p.Arg219Lys 21300560:148:66
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PMID: 21489276 [PubMed] Kolovou V et al: "ATP-binding cassette transporter A1 gene polymorphisms and serum lipid levels in young Greek nurses."
No. Sentence Comment
1 The present study was undertaken to detect the possible association of polymorphisms in the ABCA1 gene [rs2230806 (R219K) and rs2230808 (R1587K)] and lipid profile in Greek young nurses.
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ABCA1 p.Arg219Lys 21489276:1:115
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4 Results: There was no difference in the genotypic and allelic frequencies of the R219K polymorphism according to lipid profile.
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ABCA1 p.Arg219Lys 21489276:4:81
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16 This gene encodes a protein which is expressed in many tissues such as liver, macrophages, intestines, lungs etc. Several ABCA1 gene polymorphisms were identified, including rs2230806 (R219K) and rs2230808 (R1587K), which are mainly associated with the HDL cholesterol (HDL-C) concentration.
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ABCA1 p.Arg219Lys 21489276:16:185
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17 The R219K results in a single amino acid change in codon 219 from arginine to lysine.
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ABCA1 p.Arg219Lys 21489276:17:4
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ABCA1 p.Arg219Lys 21489276:17:57
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18 The K allele of the R219K polymorphism has been related to low coronary artery disease (CAD) risk [4] and to lower triglycerides (TGs) concentration [5].
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ABCA1 p.Arg219Lys 21489276:18:20
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39 DNA analysis and determination of blood lipids The ABCA1 gene polymorphisms (R219K and R1587K) were detected using polymerase chain reaction (PCR) and restricted fragment length polymorphism analysis (RFLP`s).
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ABCA1 p.Arg219Lys 21489276:39:77
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41 For R219K polymorphism the oligonucleotide primers which were used are AAAGACTTCAAG- GACCCAGCTT and CCTCACATTCCGAAAGCATTA [9].
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ABCA1 p.Arg219Lys 21489276:41:4
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58 The frequencies of R219K genotypes were 50.97% for RR, 40.91% for RK and 8.12% for KK, whereas the frequencies of R1587K genotypes were 47.08% for RR, 41.56% for RK and 11.36% for KK.
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ABCA1 p.Arg219Lys 21489276:58:19
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60 R219K and R1587K polymorphisms The distribution of R219K and R1587K polymorphisms was investigated according to Low HDL-C (n = 46) and High HDL-C concentration (n = 104).
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ABCA1 p.Arg219Lys 21489276:60:0
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ABCA1 p.Arg219Lys 21489276:60:51
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62 Moreover, no difference in the distribution of the R219K genotypes was detected according to lipid profile (Table 2).
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ABCA1 p.Arg219Lys 21489276:62:51
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ABCA1 p.Arg219Lys 21489276:62:64
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63 Also, no differences in the distribution of K and R carriers of R219K polymorphism was detected according to lipid profile (p = 0.87).
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ABCA1 p.Arg219Lys 21489276:63:64
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67 Total cholesterol levels was higher in women with the RK compared to women with the RR genotype of the R1587K polymorphism (207.41 mg/dl vs 187.69 mg/dl, p Figure 2 R219K gene polymorphism.
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ABCA1 p.Arg219Lys 21489276:67:165
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71 Table 2 R and K allele frequencies according to R219K and R1587K polymorphisms ABCA1 R allele frequency K allele frequency p value* R219K 0.72 0.28 0.11 R1587K 0.68 0.32 Fisher`s exact test = 0.006), whereas total cholesterol levels did not differ between women with RK and KK genotypes (207.41 mg/dl vs 193.66 mg/dl, p = 0.22).
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ABCA1 p.Arg219Lys 21489276:71:48
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ABCA1 p.Arg219Lys 21489276:71:132
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77 R219K gene polymorphism The frequency of R allele of R219K polymorphism in our study was 72% similar to Pasdar et al [10] who reported 73.2% in controls (68% in patients with ischemic stroke) and Porchay et al [11] [D.E.S.I.R participants (Data from an Epidemiological Study on the Insulin Resistance)] who reported 71.7%.
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ABCA1 p.Arg219Lys 21489276:77:0
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79 Concerning lipid profile, the possibly influence of the R219K polymorphism is still evaluated.
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ABCA1 p.Arg219Lys 21489276:79:110
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80 For example, Hodoğlugil et al in Turks individuals with low HDL-C concentration found the association of R219K polymorphism with HDL-C concentration [12].
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ABCA1 p.Arg219Lys 21489276:80:80
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ABCA1 p.Arg219Lys 21489276:80:111
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81 Frikke-Schmidt et al in Danish population did not found any association between R219K polymorphism and individuals with Low or High HDL-C concentration [7].
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ABCA1 p.Arg219Lys 21489276:81:80
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85 Sandhofer et al [14] studied male population and did not find any association of R219K polymorphism and lipid profile.
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86 Also, Cenarro et al [15] evaluated the R219K polymorphism in patients with familial hypercholesterolemia with and without premature CAD and reported that K allele was more frequent in subjects without premature CAD compared to individuals with premature CAD [15].
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87 Li et al [16] investigated the relation of R219K polymorphism with the manifestation of CAD in Chinese patients and did not report any significant correlation.
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89 Similarly, Delgado-Lista J et al [17] did not find association of R219K polymorphism and lipid profile.
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91 Also, no association between R219K polymorphism and Low or High HDL-C subgroups was found although small number involved in these groups may be a limitation.
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117 Thus the influence of diet or physical activities were unlikely, which may partially explain the lack of association of R219K or R1587K polymorphisms and HDL-C concentration.
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175 Li J, Wang LF, Li ZQ, Pan W: Effect of R219K polymorphism of the ABCA1 gene on the lipid-lowering effect of pravastatin in Chinese patients with coronary heart disease.
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38 DNA analysis and determination of blood lipids The ABCA1 gene polymorphisms (R219K and R1587K) were detected using polymerase chain reaction (PCR) and restricted fragment length polymorphism analysis (RFLP`s).
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40 For R219K polymorphism the oligonucleotide primers which were used are AAAGACTTCAAGGACCCAGCTT and CCTCACATTCCGAAAGCATTA [9].
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57 The frequencies of R219K genotypes were 50.97% for RR, 40.91% for RK and 8.12% for KK, whereas the frequencies of R1587K genotypes were 47.08% for RR, 41.56% for RK and 11.36% for KK.
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59 R219K and R1587K polymorphisms The distribution of R219K and R1587K polymorphisms was investigated according to Low HDL-C (n = 46) and High HDL-C concentration (n = 104).
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61 Moreover, no difference in the distribution of the R219K genotypes was detected according to lipid profile (Table 2).
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66 Total cholesterol levels was higher in women with the RK compared to women with the RR genotype of the R1587K polymorphism (207.41 mg/dl vs 187.69 mg/dl, p Figure 2 R219K gene polymorphism.
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70 Table 2 R and K allele frequencies according to R219K and R1587K polymorphisms ABCA1 R allele frequency K allele frequency p value* R219K 0.72 0.28 0.11 R1587K 0.68 0.32 Fisher`s exact test = 0.006), whereas total cholesterol levels did not differ between women with RK and KK genotypes (207.41 mg/dl vs 193.66 mg/dl, p = 0.22).
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76 R219K gene polymorphism The frequency of R allele of R219K polymorphism in our study was 72% similar to Pasdar et al [10] who reported 73.2% in controls (68% in patients with ischemic stroke) and Porchay et al [11] [D.E.S.I.R participants (Data from an Epidemiological Study on the Insulin Resistance)] who reported 71.7%.
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78 Concerning lipid profile, the possibly influence of the R219K polymorphism is still evaluated.
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84 Sandhofer et al [14] studied male population and did not find any association of R219K polymorphism and lipid profile.
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88 Similarly, Delgado-Lista J et al [17] did not find association of R219K polymorphism and lipid profile.
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90 Also, no association between R219K polymorphism and Low or High HDL-C subgroups was found although small number involved in these groups may be a limitation.
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116 Thus the influence of diet or physical activities were unlikely, which may partially explain the lack of association of R219K or R1587K polymorphisms and HDL-C concentration.
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174 Li J, Wang LF, Li ZQ, Pan W: Effect of R219K polymorphism of the ABCA1 gene on the lipid-lowering effect of pravastatin in Chinese patients with coronary heart disease.
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PMID: 21310416 [PubMed] Ma XY et al: "Associations of the ATP-binding cassette transporter A1 R219K polymorphism with HDL-C level and coronary artery disease risk: a meta-analysis."
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0 Atherosclerosis 215 (2011) 428-434 Contents lists available at ScienceDirect Atherosclerosis journal homepage: www.elsevier.com/locate/atherosclerosis Associations of the ATP-binding cassette transporter A1 R219K polymorphism with HDL-C level and coronary artery disease risk: A meta-analysis Xiang-yu Maa,b,1 , Jian-ping Liua,1 , Zhi-yuan Songa,* a Department of Cardiology, Southwest Hospital, Third Military Medical University, Gaotanyan Street 30, Chongqing 400038, China b Department of Epidemiology, Faculty of Preventive Medicine, Third Military Medical University, Gaotanyan Street 30, Chongqing 400038, China a r t i c l e i n f o Article history: Received 2 July 2010 Received in revised form 16 December 2010 Accepted 7 January 2011 Available online 21 January 2011 Keywords: Meta-analysis Coronary artery disease ATP-binding cassette transporter A1 HDL-C a b s t r a c t Objective: Previous studies have evaluated the associations of the ATP-binding cassette transporter A1 (ABCA1) R219K polymorphism (rs2230806) with the level of high-density lipoprotein cholesterol (HDL-C) and the risk of developing coronary artery disease (CAD), but results from many small, underpowered studies are conflicting.
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2 Methods: We conducted a systematic review and meta-analysis of available studies to clarify the associations of the ABCA1 R219K polymorphism with HDL-C level and CAD risk.
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3 Results: Through retrieving PubMed, Embase, Web of Science, CBM and CNKI, we identified a total of 22 studies with 6597 cases and 15,369 controls for the association between the ABCA1 R219K polymorphism and CAD risk.
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4 The carriers of allele 219K were found to have a lower risk of CAD than the non-carriers: OR = 0.76, 95% CI = 0.68-0.85, P = 3.78E-07, Pheterogeneity = 3.59E-08; meanwhile, 18 studies from 17 papers with 12,869 subjects were included in the association between the ABCA1 R219K polymorphism and the level of HDL-C.
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9 Conclusions: The synthesis of available evidence demonstrates that the ABCA1 R219K polymorphism is associated with a higher HDL-C level in Asians and a protective role for CAD risk both in Asians and Caucasians.
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29 The results showed that only the R219K polymorphism (G1051A, rs2230806), which resulted from the substitution of a lysine for arginine at amino acid 219 of the ABCA1 protein, was associated with increased HDL-C and a reduced risk of CAD.
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31 However, there have been few studies focusing on other genetic variants in the ABCA1 gene with the exception of R219K.
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32 Considering R219K being the most focused polymorphic site and the limited number of studies about other genetic variants in the ABCA1 gene, we conducted this meta-analysis to clarify the role of the ABCA1 R219K polymorphism in the synthesis of HDL-C and CAD risk.
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40 Selection criteria We selected the studies that met the following criteria: (1) the publication examined the associations of the ABCA1 R219K polymorphism with CAD or HDL-C level; (2) all CAD cases were diagnosed as myocardial infarction (defined by World Health Organization Multinational Monitoring of Trends and Determinants in Cardiovascular Disease [MONICA] criteria [7]) or angiographic coronary stenosis (generally defined as at least 50% stenosis of one major coronary artery); (3) for CAD association, the papers must offer the total number of cases and controls, distribution of genotypes or other information that can help us infer the results; for HDL-C level association, the number of population, the mean of HDL-C level and the standard deviations (SD) by genotypes should be available; (4) when multiple publications reported on the same or overlapping data, we used the most recent or largest population as recommended by Little et al. [8]; (5) publication language was limited to English and Chinese.
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49 Summary odds ratios (ORs) with their 95% confidence intervals (CIs) for alleles and genotypes were used to assess the strength of the association between the ABCA1 R219K polymorphism and CAD risk.
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51 A pooled standardized mean difference (SMD) and its 95% CIs were used for the meta-analysis of HDL-C level and the ABCA1 R219K polymorphism.
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61 Selection and characteristics of studies Through a comprehensive retrieval and evaluation, 22 studies with 6597 cases and 15,369 controls were identified with data on the ABCA1 R219K polymorphism and CAD [5,12-32].
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65 Table 2 describes the characteristics and data of the studies which were included in the association between the ABCA1 R219K polymorphism and HDL-C level.
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70 Association between the ABCA1 R219K polymorphism and CAD risk The result of all 22 comparisons showed that the carriers of allele 219K had a lower risk of CAD than the non-carriers: OR = 0.76, 95% CI = 0.68-0.85, P = 3.78E-07, Pheterogeneity = 3.59E-08 (Fig. 1).
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71 Additive genetic model, recessive genetic model and dominant genetic model were also included in the analysis of the association between the ABCA1 R219K polymorphism and CAD risk (Supplementary Figs. 1-3) and the results were similar with allele comparison.
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73 There was significant heterogeneity among the available studies and this Table 1 Characteristics of individual studies included in the meta-analysis of CAD and the ABCA1 R219K polymorphism. First author Year Country Ethnicity Source of controls Number (case/control) MAF Cases Controls RR RK KK RR RK KK Porchay-Balderelli et al. [14] 2009 France Caucasian Population-based 482/2647 0.28 270 175 37 1326 1109 212 Frikke-Schmidt et al. [19] 2008 Denmark Caucasian Population-based 1107/7858 0.26 603 429 75 4260 3032 566 Balcerzyk et al. [20] 2008 Poland Caucasian Population-based 178/180 0.29 90 68 20 91 78 11 Nebel et al. [21] 2007 Germany Caucasian Population-based 1090/728 0.36 b Cases: 578-1602; control: 376-1080 Andrikovics et al. [24] 2006 Germany Caucasian Population-based 150/193 0.29 84 55 11 97 73 23 Martin et al. [23] 2006 Spain Caucasian Hospital-based 100/100 0.31 48 42 10 49 40 11 Bertolini et al. [29] 2004 Italy Caucasian Hospital-based 97/97 NA c Cases: 65-32; control:47-50 Cenarro et al. [32] 2003 Spain Caucasian Hospital-based 216/158 0.28 123 78 15 72 71 15 Evans and Beil [31] 2003 Germany Caucasian Hospital-based 114/629 0.26 72 35 7 337 245 47 Clee et al. [5] 2001 Canada Caucasian Hospital-based 432/358 0.25 248 170 14 176 160 22 Li et al. [15] 2009 China Asian Population-based 365/246 0.39 140 170 55 92 116 38 Li et al. [26] 2005 China Asian Population-based 396/417 0.42 158 174 64 124 198 95 Zhao and Xiao [27] 2004 China Asian Population-based 236/251 0.40 96 111 29 80 123 48 Wang and Zhang [13]a 2009 China Asian Hospital-based 150/139 0.42 61 69 20 47 53 39 Zhang et al. [16] 2008 China Asian Hospital-based 162/186 0.43 71 65 26 49 93 44 Yu and Deng [17] 2008 China Asian Hospital-based 49/72 0.34 29 18 2 24 35 13 Liu et al. [18] 2008 China Asian Hospital-based 113/155 0.32 71 39 3 57 70 28 Wang et al. [22] 2006 China Asian Hospital-based 234/198 0.36 108 105 21 67 101 30 Sun et al. [25] 2005 China Asian Hospital-based 224/248 0.42 105 85 34 62 129 57 Wang et al. [28] 2004 China Asian Hospital-based 222/278 0.47 79 94 49 76 125 77 Harada et al. [30] 2003 Japan Asian Hospital-based 273/137 0.49 73 139 61 31 73 33 Doosti et al. [12]a 2010 Iran - Hospital-based 207/94 0.47 77 71 59 38 17 39 MAF = minor allele frequency; NA = not available.
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77 Meta-analysis of CAD and the ABCA1 R219K polymorphism (allele comparison).
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78 Table 2 Characteristics of individual studies included in the meta-analysis of HDL-C level and the ABCA1 R219K polymorphism. First author Year Country Ethnicity MAF RR RK KK n Mean SD n Mean SD n Mean SD Porchay-Balderelli et al. [14] 2009 France Caucasian 0.28 1596 1.31 0.36 1284 1.32 0.35 249 1.33 0.36 Sandhofer et al. [33] 2008 Austria Caucasian 0.29 350 1.41 0.34 274 1.38 0.33 64 1.38 0.29 Boekholdt et al. [36]a 2006 Holland Caucasian 0.24 302 0.92 0.21 223 0.92 0.22 21 0.92 0.20 Hodoglugil et al. [37] 2005 Turkey Caucasian 0.39 364 1.06 0.24 480 1.06 0.22 152 1.06 0.26 Hodoglugil et al. [37] 2005 Turkey Caucasian 0.37 574 0.91 0.19 688 0.91 0.19 204 0.91 0.20 Evans and Beil [31] 2003 Germany Caucasian 0.26 279 1.32 0.03 206 1.34 0.03 30 1.27 0.31 Clee et al. [5]a 2001 Canada Caucasian 0.25 424 0.92 0.22 330 0.93 0.23 36 0.92 0.20 Wang and Zhang [13]a 2009 China Asian 0.42 108 0.96 0.26 122 1.03 0.30 59 1.07 0.25 Li et al. [15] 2009 China Asian 0.38 140 1.06 0.15 170 1.09 0.13 55 1.12 0.17 Liu et al. [18]a 2008 China Asian 0.32 29 1.22 0.18 39 1.26 0.19 3 1.48 0.11 Wu and Bai [35] 2007 China Asian 0.47 52 1.27 0.29 107 1.41 0.54 41 1.48 0.45 Wang et al. [22] 2006 China Asian 0.36 175 1.09 0.18 206 1.11 0.23 51 1.34 0.35 Li et al. [26] 2005 China Asian 0.38 158 1.12 0.33 174 1.16 0.30 64 1.15 0.38 Wang et al. [28]a 2004 China Asian 0.43 79 0.96 0.14 94 0.95 0.14 49 1.01 0.12 Zhao and Xiao [27] 2004 China Asian 0.40 176 1.32 0.33 234 1.36 0.39 77 1.44 0.32 Zhao et al. [38] 2004 China Asian 0.40 394 1.3 0.4 470 1.4 0.4 179 1.4 0.4 Harada et al. [30] 2003 Japan Asian 0.48 68 1.25 0.41 140 1.24 0.40 57 1.24 0.35 Benton et al. [34]a 2007 USA Mixed 0.39 388 1.33 0.38 409 1.29 0.35 172 1.37 0.39 MAF = minor allele frequency; NA = not available; HDL-C = HDL cholesterol; 1 mmol/l HDL-C = 38.73 mg/dl HDL-C.
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83 However, the significant association between the ABCA1 R219K polymorphism and CAD risk was unchanged.
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85 The results suggested a significant association between the ABCA1 R219K polymorphism and CAD risk, but the existence of heterogeneity was not influenced.
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87 Association between the ABCA1 R219K polymorphism and HDL-C level Fig. 2 describes the result of the meta-analysis of HDL-C level and the ABCA1 R219K polymorphism (KK vs RR) and it strongly suggested that the carriers of KK genotype had higher level of HDL-C than those of RR genotype: SMD = 0.19, 95% CI = 0.06-0.32, P = 0.005, Pheterogeneity = 3.19E-09.
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97 For the ABCA1 R219K polymorphism and CAD risk, the shape of the funnel plot (Fig. 3 and Supplementary Fig. 9) did not reveal obvious asymmetry which means no publication bias.
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98 Then, it was confirmed by Egger`s test (P value for allele contrast: 0.200; P value for dominant model: 0.494); for the ABCA1 R219K polymorphism and HDL-C level, both of the shape of the funnel plot (Fig. 4 and Supplementary Fig. 10) and Egger`s test (P value for KK vs RR: 0.646; P value for RK vs RR: 0.714) confirmed the absence of publication bias.
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101 Additionally, a total of 18 studies from 17 papers with 12,869 subjects were included in the analysis of association between the ABCA1 R219K polymorphism and HDL-C level.
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103 After the associations of the ABCA1 polymorphisms with HDL-C level and CAD were reported by Clee et al. [5] in 2001, serial of studies evaluated the association of the ABCA1 R219K polymorphism with HDL-C level and CAD risk in different races, and the results manifested inconclusive and underpowered.
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104 We calculated the MAFs of the ABCA1 R219K polymorphism in all studies and found that MAFs of Asian were higher than those of Caucasian through t test (P < 0.01).
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106 To date, several well-designed genome-wide association studies (GWAS) of coronary heart disease have been performed [39-47], but the R219K variant was not tested by these GWAS because of the limited SNP coverage rate of the existing SNP microarray platforms on the ABCA1 gene.
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109 In this meta-analysis, we found that the ABCA1 R219K polymorphism was significantly associated with a higher level of HDL-C in Asians, not in Caucasians; we also confirmed the protective role of ABCA1 R219K polymorphism for CAD risk both in Asians and Caucasians (allele contrast: OR = 0.76, 95% CI = 0.68-0.85, P = 3.78E-07, Pheterogeneity = 3.59E-08), though the association in Caucasians was less consistent than that in Asians.
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111 Meta-analysis of HDL-C level and the ABCA1 R219K polymorphism (KK vs RR).
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115 Funnel plot for allele comparison of CAD and the ABCA1 R219K polymorphism.
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121 Funnel plot of HDL-C level and the ABCA1 R219K polymorphism (KK vs RR).
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129 By excluding these outlier studies, the heterogeneity among Asian subjects and Caucasian studies was effectively removed, but the significant association between the ABCA1 R219K polymorphism and CAD risk or HDL-C level was not changed.
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132 The results suggested a significant association between the ABCA1 R219K polymorphism and CAD risk or HDL-C level.
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134 The functional analysis of the ABCA1 R219K polymorphism was done by SIFT and Polyphen, which predicted not only damaging variants, but also gain-of-function mutations.
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140 During these studies, cases were all survivors of CAD, as we could not evaluate those that did not survive; second, the sample sizes of some included studies were rather small and they did not have adequate power to detect the possible risk for the R219K polymorphism.
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143 Conclusion The synthesis of available evidence supports the fact that the ABCA1 R219K polymorphism is associated with a higher level of HDL-C in Asians and a protective role for CAD risk both in Asians and Caucasians.
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PMID: 22737475 [PubMed] Khorram Khorshid HR et al: "The Association between Sporadic Alzheimer's Disease and the Human ABCA1 and APOE Gene Polymorphisms in Iranian Population."
No. Sentence Comment
3 Methods: 154 AD cases and 162 control subjects from Iranian population were genotyped for APOE genotypes and ABCA1 polymorphism (R219K).
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8 Conclusion: Unlike other studies, R219K polymorphism was not dependent on gender and APOE-ε4 allele and there was no association between APOE and ABCA1 in AD patients compared to controls.
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PMID: 20800056 [PubMed] Berge KE et al: "Mutations in APOA-I and ABCA1 in Norwegians with low levels of HDL cholesterol."
No. Sentence Comment
59 of patients (het/hom)a Mutation Nucleotide Exon/Intron (i) PolyPhen prediction (score) SNP rs ID, ref.# ABCA1 Missense 8/3 R219K c.656, GNA 7 Benign (0.489) rs2230806 0/1 R282Q c.845, GNA 9 Benign (0.592) Novel 1/0 V399A c.1196, TNC 11 Benign (0.040) rs9282543 1/0 M636V c.1906, ANG 15 Benign (0.418) Novel 3/0 V771M c.2311, GNA 16 Benign (0.931) rs2066718 2/0 V825I c.2473, GNA 17 Benign (0.440) rs2066715 3/1 I883M c.2649, ANG 18 Benign (0.147) rs2066714 1/0 C887F c.2660, GNT 19 Benign (0.888) Novel 3/0 E1172D c.3516, GNC 24 Benign (0.546) rs33918808 1/0 G1216V c.3647, GNT 25 Prob damb (2.154) Ref. [18] 1/0 L1244Q c.3731, TNA 25 Prob dam (2.269) Novel 1/0 C1477F c.4430, TNA 31 Prob dam (3.688) Ref. [17] 14/1 R1587K c.4760, ANT 35 Benign (0.284) rs2230808 1/0 V1674I c.5020, GNA 37 Benign (0.821) Novel 1/0 R1680Q c.5039, GNA 37 Poss damc (1.926) Ref. [17] 1/0 N1800H c.5398, ANC 40 Poss dam (1.845) Ref. [19] Nonsense/splice 1/0 IVS4+1, GNA c.302+1, GNA i4 - 1/0 C1429X c.4287, CNA 31 - 1/0 IVS32+1, GNA c.4559+1, GNA i32 - APOA-I 7/0 R160L c.551, GNT 4 Prob dam (2.491) Ref. [21] 1/0 del182K del c.616-618 AAG 4 - Novel a Het: heterozygote, hom: homozygote.
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78 Variants R219K, V399A, V771M, V825I, I883M, E1172D, and R1587K have been reported as single nucleotide polymorphisms (SNPs) (Table 1).
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80 In addition, R219K, V771M, V825I, I883M, E1172D, and R1587K have been found in similar frequencies in patients with low or high HDL cholesterol levels [18], indicating that these variants do not cause low HDL cholesterol levels.
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PMID: 21130966 [PubMed] Rejeb J et al: "Associations between common polymorphisms of adenosine triphosphate-binding cassette transporter A1 and coronary artery disease in a Tunisian population."
No. Sentence Comment
68 The genotypes for each ABCA1 polymorphism (G1051A [R219K], G2706A [V771M], G2868A [V825I] and -565C/T [-477C/T]) were determined by polymerase chain reaction-restriction fragment length polymorphism analysis.
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PMID: 20797885 [PubMed] Guevara-Cruz M et al: "Increase in HDL-C concentration by a dietary portfolio with soy protein and soluble fiber is associated with the presence of the ABCA1R230C variant in hyperlipidemic Mexican subjects."
No. Sentence Comment
3 Therefore, the aim of this study was to assess the response of HDL-C concentration to a dietary portfolio in a group of Mexican hyperlipidemic subjects with ABCA1R230C (rs9282541) and R219K (rs2230806) polymorphisms.
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8 There was no association between the presence of the ABCA1 R219K variant (p=.544) and HDL concentration.
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31 The effect of ABCA1 genetic polymorphisms on HDL-C levels has been widely documented mainly in adults [9]; specifically, the K allele of the ABCA1 R219K polymorphism has been associated with increased HDL-concentrations [10-13] and a reduced incidence of coronary heart disease (CHD) events [10,11].
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36 Therefore, the aim of this study was to assess the response of HDL-cholesterol concentration to a dietary portfolio consisting of soy protein and soluble fiber in a group of Mexican hyperlipidemic subjects with or without ABCA1(R230C, rs9282541) and R219K (rs2230806) polymorphisms and to evaluate its association with the dietary portfolio in responders and non-responders.
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62 [22] These two single-nucleotide polymorphisms (SNPs) of the gene ABCA1 (R230C variant (rs9282541) and R219K (rs2230806)) were determined using polymerase chain reaction (PCR)-based TaqMan allele discrimination assays (ABI Prism 7900HT Sequence Detection System; Applied Biosystems, Foster City, CA) [26].
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70 Results Genotype distribution (wild type allele homozygote, variant heterozygote, variant homozygote) for each polymorphism was as follows: R230C (31, 12, 0) and R219K (19, 21, 3).
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71 Allele frequencies (wild-type, variant) were for R230C (75.5%, 24.4%) and R219K (68.6%, 31.4%).
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80 ABCA1 R219K was also studied due to its association with the fenofibrate response; however, there was no association between the presence of the ABCA1 R219K variant and the percentage of change in HDL concentration after the dietary treatment with soy protein and soluble fiber (p=.544) (Fig. 3).
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ABCA1 p.Arg219Lys 20797885:80:6
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PMID: 20188211 [PubMed] Koldamova R et al: "The role of ATP-binding cassette transporter A1 in Alzheimer's disease and neurodegeneration."
No. Sentence Comment
55 In almost all of the reports R219K (rs2230806), I883M (rs4149313), and R1587K (rs2230808) variants are the most extensively investigated since they give rise to amino acid changes, are common in the European population and are closely associated with the risk for CAD.
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56 The association of R219K is the most controversial.
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65 Importantly, the additional analysis of AD patients included in the study for association of those two markers with AD-related quantitative traits showed a significant effect of the R219K variant on CSF Aβ42 levels, whereby RK heterozygotes had the highest trait levels.
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PMID: 20418488 [PubMed] Acuna-Alonzo V et al: "A functional ABCA1 gene variant is associated with low HDL-cholesterol levels and shows evidence of positive selection in Native Americans."
No. Sentence Comment
28 The phylogenetic reconstruction uncovered two major lineages (haplogroups A and B) defined by the non-synonymous polymorphism R219K within the ABCA1 gene.
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49 The phylogenetic reconstruction uncovered two major lineages (haplogroups A and B) defined by the non-synonymous polymorphism R219K.
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31 The phylogenetic reconstruction uncovered two major lineages (haplogroups A and B) defined by the nonsynonymous polymorphism R219K within the ABCA1 gene.
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52 The phylogenetic reconstruction uncovered two major lineages (haplogroups A and B) defined by the non-synonymous polymorphism R219K.
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PMID: 20170916 [PubMed] Abellan R et al: "Association of selected ABC gene family single nucleotide polymorphisms with postprandial lipoproteins: results from the population-based Hortega study."
No. Sentence Comment
2 In men, subjects with the AA genotype of the ABCA1 rs2230806 (R219K) polymorphism were associated with increased plasma LDLc levels, while the ABCA1 haplotype, which included the rs2230806 A allele, was associated with higher TC and LDLc plasma concentrations.
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81 ABCA1 gene polymorphisms In the total population, the rs2230806 (R219K) polymorphism in gene ABCA1 was associated with plasma LDLc levels (p = 0.046) (Table 2).
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123 The R219K variant (rs2230806 polymorphism) has been recognized as putative antiatherogenic polymorphisms, and the K219 form (A allele) has been associated with increased HDLc levels [10,11,24].
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PMID: 20434407 [PubMed] Perez-Martinez P et al: "Update on genetics of postprandial lipemia."
No. Sentence Comment
53 In this context, we have studied the influence of 3 SNPs (i27943 [rs2575875]; i48168 [rs4149272]; R219K [rs2230806]) in the postprandial lipemia of 88 normolipidemic young men who were given a fatty meal [9].
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PMID: 20394740 [PubMed] Katerina H et al: "Interaction of common sequence variants and selected risk factors in determination of HDL cholesterol levels."
No. Sentence Comment
29 The g.1051GNA (p.R219K; rs2230806) variant of the adenosine triphosphate binding cassette transporter A-1 (ABCA1; GeneID: 19) gene, the g.102ANC (p.I27L; rs1169288) variant of the hepatocyte nuclear factor-1α (HNF-1α) (HNF1A; GeneID: 6927) gene, and the g.584CNT (p.T111I; rs2000813) variant of the endothelial lipase (EL) (LIPG; GeneID: 9388) gene.
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PMID: 20346718 [PubMed] Tsai MY et al: "Effect of fenofibrate therapy and ABCA1 polymorphisms on high-density lipoprotein subclasses in the Genetics of Lipid Lowering Drugs and Diet Network."
No. Sentence Comment
6 However, after fenofibrate treatment the KK genotype of R1587K (mean 4.40 lmol/L; p = 0.004) and the RK genotype of R219K (mean 1.60 lmol/L; p = 0.02) polymorphisms were associated with significantly increased small HDL.
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7 The R1587K KK genotype (mean 4.80 lmol/L; p = 0.0002) and the R219K KK genotype (mean 2.50 lmol/L; p = 0.02) were also associated with increased HDL particle concentrations.
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22 Molecular Genetics and Metabolism 100 (2010) 118-122 Contents lists available at ScienceDirect Molecular Genetics and Metabolism journal homepage: www.elsevier.com/locate/ymgme on HDL-C concentration; specifically, the K allele of the ABCA1 R219K polymorphism has been associated with increased HDL-C concentration [8-11] and a reduced incidence of coronary artery disease (CAD) events [8,9].
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23 In a subcohort of the Multi-Ethnic Study of Atherosclerosis (MESA) we demonstrated that the K allele of the R219K polymorphism (designated as the 1051 A allele in MESA) is associated with both a lower prevalence of coronary artery calcium even when adjusted for HDL-C [12] and increased small HDL particle concentration [13].
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47 The ABCA1 rs2297404, rs2578575, rs4149272, and rs2230806 (R219K) polymorphisms were genotyped by Applied Biosystems TaqMan SNP system.
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68 Table 3 shows that quantitative changes in HDL subclass particle concentrations from baseline to after fenofibrate treatment are significant for the ABCA1 R1587K and R219K polymorphisms.
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70 The R219K RK (p = 0.02) genotype was associated with 1.6-fold higher small HDL, compared to the RR genotype.
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71 In addition, HDL particle concentration was 2.5-fold higher in the KK genotype of the R219K polymorphism, compared to the RR genotype (p = 0.02).
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79 Table 2 Differences in HDL subclass particle concentrations between genotypes of ABCA1 polymorphisms, as compared to reference genotypes, at baseline (pre-fenofibrate treatment) in 287 GOLDN participants. Polymorphism (reference genotype) na Comparison genotype n Small HDL (lmol/L) Medium HDL (lmol/L)c Large HDL (lmol/L) HDL particles (lmol/L) HDL size (nm) Mean (lower 95% CI, upper 95% CI)b Mean (lower 95% CI, upper 95% CI) Mean (lower 95% CI, upper 95% CI) Mean (lower 95% CI, upper 95% CI) Mean (lower 95% CI, upper 95% CI) R1587K (RR) 152 RK 84 1.00 (À0.50, 2.60) À0.04 (À0.74, 0.67) À0.29 (À1.00, 0.46) 0.32 (À1.30, 2.00) 0.03 (À0.07, 0.12) KK 14 À0.53 (À3.70, 2.70) À0.72 (À2.20, 0.74 0-0.67 (À2.20, 0.89) À2.50 (À5.80, 0.89) À0.02 (À0.22, 0.18) R219K (RR) 155 RK 113 À0.10 (À1.70, 1.50) À0.04 (À0.77, 0.68) 0.00 (À0.77, 0.78) 0.50 (À1.10, 2.10) À0.01 (À0.11, 0.09) KK 19 À0.01 (À2.90, 2.80) À0.82 (À2.10, 0.48) 0.41 (À0.98, 1.80) 0.47 (À2.50, 3.40) À0.05 (À0.23, 0.13) M883I (II) 191 IM 57 À0.28 (À1.90, 1.40) À0.06 (À0.82, 0.70) À0.05 (À0.85, 0.75) À0.32 (À2.10, 1.4) À0.03 (À0.13, 0.08) MM 1 9.50 (À1.70, 21.00) À2.50 (À7.60, 2.60) À0.09 (À5.50, 5.30) 9.30 (À2.40, 21.00) 0.02 (À0.68, 0.720 rs4149272 (GG) 128 GA 128 0.15 (À7.70, 8.00) À2.10 (À5.70, 1.50) 1.60 (À2.20, 5.50) 0.58 (À7.60, 8.80) 0.01 (À0.48, 0.50) AA 31 À7.90 (À22.00, 5.90) 2.40 (À3.90, 8.70) 3.70 (À3.00, 10.00) À1.60 (À16.00, 13.00) 0.47 (À0.39, 1.30) rs2297404 (GG) 252 GC 34 1.80 (À0.49, 4.10) À0.36 (À1.40, 0.68) À0.31 (À1.40, 0.81) 1.60 (À0.70, 3.90) À0.16 (À0.31, À0.02)d CC 1 À1.50 (À12.00, 9.50) 2.10 (À2.90, 7.10) 1.40 (À4.00, 6.70) 0.77 (À11.00, 12.00) 0.06 (À0.63, 0.75) rs2575875 (GG) 126 GA 129 0.24 (À7.70, 8.20) 1.90 (À1.70, 5.60) À2.10 (À6.00, 1.80) À1.30 (À9.60, 7.00) À0.05 (À0.55, 0.44) AA 32 8.60 (À5.10, 22.00) À2.60 (À8.90, 3.60) À5.10 (À12.00, 1.60) 0.23 (À14.00, 15.00) À0.67 (À1.50, 0.19) a Total genotypes for R1587K and M883I do not add to 287 because genotypes of 37 participants could not be determined for R1587K and 38 for M883I.
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86 In accordance with this observation, our laboratory demonstrated that the KK genotype of the R219K polymorphism of ABCA1 was associated with an increase in small HDL particles [13]; the finding suggests that the KK genotype is associated with increased ABCA1 activity, resulting in increased cholesterol efflux.
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93 While we previously demonstrated that the ABCA1 1051 A allele (aka R219K K allele) was associated with increased small HDL in the MESA population [13], in the current study there was no increase in small HDL subclass when stratified by ABCA1 R219K genotype.
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94 Rather, we show that the K alleles of R219K and R1587K are associated 1.6- and 4.4-fold increases in small HDL after fenofibrate treatment.
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98 Finally, to expand on previous work that examined the ABCA1 polymorphism R219K, five additional SNPs were examined in the current study-of these, R1587K was found to have a significant effect on small HDL concentration (p = 0.004).
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PMID: 20185793 [PubMed] Delgado-Lista J et al: "ABCA1 gene variants regulate postprandial lipid metabolism in healthy men."
No. Sentence Comment
7 Methods and Results-To further characterize the effects of ABCA1 variants in human postprandial lipid metabolism, we studied the influence of 3 single nucleotide polymorphisms (i27943 [rs2575875]; i48168 [rs4149272]; R219K [rs2230806]) in the postprandial lipemia of 88 normolipidemic young men who were given a fatty meal.
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17 One of the most studied ABCA1 variants is R219K (rs2230806).
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22 E-mail jlopezmir@uco.es (c) 2010 American Heart Association, Inc. Arterioscler Thromb Vasc Biol is available at http://atvb.ahajournals.org DOI: 10.1161/ATVBAHA.109.202580 though a typically plausible underlying mechanism of this altered atherosclerosis was the change in HDL concentration, this has not been found in the majority of studies.14,15 Looking for additional physiological pathways underlying ABCA1 effects on lipid metabolism and atherosclerosis, we investigated and report here the effects of ABCA1 variants i27943, i48168, and R219K on postprandial lipid metabolism of healthy males.
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36 Biochemical Determinations Single Nucleotide Polymorphisms Selection, DNA Amplification, and Genotyping R219K GϾA is a well-characterized single nucleotide polymorphism (SNP) that has been extensively studied and is associated with cardiovascular disease; however, its influence on postprandial lipemia has not been tested.14 We have reported previously on other effects of SNP i27943GϾA and i48168GϾA.19 Computational analysis ascribed potential functional characteristics to each variant allele of these SNP.19 Additionally, for the i48168 GϾA polymorphism, analysis by MAPPER indicated a potential allele-specific binding site for the cartilage paired-class homeoprotein 1 (CART1 or ALX1) transcription factor, with a motif that appears enriched in certain genes involved in cholesterol metabolism (Parnell and Ordovas, unpublished data).
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41 Baseline Characteristics of the Study Participants CHOL, mg/dL TG, mg/dL HDL, mg/dL LDL, mg/dL apoA1, mg/dL apoB, mg/dL ABCA1 R219K (rs2230806) GG nϭ50 153.61Ϯ3.39 86.7Ϯ4.6 45.64Ϯ1.38 90.68Ϯ3.1 103.64Ϯ2.55 67.88Ϯ2.48 GA/AA nϭ34/4 150.48Ϯ3.61 72.90Ϯ5.5 47.01Ϯ1.83 88.84Ϯ3.46 109.36Ϯ3.58 67.72Ϯ2.53 P 0.537 0.056 0.545 0.695 0.184 0.965 ABCA1 i48168 (rs4149272) CC nϭ23 152.54Ϯ4.78 73.64Ϯ7.29 50.061Ϯ2.07* 88.05Ϯ4.07 116.43Ϯ4.04* 63.50Ϯ3.13 CT nϭ51 152.82Ϯ3.06 80.76Ϯ4.67 45.36Ϯ1.32 90.72Ϯ3.2 103.59Ϯ2.59 69.16Ϯ2.00 TT nϭ14 149.33Ϯ5.85 81.56Ϯ8.93 45.389Ϯ2.53 87.4Ϯ5.38 106.75Ϯ4.95 67.30Ϯ3.83 P 0.867 0.685 0.041 0.820 0.033 0.310 ABCA1 i27943 (rs2575875) GG nϭ21 152.12Ϯ5.00 75.63Ϯ7.67 49.36Ϯ2.21 85.36Ϯ5.74 115.78Ϯ4.28† 63.88Ϯ3.29 GA nϭ52 153.347Ϯ2.99 79.88Ϯ4.59 45.89Ϯ1.32 91.39Ϯ3.02 104.00Ϯ2.56 69.06Ϯ1.97 AA nϭ15 147.86Ϯ5.83 81.17Ϯ8.93 46.12Ϯ2.57 87.46Ϯ4.44 107.89Ϯ4.98 66.38Ϯ3.82 P 0.707 0.867 0.395 0.574 0.039 0.385 CHOL indicates cholesterol; LDL, low-density lipoprotein.
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70 R219K was not in linkage disequilibrium with either of the other 2 SNP (r2 Ͻ0.012; PϾ0.05).
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72 R219K A statistical study is presented for a genotype-dominant effect based on previously published data.14 In parallel, an additive model was also performed but we did not observe any differences compared with the dominant model.
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80 AUC of Lipid Fractions in the Postprandial Study ABCA1 R219K ABCA1 i48168 ABCA1 i27943 Total TG GG 79.5Ϯ5.0 CC 56.6Ϯ7.3* GG 56.8Ϯ7.8‡ GA/AA 70.9Ϯ5.9 CT 76.5Ϯ4.7 GA 76.4Ϯ4.7 TT 89.6Ϯ9.0 AA 87.1Ϯ9.1 CHOL GG 80.9Ϯ1.7 CC 79.9Ϯ2.7 GG 78.5Ϯ2.8 GA/AA 80.8Ϯ2.1 CT 81.1Ϯ1.7 GA 81.9Ϯ1.7 TT 79.9Ϯ2.7 AA 79.0Ϯ3.3 Large TRL TG GG 33.4Ϯ2.5 CC 20.9Ϯ3.5* GG 21.6Ϯ3.7‡ GA/AA 28.7Ϯ3.0 CT 31.8Ϯ2.3 GA 31.3Ϯ2.3 TT 38.2Ϯ4.4 AA 37.3Ϯ4.5 Small TRL TG GG 23.7Ϯ2.0 CC 20.3Ϯ3.1 GG 20.1Ϯ3.2 GA/AA 23.4Ϯ2.4 CT 23.9Ϯ2.0 GA 24.1Ϯ2.0 TT 24.9Ϯ3.9 AA 24.2Ϯ3.9 Large TRL CHOL GG 4.7Ϯ0.3 CC 4.7Ϯ0.4 GG 4.8Ϯ0.4 GA/AA 4.8Ϯ0.3 CT 4.7Ϯ0.2 GA 4.7Ϯ0.3 TT 4.6Ϯ0.5 AA 4.7Ϯ0.5 Small TRL CHOL GG 6.3Ϯ0.4 CC 5.5Ϯ0.7 GG 5.7Ϯ0.7 GA/AA 6.0Ϯ0.5 CT 6.1Ϯ0.5 GA 5.9Ϯ0.4 TT 6.5Ϯ0.9 AA 6.9Ϯ0.9 apoA1 GG 54.0Ϯ1.3 CC 60.1Ϯ1.9† GG 59.1Ϯ2.1§ GA/AA 56.6Ϯ1.5 CT 53.6Ϯ1.2 GA 54.2Ϯ1.2 TT 55.9Ϯ2.4 AA 55.9Ϯ2.4 apoB GG 35.1Ϯ1.1 CC 32.6Ϯ1.7 GG 31.8Ϯ1.7§ GA/AA 35.5Ϯ1.3 CT 36.2Ϯ1.1 GA 36.5Ϯ1.0 TT 34.8Ϯ2.1 AA 34.2Ϯ2.0 HDL GG 23.7Ϯ0.8 CC 26.0Ϯ1.2 GG 25.3Ϯ1.3 GA/AA 24.2Ϯ0.9 CT 23.5Ϯ0.7 GA 23.9Ϯ0.8 TT 23.8Ϯ1.4 AA 23.8Ϯ1.5 Univariate ANOVA using body mass index and age as covariates.
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109 Furthermore, in a recent report of type 2 diabetic patients, the ABCA1 SNP associated with coronary heart disease (including R219K) were not associ- Figure 1.
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121 ated with HDL, and those associated with HDL were not associated with coronary heart disease.35 The explanation for these contradictory findings has been set on the limited effects that gene variation can have on final HDL levels, gene-environment interactions, or the influence of ABCA1 gene variants on other lipid molecules and enzymes that secondarily can mildly influence HDL concentrations.17 The minor allele of R219K has been associated with limited atherosclerosis,15 reduced risk for myocardial infarction, or progression of coronary disease in various studies.16,36-42 Here, we noticed only a trend toward lower fasting TG (Pϭ0.059), according to previous studies.14 Currently, this variant is thought to affect lipids mildly, but gene-environment interactions are strong, with greater effects on lipid concentration when oxidative stress or inflammation is elevated in subjects.14,15,39,40 Such is not the case in our study.
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122 However, marginal effects not reaching significance were found in our study for practically all lipid parameters toward a protective effect for the minor allele of R219K, which could become significant when the subject is exposed to the aforementioned stressors or even simply with increasing age.
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1 Methods and Results-To further characterize the effects of ABCA1 variants in human postprandial lipid metabolism, we studied the influence of 3 single nucleotide polymorphisms (i27943 [rs2575875]; i48168 [rs4149272]; R219K [rs2230806]) in the postprandial lipemia of 88 normolipidemic young men who were given a fatty meal.
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11 One of the most studied ABCA1 variants is R219K (rs2230806).
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16 E-mail jlopezmir@uco.es (c) 2010 American Heart Association, Inc. Arterioscler Thromb Vasc Biol is available at http://atvb.ahajournals.org DOI: 10.1161/ATVBAHA.109.202580 though a typically plausible underlying mechanism of this altered atherosclerosis was the change in HDL concentration, this has not been found in the majority of studies.14,15 Looking for additional physiological pathways underlying ABCA1 effects on lipid metabolism and atherosclerosis, we investigated and report here the effects of ABCA1 variants i27943, i48168, and R219K on postprandial lipid metabolism of healthy males.
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30 Biochemical Determinations Single Nucleotide Polymorphisms Selection, DNA Amplification, and Genotyping R219K Gb0e;A is a well-characterized single nucleotide polymorphism (SNP) that has been extensively studied and is associated with cardiovascular disease; however, its influence on postprandial lipemia has not been tested.14 We have reported previously on other effects of SNP i27943Gb0e;A and i48168Gb0e;A.19 Computational analysis ascribed potential functional characteristics to each variant allele of these SNP.19 Additionally, for the i48168 Gb0e;A polymorphism, analysis by MAPPER indicated a potential allele-specific binding site for the cartilage paired-class homeoprotein 1 (CART1 or ALX1) transcription factor, with a motif that appears enriched in certain genes involved in cholesterol metabolism (Parnell and Ordovas, unpublished data).
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35 Baseline Characteristics of the Study Participants CHOL, mg/dL TG, mg/dL HDL, mg/dL LDL, mg/dL apoA1, mg/dL apoB, mg/dL ABCA1 R219K (rs2230806) GG nafd;50 153.61afe;3.39 86.7afe;4.6 45.64afe;1.38 90.68afe;3.1 103.64afe;2.55 67.88afe;2.48 GA/AA nafd;34/4 150.48afe;3.61 72.90afe;5.5 47.01afe;1.83 88.84afe;3.46 109.36afe;3.58 67.72afe;2.53 P 0.537 0.056 0.545 0.695 0.184 0.965 ABCA1 i48168 (rs4149272) CC nafd;23 152.54afe;4.78 73.64afe;7.29 50.061afe;2.07* 88.05afe;4.07 116.43afe;4.04* 63.50afe;3.13 CT nafd;51 152.82afe;3.06 80.76afe;4.67 45.36afe;1.32 90.72afe;3.2 103.59afe;2.59 69.16afe;2.00 TT nafd;14 149.33afe;5.85 81.56afe;8.93 45.389afe;2.53 87.4afe;5.38 106.75afe;4.95 67.30afe;3.83 P 0.867 0.685 0.041 0.820 0.033 0.310 ABCA1 i27943 (rs2575875) GG nafd;21 152.12afe;5.00 75.63afe;7.67 49.36afe;2.21 85.36afe;5.74 115.78afe;4.28ߤ 63.88afe;3.29 GA nafd;52 153.347afe;2.99 79.88afe;4.59 45.89afe;1.32 91.39afe;3.02 104.00afe;2.56 69.06afe;1.97 AA nafd;15 147.86afe;5.83 81.17afe;8.93 46.12afe;2.57 87.46afe;4.44 107.89afe;4.98 66.38afe;3.82 P 0.707 0.867 0.395 0.574 0.039 0.385 CHOL indicates cholesterol; LDL, low-density lipoprotein.
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63 R219K was not in linkage disequilibrium with either of the other 2 SNP (r2 b0d;0.012; Pb0e;0.05).
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65 R219K A statistical study is presented for a genotype-dominant effect based on previously published data.14 In parallel, an additive model was also performed but we did not observe any differences compared with the dominant model.
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73 AUC of Lipid Fractions in the Postprandial Study ABCA1 R219K ABCA1 i48168 ABCA1 i27943 Total TG GG 79.5afe;5.0 CC 56.6afe;7.3* GG 56.8afe;7.8ߥ GA/AA 70.9afe;5.9 CT 76.5afe;4.7 GA 76.4afe;4.7 TT 89.6afe;9.0 AA 87.1afe;9.1 CHOL GG 80.9afe;1.7 CC 79.9afe;2.7 GG 78.5afe;2.8 GA/AA 80.8afe;2.1 CT 81.1afe;1.7 GA 81.9afe;1.7 TT 79.9afe;2.7 AA 79.0afe;3.3 Large TRL TG GG 33.4afe;2.5 CC 20.9afe;3.5* GG 21.6afe;3.7ߥ GA/AA 28.7afe;3.0 CT 31.8afe;2.3 GA 31.3afe;2.3 TT 38.2afe;4.4 AA 37.3afe;4.5 Small TRL TG GG 23.7afe;2.0 CC 20.3afe;3.1 GG 20.1afe;3.2 GA/AA 23.4afe;2.4 CT 23.9afe;2.0 GA 24.1afe;2.0 TT 24.9afe;3.9 AA 24.2afe;3.9 Large TRL CHOL GG 4.7afe;0.3 CC 4.7afe;0.4 GG 4.8afe;0.4 GA/AA 4.8afe;0.3 CT 4.7afe;0.2 GA 4.7afe;0.3 TT 4.6afe;0.5 AA 4.7afe;0.5 Small TRL CHOL GG 6.3afe;0.4 CC 5.5afe;0.7 GG 5.7afe;0.7 GA/AA 6.0afe;0.5 CT 6.1afe;0.5 GA 5.9afe;0.4 TT 6.5afe;0.9 AA 6.9afe;0.9 apoA1 GG 54.0afe;1.3 CC 60.1afe;1.9ߤ GG 59.1afe;2.1&#a7; GA/AA 56.6afe;1.5 CT 53.6afe;1.2 GA 54.2afe;1.2 TT 55.9afe;2.4 AA 55.9afe;2.4 apoB GG 35.1afe;1.1 CC 32.6afe;1.7 GG 31.8afe;1.7&#a7; GA/AA 35.5afe;1.3 CT 36.2afe;1.1 GA 36.5afe;1.0 TT 34.8afe;2.1 AA 34.2afe;2.0 HDL GG 23.7afe;0.8 CC 26.0afe;1.2 GG 25.3afe;1.3 GA/AA 24.2afe;0.9 CT 23.5afe;0.7 GA 23.9afe;0.8 TT 23.8afe;1.4 AA 23.8afe;1.5 Univariate ANOVA using body mass index and age as covariates.
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102 Furthermore, in a recent report of type 2 diabetic patients, the ABCA1 SNP associated with coronary heart disease (including R219K) were not associ- Figure 1.
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113 ߥPb0d;0.05 i27943 GG vs GA. Arterioscler Thromb Vasc Biol May 2010 ated with HDL, and those associated with HDL were not associated with coronary heart disease.35 The explanation for these contradictory findings has been set on the limited effects that gene variation can have on final HDL levels, gene-environment interactions, or the influence of ABCA1 gene variants on other lipid molecules and enzymes that secondarily can mildly influence HDL concentrations.17 The minor allele of R219K has been associated with limited atherosclerosis,15 reduced risk for myocardial infarction, or progression of coronary disease in various studies.16,36-42 Here, we noticed only a trend toward lower fasting TG (Pafd;0.059), according to previous studies.14 Currently, this variant is thought to affect lipids mildly, but gene-environment interactions are strong, with greater effects on lipid concentration when oxidative stress or inflammation is elevated in subjects.14,15,39,40 Such is not the case in our study.
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114 However, marginal effects not reaching significance were found in our study for practically all lipid parameters toward a protective effect for the minor allele of R219K, which could become significant when the subject is exposed to the aforementioned stressors or even simply with increasing age.
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PMID: 18621447 [PubMed] Wang N et al: "The R219K polymorphism in the ATP-binding cassette transporter 1 gene has a protective effect on atherothrombotic cerebral infarction in Chinese Han ethnic population."
No. Sentence Comment
0 Neurobiology of Aging 31 (2010) 647-653 The R219K polymorphism in the ATP-binding cassette transporter 1 gene has a protective effect on atherothrombotic cerebral infarction in Chinese Han ethnic population Ning Wanga, Xie-Hua Xuea, Yi Lina, Ling Fanga, Shenxing Muronga, Zhi-Ying Wua,b,* a Department of Neurology and Institute of Neurology, First Affiliated Hospital, Center of Neuroscience, Fujian Medical University, 20 Chazhong Road, Fuzhou 350005, China b Department of Neurology and Institute of Neurology, Huashan Hospital, Institutes of Brain Science and State Key Laboratory of Medical Neurobiology, Shanghai Medical College, Fudan University, 12 Wulumuqi Middle Road, Shanghai 200040, China Received 30 November 2007; received in revised form 29 April 2008; accepted 28 May 2008 Available online 14 July 2008 Abstract The association of R219K and V825I polymorphisms of ABCA1 gene with cerebral infarction has been rarely reported.
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ABCA1 p.Arg219Lys 18621447:0:44
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3 Genotyping of R219K and V825I were performed by PCR-RFLP analysis.
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ABCA1 p.Arg219Lys 18621447:3:14
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5 The R219K genotype frequency distributions were significantly different between patients with atherothrombotic cerebral infarction (ACI) and control individuals, with fewer KK genotypes and more RR genotypes in ACI patients (χ2 = 9.89, P < 0.01).
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8 These results indicate that the K allele of R219K polymorphism is an independent protective factor against ACI.
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11 Keywords: Cerebral infarction; ATP-binding cassette transporter 1; R219K; V825I 1.
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19 The more common SNPs are R219K in exon 7 and V825I in exon 17.
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23 Besides, there was a report that KK individuals had a higher level of LDL-C and the K allele carriers had a lower TG (Pasdar et al., 2007) and another report that R219K did not influence the plasma lipids levels (Takagi et al., 2002).
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26 Taken together, these controversial findings indicate that the function of R219K and V825I may be significant in certain environmental factors and population backgrounds.
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ABCA1 p.Arg219Lys 18621447:26:75
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27 Although the association of R219K and/or V825I with CAD has been widely reported in different ethnic populations, the association of them with cerebral infarction has been reported rarely (Andrikovics et al., 2006; Pasdar et al., 2007).
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30 The aim of this study is to investigate the association of R219K and V825I with cerebral infarction and levels of plasma lipids in the Han ethnic group in Chinese population.
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111 R219K is located in the extracellular loop of the ABCA1 protein, and plays an important role for the interaction of ApoA1 and cholesterol efflux.
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115 R219K is the most common polymorphism of ABCA1 and the allele frequency of the K allele is 26-46% in Caucasian population (Koren-Morag et al., 2002; Pasdar et al., 2007; Singaraja et al., 2003).
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116 To date, several studies have reported controversial results about the possible role of R219K in arteriosclerosis.
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ABCA1 p.Arg219Lys 18621447:116:88
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119 They concluded that observed effects were independent of any other SNPs found in association with R219K (Clee et al., 2001).
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ABCA1 p.Arg219Lys 18621447:119:98
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123 In our present study, R219K was 47.70% in control group, similar to that of Caucasian population (Singaraja et al., 2003).
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ABCA1 p.Arg219Lys 18621447:123:22
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124 In addition, the K allele of R219K was associated with increased HDL-C and apoA1 levels in the female subgroup.
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ABCA1 p.Arg219Lys 18621447:124:29
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127 Although the association of R219K with CAD has been widely studied in different ethnic populations, the association of R219K with cerebral infarction has been reported rarely.
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ABCA1 p.Arg219Lys 18621447:127:28
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ABCA1 p.Arg219Lys 18621447:127:119
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136 This may be due to the substitution of V825I is conservative and the polymorphism may only exert minimal influence on cholesterol efflux activity (Tan et al., 2003).
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ABCA1 p.Arg219Lys 18621447:136:67
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137 There was few report associated with the synergistic effects among R219K, V825I and risk factors.
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ABCA1 p.Arg219Lys 18621447:137:67
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126 Although the association of R219K with CAD has been widely studied in different ethnic populations, the association of R219K with cerebral infarction has been reported rarely.
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ABCA1 p.Arg219Lys 18621447:126:28
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PMID: 20303467 [PubMed] Doosti M et al: "The role of ATP-binding-cassette-transporter-A1 (ABCA1) gene polymorphism on coronary artery disease risk."
No. Sentence Comment
4 We determined the presence of the R219K variant in the ABCA1 gene by polymerase chain reaction (PCR) and restriction analysis in 301 patients with and without CAD.
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29 R219K polymorphism analysis.
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40 The bands were visualized by staining with ethidium bromide.22 The R219 K polymorphism is the result of a nucleotide change G to A at position 1051 of the complementary DNA sequence, and it results in the substitution of lysine for arginine at amino acid 219 of the ABCA1 protein.
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28 R219K polymorphism analysis.
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39 The bands were visualized by staining with ethidium bromide.22 The R219 K polymorphism is the result of a nucleotide change G to A at position 1051 of the complementary DNA sequence, and it results in the substitution of lysine for arginine at amino acid 219 of the ABCA1 protein.
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PMID: 20590502 [PubMed] Stankovic S et al: "Genetic aspects of ischemic stroke: coagulation, homocysteine, and lipoprotein metabolism as potential risk factors."
No. Sentence Comment
382 (135, 434-436) Two publications assessed the distribution of different polymorphisms (L158L, R219K, G316G, R1587K) and haplotype arrangements of the ABCA I gene in IS patients.
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ABCA1 p.Arg219Lys 20590502:382:93
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383 A study of 244 Hungarian patients suggested a protective role for the ABCA I -R219K and V771M polymorphisms against IS.
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ABCA1 p.Arg219Lys 20590502:383:78
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PMID: 19596329 [PubMed] Frikke-Schmidt R et al: "Genetic variation in the ABCA1 gene, HDL cholesterol, and risk of ischemic heart disease in the general population."
No. Sentence Comment
2387 Common ABCA1 variants in the general population 5.1. Frequency of common variants in the extreme tails of the HDL distribution Several resequencing studies have identified a number of common non-synonymous variations in ABCA1 [57,58,81-84]: R219K, V771M, V825I, I883M, E1172D and R1587K.
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2395 Frequencies of common variants and association with variation in lipid levels in the general population Frequencies for the most common non-synonymous ABCA1 SNPs (R219K, V825I, I883M, R1587K) are largely similar across studies that partly or as a whole represent general populations [57,58,81,82,86-88], whereas the less common SNPs (V771M, and E1172D) are reported in some [57,58,81,82,86,88], but not in all studies [58,87].
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2386 Common ABCA1 variants in the general population 5.1. Frequency of common variants in the extreme tails of the HDL distribution Several resequencing studies have identified a number of common non-synonymous variations in ABCA1 [57,58,81-84]: R219K, V771M, V825I, I883M, E1172D and R1587K.
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2394 Frequencies of common variants and association with variation in lipid levels in the general population Frequencies for the most common non-synonymous ABCA1 SNPs (R219K, V825I, I883M, R1587K) are largely similar across studies that partly or as a whole represent general populations [57,58,81,82,86-88], whereas the less common SNPs (V771M, and E1172D) are reported in some [57,58,81,82,86,88], but not in all studies [58,87].
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PMID: 19489872 [PubMed] Lamon-Fava S et al: "Association of polymorphisms in genes involved in lipoprotein metabolism with plasma concentrations of remnant lipoproteins and HDL subpopulations before and after hormone therapy in postmenopausal women."
No. Sentence Comment
27 The genes and SNPs of interest were: oestrogen receptor a [ESR1; rs2234693 (PvuII, intron 1), rs9340799 (XbaI, intron 1), rs4870056 (IVS1-1505, intron 1), rs9340894 (intron 3), rs985192 (intron 4), rs926777 (intron 4), rs3020325 (intron 4), and rs3020368 (intron 5)], ABCA1 [(G3456C (E1112D) and rs2230806 (R219K)], CETP [rs708272 (TaqIB)], HL [LIPC; rs1800588 (C-514T)], LPL [rs1800590 (T-93G), rs1801177 (D9N), rs268 (9N291S), and rs328 (S447X)], and SR-BI [SCARB1; rs4238001 (G2S)].
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PMID: 19344898 [PubMed] Maekawa M et al: "A novel missense mutation of ABCA1 in transmembrane alpha-helix in a Japanese patient with Tangier disease."
No. Sentence Comment
112 5 SNPs, InsG319, R219K, I680I, I883 M and T1472T, in this family (Supplementary Table 1).
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ABCA1 p.Arg219Lys 19344898:112:17
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161 Among five SNPs identified in this family, previous epidemiological studies demonstrated that R219K and I883 M variants are associated with higher HDL-C levels [30,31], whereas InsG319 is negatively correlated with atherosclerosis independently of plasma HDL-C concentrations [32].
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ABCA1 p.Arg219Lys 19344898:161:94
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164 For instance, the R219K variant is significantly associated with higher HDL-C levels in normal body weight individuals, but with lower HDL-C levels in overweight people [30].
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ABCA1 p.Arg219Lys 19344898:164:18
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165 This may explain why HDL-C is low in the proband`s father despite the presence of homozygous R219K.
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ABCA1 p.Arg219Lys 19344898:165:93
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PMID: 19606474 [PubMed] Reynolds CA et al: "A survey of ABCA1 sequence variation confirms association with dementia."
No. Sentence Comment
120 From the outset, we were particularly interested in rs2230806 (R219K), rs2230808 (R1587K), and rs4149313 (I883M), becuase these are the only known common nonsynonymous variants (nsSNPs) in the region.
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PMID: 19059534 [PubMed] Porchay-Balderelli I et al: "Relationships between common polymorphisms of adenosine triphosphate-binding cassette transporter A1 and high-density lipoprotein cholesterol and coronary heart disease in a population with type 2 diabetes mellitus."
No. Sentence Comment
3 We studied 5 SNPs: +69CNT, +378GNC, R219K, I883M, and R1587K.
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ABCA1 p.Arg219Lys 19059534:3:36
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27 We chose to study 2 noncoding SNPs located in 5' untranslated regions- +69CNT and +378GNC-and 3 nonsynonymous SNPs- R219K, I883M, and R1587K-based on their potential regulatory role or their influence on lipid levels or CHD, as described in other population studies [5].
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45 Genotyping The +69CNT (rs1800977), +378GNC (rs1800978), and R219K (+1051GNA, rs2230806) SNPs were genotyped using a polymerase chain reaction-molecular beacon technique [10].
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65 A cross-sectional analysis of data for the patients on entry into the DIABHYCAR study showed that the prevalence of previous CHD depended on R219K genotype (Tables 4 and 5).
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77 The influence of +378GNC on HDL-C is consistent with the results we previously obtained for a sample from the French general population in the Data From an Epidemio- Table 2 Sequences of primers and probes used for genotyping ABCA1 SNPs SNP Primers (5'-3') Allele-specific probes (5'-3') +69CNT (rs1800977) a U: GAGGAGGGAGAGCACAGG Fam-GCGACAACTAGTCCCGGCAAAAGTCGC-dabcyl L: CTCACTCTCGCTCGCAATTA Tamra-GCGACAACTAGTCTCGGCAAAAGTCGC-dabcyl +378GNC (rs1800978) a U: CCTGCTGTGAGCTCTGG Fam-GCGACACGCTGGGGGTGCTGGCGTCGC-dabcyl L: AGGTTCTTCCACAGCAGCA Tamra-GCGACACGCTGGGCGTGCTGGCGTCGC-dabcyl R219K (rs2230806)a U: GATTCAACTTGGTGACCAAG Fam-GCGACCCTACCAAAGGAGAAACGTCGC-dabcyl L: GAACGAAGTACTCGCTCTGC Tamra-GCGACCCTACCAAGGGAGAAACGTCGC-dabcyl I883M (rs4149313)b U: CTACTGGTTTGGCGAGGAAA Fam-CTTTCTGATATTCTCTTC-Bhq L: AGCAGGAGGTCAACAGCACT Hex-CTTTCTGACATTCTCTTC-Bhq R1587K (rs2230808)b U: CCCTGCCAACTTTACCATGA Fam-CATTATTTTTGGTGTCC-Bhq L: CGATTTCTCAACAGCTTGGG Hex-CATTATTTCTGGTGTCC-Bhq a Molecular beacon.
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ABCA1 p.Arg219Lys 19059534:77:581
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79 Table 3 High-density lipoprotein cholesterol levels (mean ± SD; in millimoles per liter) as a function of ABCA1 SNPs +69CNT +378GNC R219K I883M R1587K 0 1.30 ± 0.35 1.32 ± 0.36 1.31 ± 0.36 1.31 ± 0.35 1.33 ± 0.35 1 1.33 ± 0.37 1.30 ± 0.35 1.32 ± 0.35 1.34 ± 0.36 1.31 ± 0.36 2 1.31 ± 0.33 1.26 ± 0.24 1.33 ± 0.36 1.35 ± 0.33 1.29 ± 034 P .18 .04 .69 .03 .06 Trend test (multiple linear regression) with genotypes coded 0, 1, or 2 according to the number of minor alleles, adjusted for sex, age, BMI, smoking, HbA1c, and lipid-lowering treatment.
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ABCA1 p.Arg219Lys 19059534:79:136
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81 The lack of association between +69CNT and R219K and HDL ( Systat Software Inc, San Jose, CA, USA).
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ABCA1 p.Arg219Lys 19059534:81:43
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91 Associations between R219K and lipid levels or atherosclerosis progression and atherosclerosis have been widely reported [16,21-25].
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ABCA1 p.Arg219Lys 19059534:91:21
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96 The cholesterol efflux from cells in the arterial wall that have the potential to transform into foam cells, primarily macrophages, Table 4 Genotype distribution (percentage) of ABCA1 SNPs as a function of CHD, with P values for χ2 tests CHD history MI history Angina history Incident CHD Without With Without With Without With Without With n = 2647 n = 482 n = 2957 n = 172 n = 2750 n = 379 n = 2906 n = 223 CC 41.7 40.5 41.2 47.1 41.9 38.3 41.5 40.8 +69CNT CT 45.4 48.9 45.7 48.8 45.5 48.7 45.8 47.5 TT 13.0 10.6 13.1 4.1 12.5 13.0 12.7 11.7 P .23 .002 .40 .85 GG 75.3 74.6 75.3 73.5 75.2 74.8 75.2 74.9 +378GNC GC 22.9 23.5 22.8 25.3 23.0 22.8 22.9 23.3 CC 1.9 1.9 1.9 1.2 1.8 2.4 1.9 1.8 P .95 .63 .72 .99 RR 50.1 56.1 50.6 56.6 50.4 55.9 51.3 47.3 R219K RK 41.9 36.3 41.6 33.9 41.6 37.2 40.7 45.9 KK 8.0 7.6 7.8 9.5 8.1 7.0 8.0 6.8 P .05 .15 .13 .29 II 70.7 73.0 70.9 72.8 70.8 73.1 70.8 74.2 I883M IM 26.9 25.2 26.7 25.4 27.0 24.5 26.9 23.1 MM 2.4 1.9 2.3 1.8 2.3 2.4 2.3 2.7 P .56 .82 .61 .44 RR 54.8 51.2 54.3 53.5 54.8 50.4 54.0 57.5 R1587K RK 37.8 42.9 38.4 41.9 38.0 43.2 38.9 34.8 KK 7.3 5.9 7.3 4.7 7.2 6.4 7.1 7.7 P .09 .36 .16 .49 Table 5 Logistic regression analysis for CHD history (odds ratio with 95% CI) CHD MI Angina +69CNT Codominant 0.98 (0.84-1.14) P = .79 0.71 (0.56-0.91) P = .006 1.11 (0.94-1.30) P = .21 Recessive (TT vs C+) 0.83 (0.60-1.14) P = .26 0.28 (0.13-0.61) P = .001 1.10 (0.79-1.53) P = .57 R219K Codominant 0.86 (0.74-1.02) P = .08 0.92 (0.71-1.18) P = .50 0.86 (0.72-1.03) P = .10 Dominant (K+ vs RR) 0.80 (0.65-0.98) P = .03 0.81 (0.59-1.11) P = .19 0.82 (0.65-1.02) P = .08 R1587K Dominant (K+ vs RR) 1.22 (1.00-1.49) P = .06 1.04 (0.76-1.43) P = .79 1.27 (1.01-1.58) P = .04 Odds ratios (95% CI) for minor alleles of ABCA1 SNPs adjusted for age, sex, smoking, BMI, diabetes duration, hypertension, lipid-lowering treatment, serum creatinine, plasma triglyceride, and urinary albumin concentrations.
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ABCA1 p.Arg219Lys 19059534:96:758
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PMID: 18927311 [PubMed] Isomura M et al: "IL12RB2 and ABCA1 genes are associated with susceptibility to radiation dermatitis."
No. Sentence Comment
7 In the ABCA1 gene, one of these SNPs was a nonsynonymous coding SNP causing R219K (P = 0.0065).
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ABCA1 p.Arg219Lys 18927311:7:76
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PMID: 18706283 [PubMed] Iatan I et al: "Effect of ABCA1 mutations on risk for myocardial infarction."
No. Sentence Comment
74 To date, the largest study examining ABCA1 single nucleotide polymorphisms (SNPs) and HDL-C is the Copenhagen City Heart Study [24], in which the relationship between six ABCA1 nonsynonymous common SNPs (R219K, V771M, M825I, I883M, E1172D, and R1587K) and HDL-C was analyzed.
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ABCA1 p.Arg219Lys 18706283:74:204
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109 As previously described [30,33,34], of the 16 polymorphisms located in the promoter and the 10 found in the coding region, it was concluded that only the R219K polymorphism was associated with MI, decreasing its risk (odds ratio of 0.80; 95% CI, 0.68-0.94; P = 0.007), whereas no haplotypes were involved in the susceptibility to CHD.
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ABCA1 p.Arg219Lys 18706283:109:154
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112 Additional insights into the effects of ABCA1 on MI have recently been described by Frikke-Schmidt et al. [35•] in a study where six nonsynonymous ABCA1 SNPs, R219K, V771M, V825I, I883M, E1172D, and R1587K (identified by resequencing ABCA1 in 190 individuals of Danish ancestry [24]), were genotyped in 9259 individuals from the Copenhagen City Heart Study to assess their risk of CHD (Table 2).
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ABCA1 p.Arg219Lys 18706283:112:166
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113 The principal finding of the study indicated that common genetic variation in ABCA1 predicts risk of CHD in the general population, but that their association was independent of plasma HDL-C levels: SNPs predicting increased MI risk were associated with either increases (V771 and V825I) or decreases (R1587K) in HDL-C, or no effect on HDL-C (R219K, I883M, E1172D).
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ABCA1 p.Arg219Lys 18706283:113:343
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121 TD patients ( n = 5) 0.08 ± 0.05 ABCA1 heterozygous patients ( n = 77) 0.74 ± 0.24 Unaffected individuals ( n = 156) 1.31 ± 0.35 Brousseau et al. [30] / 2001 VA-HIT study, men with established CHD ( n = 1014) 0.83 ± 0.13 R219K, I883M, E1172D † Frequencies of the 3 ABCA1 variants were signifi cantly increased in VA-HIT.
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ABCA1 p.Arg219Lys 18706283:121:241
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124 Framingham Offspring Study, CHD-free control men ( n = 1014) 1.14 ± 0.31 Clee et al. [33] / 2001 REGRESS cohort, with established CHD ( n = 804) R219K genotype: R219K † The R219K SNP is associated with a decreased progression of CHD, decreased TG, and increased HDL-C RR: 0.92 ± 0.22 RK: 0.93 ± 0.23 KK: 0.92 ± 0.20 Lutucuta et al. [38] / 2001 Lipoprotein Coronary Atherosclerosis Study patients ( n = 372) C-477T genotype: C-477T † , A-419C, G-320C The C-477T variant was strongly associated with the severity of coronary atherosclerosis, with modest effect on HDL-C CC: 1.14 ± 0.29 CT: 1.10 ± 0.28 TT: 1.19 ± 0.32 *Studies reporting the initial molecular and biochemical characterization of fewer than 5 probands with an ABCA1 gene defect and their families were not included in Table 2.
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ABCA1 p.Arg219Lys 18706283:124:150
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ABCA1 p.Arg219Lys 18706283:124:166
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132 GG: 0.93 ± 0.23 GC: 0.92 ± 0.22 CC: 0.94 ± 0.29 C-17G genotype: CC: 0.92 ± 0.22 CG: 0.93 ± 0.23 GG: 0.88 ± 0.21 C69T genotype: CC: 0.91 ± 0.22 CT: 0.91 ± 0.19 TT: 0.95 ± 0.30 A-1095G genotype: AA: 0.93 ± 0.24 AG: 0.93 ± 0.22 GG: 0.83 ± 0.20 InsG319 genotype: No ins: 0.92 ± 0.23 G: 0.93 ± 0.23 GG: 0.89 ± 0.30 Cenarro et al. [34] / 2003 Spanish heterozygous FH patients with premature CHD ( n = 216) or without ( n = 158) R219K genotype: R219K † The frequency of the K219 allele was signifi cantly higher in the FH group without premature CHD than in FH patients with premature CHD RR: 1.27 ± 0.36 RK + KK: 1.32 ± 0.40 *Studies reporting the initial molecular and biochemical characterization of fewer than 5 probands with an ABCA1 gene defect and their families were not included in Table 2.
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ABCA1 p.Arg219Lys 18706283:132:497
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135 Genetic variation in ABCA1 and risk of myocardial infarction Study* / year Population screened HDL-C, mmol/L ABCA1 variants Conclusions Evans and Beil [41] / 2003 Patients attending a lipid outpatient clinic ( n = 813) R219K genotype: R219K † The K219 allele was signifi cantly protective against CHD in patients with hyperlipidemia and elevated Lp(a), as well as decreasing TG levels RR: 1.32 ± 0.03 RK: 1.34 ± 0.03 KK: 1.27 ± 0.31 Harada et al. [29] / 2003 Japanese patients ( n = 410) I883M genotype: I883M, R219K The I883M polymorphism was signifi cantly associated with higher HDL-C in Japanese patients, but not with CHD II: 1.16 ± 0.30 IM: 1.26 ± 0.42 MM: 1.27 ± 0.37; P = 0.05 R219K genotype: RR: 1.26 ± 0.41 RK: 1.25 ± 0.40 KK: 1.24 ± 0.35 Tan et al. [42] / 2003 Cases: Chinese ( n = 512), Malay ( n = 110), and Indian ( n = 164) men with established CHD Chinese: CAD: 0.89 ± 0.28, Ctl: 1.19 ± 0.32; P < 0.0005 C-14T, 237indelG, V825I † , M883I † , A8994G The V825I and M883I polymorphisms are positive markers for the CHD phenotype in Malays, but with no effect on HDL-C Malays: CAD: 0.83 ± 0.27, Ctl: 1.15 ± 0.27; P < 0.0005 Controls: Chinese ( n = 271), Malay ( n = 179), and Indian ( n = 231) men Indians: CAD: 0.79 ± 0.24, Ctl: 1.00 ± 0.26; P < 0.0005 Tregouet et al. [31] / 2004 Subgroup of ECTIM cohort ( n = 452 cases and n = 465 controls) NA C-564T, R219K † , R1587K ABCA1 polymorphisms, but not haplotypes, are involved in variability of apoA-I and the susceptibility to CHD.
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ABCA1 p.Arg219Lys 18706283:135:219
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ABCA1 p.Arg219Lys 18706283:135:722
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ABCA1 p.Arg219Lys 18706283:135:1464
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137 R219K was associated with MI (K219 allele associated with a decreased risk), but not with apoA-I.
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ABCA1 p.Arg219Lys 18706283:137:0
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141 Genetic variation in ABCA1 and risk of myocardial infarction Study* / year Population screened HDL-C, mmol/L ABCA1 variants Conclusions Shioji et al. [43] / 2004 Japanese Suita Study ( n = 1880) Suita group: 1.44 ± 0.02 G-273C The G-273C polymorphism was signifi cantly associated with HDL-C in the general Japanese population but not on the incidence of MI MI group ( n = 598 men) MI group: 1.09 ± 0.01; P < 0.0001 Bertolini et al. [39] / 2004 FH patients: All FH patients: males: 1.18 ± 0.02, females: 1.39 ± 0.02; P < 0.0001 R219K † The K219 allele was signifi cantly protective against CHD, and this effect was more pronounced in males than in females and in smokers versus nonsmokers (but there was no signifi cant effect on lipid concentrations).
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ABCA1 p.Arg219Lys 18706283:141:548
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146 Noncarriers ( n = 9039) Women: 1.72 ± 0.01 Men: 1.38 ± 0.01 K776N carriers ( n = 37) Women: 1.82 ± 0.11 Men: 1.18 ± 0.09 P = 0.05 Martin et al. [37] / 2006 Cohort of males diagnosed with MI ( n = 170) NA C-477T † , R219K, I883M In long-term MI prognosis, the C-477T ABCA1 variant was associated with an unfavorable clinical evolution Controls: valvular patients with normal coronariography controls ( n = 100) *Studies reporting the initial molecular and biochemical characterization of fewer than 5 probands with an ABCA1 gene defect and their families were not included in Table 2.
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ABCA1 p.Arg219Lys 18706283:146:242
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149 Genetic variation in ABCA1 and risk of myocardial infarction Study* / year Population screened HDL-C, mmol/L ABCA1 variants Conclusions Andrikovics et al. [45] / 2006 Hungarian patients with ischemic stroke ( n = 244) NA R219K † , V771M † , I883M A higher frequency of R219K and V771M was observed in controls than in Hungarian stroke patients, suggesting a protective role against CHD Hungarian patients with CHD ( n = 150) Controls (n = 193) Benton et al. [46] / 2007 Subgroup of Multi-Ethnic Study of Atherosclerosis study group ( n = 969) R219K genotype: C-565T, R219K † The R219K polymorphism was associated with a 28% lower prevalence of coronary calcifi cation, a measure of subclinical atherosclerosis, and slightly higher HDL-C level RR: 1.34 ± 0.38 RK: 1.29 ± 0.35 KK: 1.37 ± 0.39 Tsai et al. [47] / 2007 Taiwanese patients with CHD ( n = 205) and controls ( n = 201) Cases: 1.04 ± 0.25 I823M The M823 allele was associated with higher HDL-C.
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ABCA1 p.Arg219Lys 18706283:149:221
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152 Cases: 1.70 (1.5-2.0) Ctl: 1.30 (1.1-1.6) Pasdar et al. [49] / 2007 White ischemic stroke patients ( n = 400) Cases: 1.20 ± 0.40 L158L, R219K, G316G, R1587K The ABCA1 gene was not found to be associated with ischemic stroke, but R219K had the greatest impact on lipid profi le, especially on LDL and TG White controls ( n = 487) Ctl: 1.40 ± 0.40 Nebel et al. [50] / 2007 German patients with CHD ( n = 1090) and controls ( n = 728) NA R219K, V771M, I883M † , E1172D, R1587K Only the I883M polymorphism was signifi cantly associated with CHD *Studies reporting the initial molecular and biochemical characterization of fewer than 5 probands with an ABCA1 gene defect and their families were not included in Table 2.
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ABCA1 p.Arg219Lys 18706283:152:141
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ABCA1 p.Arg219Lys 18706283:152:234
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155 Genetic variation in ABCA1 and risk of myocardial infarction Study* / year Population screened HDL-C, mmol/L ABCA1 variants Conclusions Frikke-Schmidt et al. [35••] / 2008 Copenhagen City Heart Study: Women: R219K, V771M † , V825I † , I883M † , E1172D † , R1587K † Common genetic variation at the ABCA1 locus predicts IHD risk independently of plasma HDL-C levels.
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ABCA1 p.Arg219Lys 18706283:155:222
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170 Three ABCA1 SNPs were analyzed (-477C/T, R219K, and I883) in a cohort of 170 young male survivors of MI (mean age, 43 ± 5 years) in order to determine their influence in long-term prognosis.
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ABCA1 p.Arg219Lys 18706283:170:41
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174 Additionally, several recent studies have examined the role of the R219K SNP in lipoprotein metabolism and CHD.
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PMID: 18803945 [PubMed] Sandhofer A et al: "The influence of two variants in the adenosine triphosphate-binding cassette transporter 1 gene on plasma lipids and carotid atherosclerosis."
No. Sentence Comment
1 We investigated the influence of the R219K and I883M variants in the ABCA1 gene on plasma lipids and carotid intima media thickness and plaque extent in 688 healthy men (40-60 years old).
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ABCA1 p.Arg219Lys 18803945:1:37
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2 The R219K variant showed no effect on plasma lipids, but carriers of the K allele displayed a lower intima media thickness (P = .001) and a reduced risk of advanced plaque extent (odds ratio [OR], 0.59; 0.39-0.88; P = .009) compared with noncarriers.
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5 Risk of advanced plaque extent was reduced in subjects carrying the R219K variant alone (OR, 0.59; 0.38-0.94; P = .025), but not in subjects carrying both variants.
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7 We conclude that smoking abrogates the protective effect of the R219K.
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ABCA1 p.Arg219Lys 18803945:7:64
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24 We investigated and report here the role of smoking on the influence of the R219K and I883M variants in the ABCA1 gene on plasma lipid levels and ultrasonographically quantified intima media thickness (IMT) and severity of atherosclerosis of the carotid artery in a cross-sectional cohort of 688 middle-aged men.
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ABCA1 p.Arg219Lys 18803945:24:76
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43 The R219K and I883M status was determined using polymerase chain reaction-based restriction fragment length analysis, as described [5,6].
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50 Table 1 Clinical and laboratory characteristics R219K I883M RR (350) RK (274) KK (64) RK + KK II (522) IM (151) MM (15) IM + MM (166) Age (y) 50.0 (5.2) 49.4 (5.5) 50.9 (5.5) 49.7 (5.5) 50.1 (5.3) 49.2 (5.4) 47.9 (5.7) 49.1 (5.4) BMI (kg/m2 ) 27.2 (3.4) 27.2 (3.8) 26.9 (4.4) 27.2 (3.9) 27.2 (3.9) 27.1 (4.1) 26.3 (4.7) 27.0 (4.1) SBP (mm Hg) 130.9 (11.8) 129.4 (12.1) 130.9 (13.3) 129.7 (12.3) 130.7 (12.1 129.0 (11.9) 127.9 (12.2) 128.9 (11.9) DBP (mm Hg) 80.3 (7.4) 79.1 (7.1) 79.7 (6.5) 79.27 (7.0) 79.9 (7.1) 79.5 (7.6) 76.1 (5.2) 79.2 (7.4) Smoking (%)† 49.1 40.5 53.6 46.2 47.5 40.8 50.0 47.2 DM (%)† 4.9 4.7 0 3.8 4.4 4.0 6.7 4.2 TC (mg/dL) 230.5 (41.7) 225.5 (40.3) 228.5 (36.0) 226.1 (39.5) 226.9 (40.2) 233.0 (42.5) 234.1 (35.8) 233.1 (41.8) LDL-C (mg/dL) 148.2 (37.7) 144.2 (37.2) 150.0 (35.7) 145.3 (37.0) 145.2 (37.2) 151.5 (37.9) 155.0 (34.8) 151.8⁎ (37.5) HDL-C (mg/dL) 54.6 (13.2) 53.4 (12.9) 53.5 (11.4) 53.5 (12.7) 53.9 (13.0) 54.0 (13.0) 57.6 (11.9) 54.3 (12.9) TGs (mg/dL) 138.4 (92.0) 138.7 (81.0) 132.8 (74.5) 137.6 (79.7) 138.5 (87.2) 138.5 (85.7) 116.2 (45.6) 136.5 (83.0) Apo A-I (mg/dL) 149.0 (22.2) 148.7 (23.0) 148.8 (20.1) 148.7 (22.4) 148.8 (22.5) 148.7 (21.4) 150.9 (23.8) 148.9 (21.6) Apo B (mg/dL) 119.7 (25.4) 119.8 (25.5) 120.9 (25.7) 119.2 (25.5) 118.7 (24.8) 122.0 (18.0) 118.9 (19.5) 121.7 (27.3) LDL size (nm) 26.4 (1.11) 26.2 (1.17) 26.3 (1.28) 26.2 (1.19) 26.3 (1.14) 26.2 (1.20) 26.4 (0.88) 26.3 (1.17) Values are means (SD).
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ABCA1 p.Arg219Lys 18803945:50:48
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68 Frequencies of the R219K and I883M variants Allele frequency was 29.2% for the K allele at position 219 and 13.1% for the M allele at position 883; carrier frequency was 49.1% for the K allele and 21.9% for the M allele.
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ABCA1 p.Arg219Lys 18803945:68:19
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69 Distribution of genotypes was in Hardy-Weinberg equilibrium (P = .30 and P = .33, for R219K and I883M, respectively).
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ABCA1 p.Arg219Lys 18803945:69:86
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73 Effect of the R219K and I883M variants on plasma lipids and IMT Table 1 illustrates the clinical characteristics and laboratory parameters of the subjects according to the genotypes.
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74 Carriers of the I883M variant had a higher LDL-C compared with men homozygous for the wild-type allele.
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75 Carriers of the R219K variant had a lower IMT compared with noncarriers (781 ± 6 vs 802 ± 7 μm, P b.01), whereas the I883M variant had no effect on IMT (798 ± 9 vs 798 ± 6 μm, not significant [NS]) (Fig. 1).
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77 Effect of the R219K and I883M variants in combination on plasma lipids and IMT Furthermore, plasma lipids, apolipoproteins, and LDL size did not differ between the groups according to the combined carrier status of the 2 variants (Table 2).
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79 The R219K and I883M variants and IMT.
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85 Effect of the R219K and I883M variants on risk of atherosclerosis The risk of advanced atherosclerosis-defined as a plaque score of 3 and higher-was significantly reduced in carriers of the K allele (Table 3).
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ABCA1 p.Arg219Lys 18803945:85:14
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92 Effect of the R219K and I883M variants in combination on risk of atherosclerosis The reduced risk of advanced atherosclerosis observed in carriers of the K allele at position 219 was attenuated by the carrier status at position 883.
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ABCA1 p.Arg219Lys 18803945:92:14
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ABCA1 p.Arg219Lys 18803945:92:248
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93 The unadjusted relative risk was 0.85 (95% CI, 0.72-1.00; P = .065) for carriers of the K allele alone, 1.04 (95% CI, 0.92-1.16; NS) for carriers of the M variant alone, and 0.87 (95% CI, 0.78-0.98; P b .05) for carriers of both variants, that is, R219K and I883M.
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ABCA1 p.Arg219Lys 18803945:93:248
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100 A positive smoking history abolished the protective effect of the R219K variant.
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114 We therefore used this imaging technique to investigate the influence of the R219K and I883M variants in the ABCA1 gene on the extent of carotid atherosclerosis and plasma lipids in 688 middle-aged men.
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ABCA1 p.Arg219Lys 18803945:114:77
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116 Men carrying the R219K variant had a reduced risk of carotid atherosclerosis and lower IMT values.
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119 This finding is in accordance with a previous report showing, for the R219K allele, less severe CAD and slower progression of CAD in carriers of the K allele [6]; but although Clee et al [6] demonstrated increased HDL-C and reduced TG levels in carriers, we observed no effect of the K allele on plasma lipids.
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ABCA1 p.Arg219Lys 18803945:119:70
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127 Previous reports suggest that the R219K variant influences HDL-C concentration only in special subpopulations, such as smokers [8] or subjects with elevated Lp(a) or apo E3 [28], indicating a gene-environment or gene-gene interaction.
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128 However, in our population, the R219K variant was protective independent of Lp(a) concentration and apo E genotype (data not shown).
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129 In contrast to previous reports, the R219K variant was protective in nonsmokers only, suggesting that the "genetic advantage" of carrying the K variant is abolished by the established risk factor of smoking.
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136 However, this possible effect of the R219K variant needs further investigation.
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ABCA1 p.Arg219Lys 18803945:136:37
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140 To further investigate if the R219K variant is the causative variant, we combined the R219K carrier status with the I883M carrier status.
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ABCA1 p.Arg219Lys 18803945:140:30
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ABCA1 p.Arg219Lys 18803945:140:86
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143 However, in our population, the I883M variant itself had no effect on carotid atherosclerosis.
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ABCA1 p.Arg219Lys 18803945:143:31
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144 Therefore, we suggest that the R219K variant is possibly not the causative variant.
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ABCA1 p.Arg219Lys 18803945:144:13
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ABCA1 p.Arg219Lys 18803945:144:31
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145 In fact, the R219K variant may be in linkage disequilibrium with another variant responsible for the observed risk reduction.
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ABCA1 p.Arg219Lys 18803945:145:13
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147 We conclude from this study that the R219K variant in the ABCA1 gene can alter risk of atherosclerosis independently from HDL-C and TG plasma concentration in nonsmoking, healthy, middle-aged men.
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ABCA1 p.Arg219Lys 18803945:147:37
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148 Because smoking abolished the protective effect of the R219K variant, we hypothesize that smoking may influence ABCA1 efficacy.
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ABCA1 p.Arg219Lys 18803945:148:55
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ABCA1 p.Arg219Lys 18803945:148:106
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149 Considering the functions of ABCA1 other than lipid transport, the fact that the protective effect of the R219K is not dependent on plasma HDL-C or TG concentration suggests to us that another function of ABCA1 may be implicated.
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67 Frequencies of the R219K and I883M variants Allele frequency was 29.2% for the K allele at position 219 and 13.1% for the M allele at position 883; carrier frequency was 49.1% for the K allele and 21.9% for the M allele.
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72 Effect of the R219K and I883M variants on plasma lipids and IMT Table 1 illustrates the clinical characteristics and laboratory parameters of the subjects according to the genotypes.
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ABCA1 p.Arg219Lys 18803945:72:14
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76 Effect of the R219K and I883M variants in combination on plasma lipids and IMT Furthermore, plasma lipids, apolipoproteins, and LDL size did not differ between the groups according to the combined carrier status of the 2 variants (Table 2).
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78 The R219K and I883M variants and IMT.
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ABCA1 p.Arg219Lys 18803945:78:4
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84 Effect of the R219K and I883M variants on risk of atherosclerosis The risk of advanced atherosclerosis-defined as a plaque score of 3 and higher-was significantly reduced in carriers of the K allele (Table 3).
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ABCA1 p.Arg219Lys 18803945:84:14
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91 Effect of the R219K and I883M variants in combination on risk of atherosclerosis The reduced risk of advanced atherosclerosis observed in carriers of the K allele at position 219 was attenuated by the carrier status at position 883.
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99 A positive smoking history abolished the protective effect of the R219K variant.
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113 We therefore used this imaging technique to investigate the influence of the R219K and I883M variants in the ABCA1 gene on the extent of carotid atherosclerosis and plasma lipids in 688 middle-aged men.
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ABCA1 p.Arg219Lys 18803945:113:77
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115 Men carrying the R219K variant had a reduced risk of carotid atherosclerosis and lower IMT values.
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ABCA1 p.Arg219Lys 18803945:115:17
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118 This finding is in accordance with a previous report showing, for the R219K allele, less severe CAD and slower progression of CAD in carriers of the K allele [6]; but although Clee et al [6] demonstrated increased HDL-C and reduced TG levels in carriers, we observed no effect of the K allele on plasma lipids.
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ABCA1 p.Arg219Lys 18803945:118:70
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126 Previous reports suggest that the R219K variant influences HDL-C concentration only in special subpopulations, such as smokers [8] or subjects with elevated Lp(a) or apo E3 [28], indicating a gene-environment or gene-gene interaction.
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135 However, this possible effect of the R219K variant needs further investigation.
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ABCA1 p.Arg219Lys 18803945:135:37
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139 To further investigate if the R219K variant is the causative variant, we combined the R219K carrier status with the I883M carrier status.
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ABCA1 p.Arg219Lys 18803945:139:30
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ABCA1 p.Arg219Lys 18803945:139:86
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146 We conclude from this study that the R219K variant in the ABCA1 gene can alter risk of atherosclerosis independently from HDL-C and TG plasma concentration in nonsmoking, healthy, middle-aged men.
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PMID: 18164264 [PubMed] Genvigir FD et al: "Effects of ABCA1 SNPs, including the C-105T novel variant, on serum lipids of Brazilian individuals."
No. Sentence Comment
2 Methods: The effect of the ABCA1 SNPs C-14T, R219K and of a novel variant C-105T on serum lipids was investigated in 367 unrelated Brazilian individuals (224 hypercholesterolemic and 143 normolipidemic).
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ABCA1 p.Arg219Lys 18164264:2:45
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7 The R219K SNP was associated with reduced serum triglyceride, VLDL-c and TG/HDL-c ratio in the HC group (pb0.05), and with an increased serum apoAI in NL individuals.
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ABCA1 p.Arg219Lys 18164264:7:4
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9 Conclusions: The ABCA1 SNPs R219K and C-105T were associated with a less atherogenic lipid profile but not with the lowering-cholesterol response to atorvastatin in a Brazilian population.
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ABCA1 p.Arg219Lys 18164264:9:28
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25 The R219K single nucleotide polymorphism (SNP) has been associated with protection against coronary artery disease (CAD) risk and severity [18-23].
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65 ABCA1 C-14T and R219K SNPs were detected by polymerase chain reaction (PCR) and restriction fragment length polymorphism (RFLP) assays.
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66 The primers for C-14T (forward: 5'-CTCCACGTGCTTTCTGC- TGA-3', and reverse 5'-CACTCACTCTCGCTCGCAAT-3') and R219K (forward: 5'-GAAGAGATGATTCAACTTGGTGAC-3', and reverse 5'-GCCCAAAAG- TCTGAAAGAACAC-3') were selected using the ABCA1 reference sequence (GenBank Acession number AF275948) previously described [39].
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ABCA1 p.Arg219Lys 18164264:66:106
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68 The PCR thermal cycling conditions consisted of initial incubation at 98 °C for 3 min, followed by 29 cycles at 94 °C for 1 min, 57 °C for 2 min and 72 °C for 1 min for C-14T polymorphism or by 32 cycles at 94 °C for 45 s, 58 °C for 1.5 min and 72 °C for 1.5 min for R219K SNP and a final extension period of 72 °C for 10 min.
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ABCA1 p.Arg219Lys 18164264:68:295
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70 PCR products of C-14T and R219K SNPs (173 bp and 295 bp respectively) were analyzed by 1% agarose gel electrophoresis after ethidium bromide staining.
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71 PCR products of the C-14T and R219K SNPs were initially digested with the MspI and StyI endonucleases (New England Biolabs Inc., Ipswich MA) respectively, at 37 °C.
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ABCA1 p.Arg219Lys 18164264:71:30
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108 Genotype and allele frequencies of ABCA1 R219K, C-14T and C-105T SNPs in NL and HC groups are shown in Table 2.
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ABCA1 p.Arg219Lys 18164264:108:41
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109 Table 2 Genotype and allele frequencies for ABCA1 R219K, C-14T and C-105T polymorphisms in the NL and HC groups Polymorphisms NL (143) HC (224) R219K genotypes, % RR 37.8 (54) 33.9 (76) χ2 =0.857 p=0.652 RK 43.3 (62) 48.2 (108) KK 18.9 (27) 17.9 (40) K allele 40.6 42.0 C-14T genotypes, % CC 42.0 (60) 43.3 (97) χ2 =2.000 p=0.363 CT 48.9 (70) 43.3 (97) TT 9.1 (13) 13.4 (30) T allele 33.6 35.0 C-105T genotypes, % CC 97.2 (139) 96.4 (216) Exact Fisher test p=1.000CT 2.8 (4) 3.1 (7) TT 0 (0) 0.5 (1) T allele 1.4 2.0 Number of individuals in parenthesis.
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ABCA1 p.Arg219Lys 18164264:109:50
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110 Hardy-Weinberg Equilibrium: R219K SNP: χ2 =0.76 (pN0.05).
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ABCA1 p.Arg219Lys 18164264:110:28
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113 Table 3 Effects of ABCA1 R219K polymorphism on basal serum lipids in NL and HC groups Variables NL genotypes (143) HC genotypes (224) 219RR (54) 219RK/ KK (89) p 219RR (76) 219RK/ KK (148) p Total cholesterol (mmol/l) 4.47±0.51 4.49±0.45 0.723 6.67±1.17 6.64±1.23 0.822 LDL-c (mmol/l) 2.59±0.48 2.55±0.44 0.696 4.39±1.11 4.41±1.13 0.890 HDL-c (mmol/l) 1.43±0.32 1.51±0.34 0.150 1.43±0.38 1.50±0.38 0.157 VLDL-c (mmol/l) 0.44±0.15 0.43±0.15 0.557 0.85±0.40 0.72±0.29 0.036 Triglyceride (mmol/l) 0.96±0.32 0.93±0.32 0.557 1.86±0.88 1.58±0.64 0.039 ApoAI (g/l) 1.36±0.29 1.46±0.27 0.035 1.37±0.28 1.40±0.30 0.513 ApoB (g/l) 0.88±0.24 0.84±0.21 0.416 1.31±0.33 1.31±0.28 0.876 ApoB/apoAI 0.67±0.23 0.60±0.21 0.074 1.00±0.33 0.99±0.37 0.732 TG/HDL-c 0.73±0.34 0.66±0.34 0.266 1.48±0.96 1.17±0.69 0.030 Number of individuals in parenthesis. Values are presented as mean±SD of log transformed data. Results were compared by t-test. ApoAI, apolipoprotein AI; apoB, apolipoprotein B; HC, hypercholesterolemic patients; HDL-c, high-density lipoprotein cholesterol; LDL-c, low-density lipoprotein cholesterol; NL, normolipidemic patients; TG, triglyceride; VLDL-c, very low-density lipoprotein cholesterol. Table 4 Effects of ABCA1 C-14T SNP on basal serum lipids in NL and HC groups Variables NL genotypes (143) HC genotypes (224) -14CC (60) -14CT/TT (83) p -14CC (97) -14CT/TT (127) p Total cholesterol (mmol/l) 4.45±0.39 4.51±0.52 0.739 6.68±1.29 6.63±1.14 0.778 LDL-c (mmol/l) 2.51±0.41 2.62±0.49 0.276 4.43±1.16 4.38±1.09 0.796 HDL-c (mmol/l) 1.53±0.34 1.45±0.34 0.262 1.50±0.41 1.45±0.36 0.466 VLDL-c (mmol/l) 0.44±0.15 0.44±0.15 0.922 0.75±0.36 0.78±0.31 0.138 Triglyceride (mmol/l) 0.94±0.33 0.95±0.32 0.922 1.62±0.79 1.71±0.69 0.151 ApoAI (g/l) 1.45±0.30 1.40±0.26 0.367 1.40±0.32 1.38±0.27 0.639 ApoB (g/l) 0.81±0.19 0.88±0.24 0.064 1.30±0.33 1.31±0.27 0.705 ApoB/apoAI 0.59±0.20 0.66±0.23 0.065 0.98±0.32 1.00±0.38 0.599 TG/HDL-c 0.67±0.36 0.70±0.33 0.500 1.23±0.85 1.31±0.77 0.147 Number of individuals in parenthesis. Values are presented as mean±SD of log transformed data. Results were compared by t-test. ApoAI, apolipoprotein AI; apoB, apolipoprotein B; HC, hypercholesterolemic patients; HDL-c, high-density lipoprotein cholesterol; LDL-c, low-density lipoprotein cholesterol; NL, normolipidemic patients; TG, triglyceride; VLDL-c, very low-density lipoprotein cholesterol.
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ABCA1 p.Arg219Lys 18164264:113:25
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122 These results are suggestive that ABCA1 R219K SNP and possibly the novel variant C-105T are associated with a less atherogenic serum lipid profile.
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ABCA1 p.Arg219Lys 18164264:122:40
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128 After the therapy, R219K and C-105T SNPs continued to show an association with a less atherogenic serum lipid profile (Fig. 2), but no ABCA1 SNP was associated with percentual variations in serum lipids after the treatment (data not shown).
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ABCA1 p.Arg219Lys 18164264:128:19
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138 In this study ABCA1 R219K SNP was associated with an increased serum apoAI in the NL group and with a reduced serum triglyceride and VLDL-c in HC individuals.
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ABCA1 p.Arg219Lys 18164264:138:20
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153 The C-105T SNP, like R219K also appears to be related to a less atherogenic lipid profile since the -105T allele was Fig. 2.
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ABCA1 p.Arg219Lys 18164264:153:21
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155 A) R219K SNP.
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ABCA1 p.Arg219Lys 18164264:155:3
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179 In our study, the HDL-c response to atorvastatin was independent of the ABCA1 C-105T, C-14T or R219K SNP.
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ABCA1 p.Arg219Lys 18164264:179:95
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184 In addition, R219K and, possibly, C-105T polymorphisms are associated with a less atherogenic serum lipid profile in Brazilian hypercholesterolemic patients before and after treatment with atorvastatin.
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ABCA1 p.Arg219Lys 18164264:184:13
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PMID: 18468402 [PubMed] Ergen A et al: "Investigation of ABCA1 C69T and G-191C polymorphisms in coronary artery disease."
No. Sentence Comment
74 They found that the rare alleles of C-14T(C69T) and V771M polymorphisms were associated with higher HDL-C levels in men and, in combination with the rare alleles of R219K and I883M, respectively, with higher HDL-C in both sexes.
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ABCA1 p.Arg219Lys 18468402:74:165
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75 In another study of six common polymorphisms of ABCA1, very high HDL-C was found to be associated with a higher genotype frequency for R219K and higher genotype and allelic frequency for E1172D compared with lower HDL-C (21).
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ABCA1 p.Arg219Lys 18468402:75:135
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79 They suggested that R219K polymorphism in Ergen et al: Investigation of ABCA1 C69T and G-191C Polymorphisms in Coronary Artery Disease 189 Table III.
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ABCA1 p.Arg219Lys 18468402:79:20
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PMID: 18215356 [PubMed] Wang J et al: "Effects of ABCA1 variants on rosiglitazone monotherapy in newly diagnosed type 2 diabetes patients."
No. Sentence Comment
0 (c)2008 CPS and SIMM Acta Pharmacol Sin 2008 Feb; 29 (2): 252-258 Full-lengtharticle Effects of ABCA1 variants on rosiglitazone monotherapy in newly diagnosed type 2 diabetes patients1 Jie WANG2 , Yu-qian BAO2 , Cheng HU2 , Rong ZHANG2 , Cong-rong WANG2 , Jun-xi LU2 , Wei-ping JIA2,3 , Kun-san XIANG2 Shanghai Diabetes Institute, Department of Endocrinology and Metabolism, Shanghai Jiao Tong University Affiliated Sixth People`s Hospital, Shanghai 200233, China Abstract Aim: The aim of the present study was to investigate the relationship between R219K, M883I, and R1587K variants of the ATP-binding cassette transporter subfamilyA number 1 (ABCA1) gene and response to rosiglitazone treatment in newly diagnosed patients with type 2 diabetes.
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ABCA1 p.Arg219Lys 18215356:0:551
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2 Three non-synonymous variants R219K, M883I, and R1587K, were genotyped in all patients.
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ABCA1 p.Arg219Lys 18215356:2:30
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4 The R219K variant of ABCA1had an effect on rosiglitazone response with the per-allele odds ratio of 2.04 for treatment failure (P<0.05).
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ABCA1 p.Arg219Lys 18215356:4:4
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7 Conclusion: The R219K variant ofABCA1was associated with the therapeutic effect ofrosiglitazone.
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ABCA1 p.Arg219Lys 18215356:7:16
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32 In this study, we selected 3 non-synonymous variants of ABCA1, R219K, M883I, and R1587K, toevaluate their effects on rosiglitazone treatment in newly diagnosed patients with type 2 diabetes.
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ABCA1 p.Arg219Lys 18215356:32:63
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88 Pairwise linkage disequilibrium analyses among ABCA1 gene R219K, M883I and R1587K variants.
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ABCA1 p.Arg219Lys 18215356:88:58
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89 | D´| \r2 R219K M883I R1587K R219K 0.041 0.027 M883I 0.372 0.031 R1587K 0.191 0.377 Linkage disequilibrium estimates are shown as |D´| in the lower triangle and r2 in the upper triangle.
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ABCA1 p.Arg219Lys 18215356:89:14
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ABCA1 p.Arg219Lys 18215356:89:15
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91 According to the first criterion, R219K was associated with response to rosiglitazone treatment with more treatment failures in the rare allele homozygotes KK.
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ABCA1 p.Arg219Lys 18215356:91:34
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97 Association between ABCA1 genetic variants and the effect of rosiglitazone treatment on clinical features The association between R219K and clinical features is shown in Table 4.
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ABCA1 p.Arg219Lys 18215356:97:130
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106 In this study, we found that the R219K variant of the ABCA1 gene was associated with response to rosiglitazone therapy in newly diagnosed type 2 diabetes patients.
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ABCA1 p.Arg219Lys 18215356:106:33
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113 The main outcome of our study was that R219K was associated with insulin sensitivityimprovement.
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ABCA1 p.Arg219Lys 18215356:113:39
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119 Criterion 1 Criterion 2 R219K RR RK KK RR RK KK Responder 14 (0.483) 19 (0.452) 2 (0.118) 24 (0.889) 33 (0.767) 11 (0.647) Non-responderb 15 (0.517) 23 (0.548) 15 (0.882) 3 (0.111) 10 (0.233) 6 (0.353) M883I MM MI II MM MI II Responder 15 (0.319) 15 (0.455) 5 (0.625) 33 (0.717) 29 (0.878) 6 (0.750) Non-responder 32 (0.681) 18 (0.545) 3 (0.375) 13 (0.283) 4 (0.121) 2 (0.250) R1587K RR RK KK RR RK KK Responder 13 (0.394) 18 (0.400) 4 (0.400) 26 (0.788) 37 (0.822) 5 (0.556) Non-responder 20 (0.606) 27 (0.600) 6 (0.600) 7 (0.212) 8 (0.178) 4 (0.444) pose that a small change in ABCA1 activity could affect rosiglitazone response without markedlyimpacting circulating cholesterol profiles.
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ABCA1 p.Arg219Lys 18215356:119:24
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126 Association between ABCA1 R219K variant and clinical features.
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ABCA1 p.Arg219Lys 18215356:126:26
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130 The K allele carriers of the R219K variant showed a relatively higher mean drug dose compared with the RR homozygotes, which may also reflect a poorer response torosiglitazone treatment.
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ABCA1 p.Arg219Lys 18215356:130:29
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133 In conclusion, we provide evidence that the R219K variant of the ABCA1 gene either directly or as a marker with additional functional variant in linkage disequilibrium, has an effect on response torosiglitazone treatment.
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ABCA1 p.Arg219Lys 18215356:133:44
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PMID: 18199144 [PubMed] Slatter TL et al: "Novel rare mutations and promoter haplotypes in ABCA1 contribute to low-HDL-C levels."
No. Sentence Comment
41 Genotyping of ABCA1 SNPs by RFLP Fourteen SNPs including five promoter SNPs (C-564T, G-407C, G-278C, G-99C, and C-14T), one 5#-UTR SNP [-76(-75) insG], six non-synonymous coding SNPs (R219K, V771M, V825I, I883M, E1172D, and R1587K) and two 3#-UTR SNPs [A-960G -383(-381)delGTT] were genotyped in the low-, mid-, and high-HDL-C groups by restriction fragment length polymorphism (RFLP) analysis.
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ABCA1 p.Arg219Lys 18199144:41:184
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55 Six of the non-synonymous variants were previously reported SNPs (R219K, V771M, V825I, I883M, E1172D and R1587K).
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ABCA1 p.Arg219Lys 18199144:55:66
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105 a Coding haplotypes were derived from the following six non-synonymous SNPs (left to right): R219K (G.A), V771M (G.A), V825I (G.A), I883M (A.G), E1172D (G.C), and R1587K (G.A).
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ABCA1 p.Arg219Lys 18199144:105:93
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PMID: 18003760 [PubMed] Villarreal-Molina MT et al: "Association of the ATP-binding cassette transporter A1 R230C variant with early-onset type 2 diabetes in a Mexican population."
No. Sentence Comment
87 TABLE 3 Allelic association analyses results of individual SNPs in the ABCA1 gene in case-control samples of the initial study group dbSNP ID Position* ABCA1 region Major/minor allele MAF Allele frequencies P† P‡ Type 2 diabetes Nondiabetic rs2000069 106675690 Intron 5 C/T 0.380 0.372 0.390 0.729 0.999 rs2230806 (R219K) 106660688 Exon 7 G/A 0.327 0.312 0.346 0.311 0.845 rs9282541 (R230C) 106660656 Exon 7 C/T 0.097 0.131 0.056 0.0002 0.001 rs2487037 106657158 Intron 7 C/T 0.261 0.256 0.267 0.585 0.998 rs3818689 106634837 Intron 18 G/C 0.054 0.056 0.052 0.772 0.999 *Position is in contiguous NT_008470.18; †P values for type 2 diabetes with respect to the minor allele; ‡P values after Bonferroni correction for the five different SNPs tested.
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ABCA1 p.Arg219Lys 18003760:87:327
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125 However, SNPs rs2230806 (R219K) and r2487037 were in high LD (r2 >0.8).
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ABCA1 p.Arg219Lys 18003760:125:25
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126 However, SNPs rs2230806 (R219K) and r2487037 were in high LD (r2 >0.8).
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ABCA1 p.Arg219Lys 18003760:126:25
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PMID: 17951323 [PubMed] Frikke-Schmidt R et al: "Genetic variation in ABCA1 predicts ischemic heart disease in the general population."
No. Sentence Comment
7 Two SNPs (V771M and V825I) were previously associated with increases in HDL-C, 1 (R1587K) with decreased HDL-C, whereas 3 (R219K, I883M and E1172D) did not affect HDL-C levels.
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ABCA1 p.Arg219Lys 17951323:7:123
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10 A stepwise regression approach identified V771M, I883M, and E1172D as the most important predictors of IHD and additive effects on IHD risk were present for V771M/I883M and I883M/E1172D pairs.
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ABCA1 p.Arg219Lys 17951323:10:131
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16 In the present study we included 9259 individuals from the 1991 to 1994 examination, whom we genotyped for all nonsynonymous SNPs (R219K, V771M, V825I, I883M, E1172D, R1587K) identified by resequencing ABCA1 in 190 individuals of Danish ancestry.8 Information on diagnosis of IHD (nϭ1170; World Health Organization; International Classification of Diseases, 8th edition: codes 410 to 414; 10th edition: codes I20-I25) was collected and verified until 31st December 2000 by reviewing all hospital admissions and diagnoses entered in the national Danish Patient Registry, all causes of death entered in the national Danish Causes of Death Registry, and medical records from hospitals and general practitioners.
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ABCA1 p.Arg219Lys 17951323:16:131
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29 The cohort was participants in The Copenhagen City Heart Study who attended the 1991 to 1994 examination, and for whom combined genotypes for all 6 nonsynonymous SNPs (R219K, V771M, V825I, I883M, E1172D, R1587K) were available as well as all clinical and biochemical data (nϭ9028 out of nϭ9259; Table 1).
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ABCA1 p.Arg219Lys 17951323:29:168
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38 SNP Genotyping The ABI PRISM 7900HT Sequence Detection System (Applied Biosystem Inc) was used to genotype for all 6 nonsynonymous SNPs (R219K, V771M, V825I, I883M, E1172D, R1587K) identified by resequencing ABCA1 in 190 individuals, as previously described.8 Biochemical Analyses Colorimetric and turbidimetric assays (Hitachi autoanalyzer) were used to measure plasma levels of total cholesterol, HDL-C, triglycerides, and apolipoproteins B and -AI (all Boehringer Mannheim GmbH).
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ABCA1 p.Arg219Lys 17951323:38:137
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55 Frikke-Schmidt et al ABCA1 and Ischemic Heart Disease 181 the entire ABCA1 gene in 190 individuals of Danish descent were: 0.26 (R219K), 0.03 (V771M), 0.03 (E1172D), 0.06 (V825I), 0.12 (I883M), and 0.24 (R1587K).8 Similar allele frequencies have been reported for other White populations.14 Please see Data Supplements, Expanded Results for description of Hardy-Weinberg equilibrium.
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ABCA1 p.Arg219Lys 17951323:55:130
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57 A strong positive DЈ was present for R219K/V771M, M825I/I883M, and E1172D/ R1587K (DЈϾ0.9), whereas a strong negative DЈ was present for R219K/V825I, V771M/V825I, and V771M/I883M (DЈϽ-0.9).
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ABCA1 p.Arg219Lys 17951323:57:43
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ABCA1 p.Arg219Lys 17951323:57:161
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60 Risk of IHD Prospective Study The cumulative incidence of IHD as a function of age was increased for V771M (GAϩAA versus GG, borderline Pϭ0.06), V825I (GAϩAA versus GG; Pϭ0.02), I883M (AGϩGG versus AA, Pϭ0.01), E1172D (GCϩCC versus GG, Pϭ0.03), and for R1587K (AA versus GG, borderline Pϭ0.06), but not for R219K (Figure 2).
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ABCA1 p.Arg219Lys 17951323:60:361
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69 For R219K and R1587K, all 3 genotypes were presented (homozygote in red, heterozygote in black, common genotype in green).
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ABCA1 p.Arg219Lys 17951323:69:4
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82 R1587K was associated with a decrease in HDL-C of 0.03 mmol/L (PϽ0.005), whereas R219K, I883M, and E1172D were not associated with changes in HDL-C levels (Figure 3, upper panel).
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ABCA1 p.Arg219Lys 17951323:82:87
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85 Risk of Ischemic Heart Disease as a Function of ABCA1 Genotype in the Prospective Study n, % Number of Events Incidence Rate (95% CI) per 10 000 Person-Years Hazard Ratio (95% CI) Observed Expected Age Adjusted HDL-C Adjusted Multifactorially Adjusted R219K GG 4863 (54) 603 603 64 (59-70) 1 1 1 GA 3461 (39) 429 426 64 (58-71) 1.0 (0.9-1.1) 1.0 (0.9-1.1) 1.0 (0.9-1.2) AA 641 (7) 75 79 64 (50-80) 1.0 (0.8-1.2) 1.0 (0.8-1.2) 1.0 (0.8-1.3) V771M GG 8379 (93) 1023 1040 64 (60-68) 1 1 1 GAϩAA 586 (7) 84 69 75 (60-93)* 1.2 (1.0-1.5) 1.3 (1.0-1.6) 1.2 (1.0-1.5) M825I GG 7959 (89) 962 988 63 (59-67) 1 1 1 GAϩAA 1006 (11) 145 122 76 (64-89)† 1.2 (1.0-1.5) 1.2 (1.0-1.5) 1.2 (1.0-1.4) I883M AA 6934 (77) 827 864 62 (58-66) 1 1 1 AGϩGG 2031 (23) 280 245 72 (64-81)† 1.2 (1.0-1.4) 1.2 (1.1-1.4) 1.2 (1.1-1.4) E1172D GG 8469 (94) 1026 1045 63 (59-67) 1 1 1 GCϩCC 496 (6) 81 64 86 (68-106)† 1.3 (1.0-1.6) 1.3 (1.0-1.6) 1.3 (1.0-1.6) R1587K GG 5216 (58) 626 645 62 (58-67) 1 1 1 GA 3213 (36) 399 396 65 (58-71) 1.0 (0.9-1.2) 1.0 (0.9-1.2) 1.0 (0.9-1.2) AA 536 (6) 82 68 82 (65-102)* 1.2 (1.0-1.6) 1.2 (1.0-1.5) 1.3 (1.0-1.6) Nonincident cases (nϭ63) were excluded, leaving 8965 individuals for the survival analyses and Cox regression.
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ABCA1 p.Arg219Lys 17951323:85:252
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89 Rs numbers: R219K (rs2230806); V771M (rs2066718); V825I (rs2066715); I883M (rs4149313); E1172D (rs33918808); R1587K (rs2230808).
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ABCA1 p.Arg219Lys 17951323:89:12
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98 The rare allele of the R219K SNP has previously been reported to be associated with decreased14,17 or increased risk of coronary heart disease.18 The present largest prospective results as well as a recent case-control study did not find any association with atherosclerosis susceptibility.19 In support of I883M and E1172D as 2 of the 3 most important ABCA1 SNPs for IHD prediction, a previous study of 2028 White men found increased frequencies in cases compared with controls, and also detected increased risk of future IHD events associated with the 1172D allele.18 The pairwise LD structure of the SNPs is important for the interpretation of the association results.
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ABCA1 p.Arg219Lys 17951323:98:23
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1 Two SNPs (V771M and V825I) were previously associated with increases in HDL-C, 1 (R1587K) with decreased HDL-C, whereas 3 (R219K, I883M and E1172D) did not affect HDL-C levels.
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ABCA1 p.Arg219Lys 17951323:1:123
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23 The cohort was participants in The Copenhagen City Heart Study who attended the 1991 to 1994 examination, and for whom combined genotypes for all 6 nonsynonymous SNPs (R219K, V771M, V825I, I883M, E1172D, R1587K) were available as well as all clinical and biochemical data (nafd;9028 out of nafd;9259; Table 1).
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ABCA1 p.Arg219Lys 17951323:23:168
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32 SNP Genotyping The ABI PRISM 7900HT Sequence Detection System (Applied Biosystem Inc) was used to genotype for all 6 nonsynonymous SNPs (R219K, V771M, V825I, I883M, E1172D, R1587K) identified by resequencing ABCA1 in 190 individuals, as previously described.8 Biochemical Analyses Colorimetric and turbidimetric assays (Hitachi autoanalyzer) were used to measure plasma levels of total cholesterol, HDL-C, triglycerides, and apolipoproteins B and -AI (all Boehringer Mannheim GmbH).
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ABCA1 p.Arg219Lys 17951323:32:137
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49 Frikke-Schmidt et al ABCA1 and Ischemic Heart Disease 181 at Semmelweis University (Egyetem) on December 3, 2015 http://atvb.ahajournals.org/ Downloaded from the entire ABCA1 gene in 190 individuals of Danish descent were: 0.26 (R219K), 0.03 (V771M), 0.03 (E1172D), 0.06 (V825I), 0.12 (I883M), and 0.24 (R1587K).8 Similar allele frequencies have been reported for other White populations.14 Please see Data Supplements, Expanded Results for description of Hardy-Weinberg equilibrium.
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ABCA1 p.Arg219Lys 17951323:49:230
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51 A strong positive Db18; was present for R219K/V771M, M825I/I883M, and E1172D/ R1587K (Db18;b0e;0.9), whereas a strong negative Db18; was present for R219K/V825I, V771M/V825I, and V771M/I883M (Db18;b0d;afa;0.9).
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ABCA1 p.Arg219Lys 17951323:51:43
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ABCA1 p.Arg219Lys 17951323:51:161
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54 Risk of IHD Prospective Study The cumulative incidence of IHD as a function of age was increased for V771M (GAaf9;AA versus GG, borderline Pafd;0.06), V825I (GAaf9;AA versus GG; Pafd;0.02), I883M (AGaf9;GG versus AA, Pafd;0.01), E1172D (GCaf9;CC versus GG, Pafd;0.03), and for R1587K (AA versus GG, borderline Pafd;0.06), but not for R219K (Figure 2).
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ABCA1 p.Arg219Lys 17951323:54:361
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63 For R219K and R1587K, all 3 genotypes were presented (homozygote in red, heterozygote in black, common genotype in green).
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ABCA1 p.Arg219Lys 17951323:63:4
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76 R1587K was associated with a decrease in HDL-C of 0.03 mmol/L (Pb0d;0.005), whereas R219K, I883M, and E1172D were not associated with changes in HDL-C levels (Figure 3, upper panel).
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ABCA1 p.Arg219Lys 17951323:76:87
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79 Risk of Ischemic Heart Disease as a Function of ABCA1 Genotype in the Prospective Study n, % Number of Events Incidence Rate (95% CI) per 10 000 Person-Years Hazard Ratio (95% CI) Observed Expected Age Adjusted HDL-C Adjusted Multifactorially Adjusted R219K GG 4863 (54) 603 603 64 (59-70) 1 1 1 GA 3461 (39) 429 426 64 (58-71) 1.0 (0.9-1.1) 1.0 (0.9-1.1) 1.0 (0.9-1.2) AA 641 (7) 75 79 64 (50-80) 1.0 (0.8-1.2) 1.0 (0.8-1.2) 1.0 (0.8-1.3) V771M GG 8379 (93) 1023 1040 64 (60-68) 1 1 1 GAaf9;AA 586 (7) 84 69 75 (60-93)* 1.2 (1.0-1.5) 1.3 (1.0-1.6) 1.2 (1.0-1.5) M825I GG 7959 (89) 962 988 63 (59-67) 1 1 1 GAaf9;AA 1006 (11) 145 122 76 (64-89)ߤ 1.2 (1.0-1.5) 1.2 (1.0-1.5) 1.2 (1.0-1.4) I883M AA 6934 (77) 827 864 62 (58-66) 1 1 1 AGaf9;GG 2031 (23) 280 245 72 (64-81)ߤ 1.2 (1.0-1.4) 1.2 (1.1-1.4) 1.2 (1.1-1.4) E1172D GG 8469 (94) 1026 1045 63 (59-67) 1 1 1 GCaf9;CC 496 (6) 81 64 86 (68-106)ߤ 1.3 (1.0-1.6) 1.3 (1.0-1.6) 1.3 (1.0-1.6) R1587K GG 5216 (58) 626 645 62 (58-67) 1 1 1 GA 3213 (36) 399 396 65 (58-71) 1.0 (0.9-1.2) 1.0 (0.9-1.2) 1.0 (0.9-1.2) AA 536 (6) 82 68 82 (65-102)* 1.2 (1.0-1.6) 1.2 (1.0-1.5) 1.3 (1.0-1.6) Nonincident cases (nafd;63) were excluded, leaving 8965 individuals for the survival analyses and Cox regression.
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ABCA1 p.Arg219Lys 17951323:79:252
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83 Rs numbers: R219K (rs2230806); V771M (rs2066718); V825I (rs2066715); I883M (rs4149313); E1172D (rs33918808); R1587K (rs2230808).
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ABCA1 p.Arg219Lys 17951323:83:12
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92 The rare allele of the R219K SNP has previously been reported to be associated with decreased14,17 or increased risk of coronary heart disease.18 The present largest prospective results as well as a recent case-control study did not find any association with atherosclerosis susceptibility.19 In support of I883M and E1172D as 2 of the 3 most important ABCA1 SNPs for IHD prediction, a previous study of 2028 White men found increased frequencies in cases compared with controls, and also detected increased risk of future IHD events associated with the 1172D allele.18 The pairwise LD structure of the SNPs is important for the interpretation of the association results.
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ABCA1 p.Arg219Lys 17951323:92:23
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PMID: 17510949 [PubMed] Chu LW et al: "A novel intronic polymorphism of ABCA1 gene reveals risk for sporadic Alzheimer's disease in Chinese."
No. Sentence Comment
133 SNP18 (R219K) is in an N-terminal extracellular loop which possibly mediates ABCA1 interaction with ApoAI; while SNP10 (K1587R) is located in the regulatory segment 2 of the protein [Fitzgerald et al., 2002; Frikke-Schmidt et al., 2004].
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ABCA1 p.Arg219Lys 17510949:133:7
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PMID: 17923263 [PubMed] Kitjaroentham A et al: "R219K polymorphism of ATP binding cassette transporter A1 related with low HDL in overweight/obese Thai males."
No. Sentence Comment
6 The presence of R219K and I883M genetic variant was determined by PCR-RFLP analysis in 112 overweight/obese and 117 control subjects of both sexes.
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ABCA1 p.Arg219Lys 17923263:6:16
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9 Overweight/obese men carrying the mutant allele of R219K had lower level of HDL than the control ( p 5 0.006).
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ABCA1 p.Arg219Lys 17923263:9:51
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15 Although the lower level of HDL in overweight/obese men carrying R219K in comparison to the control suggests the possible involvement of this gene with obesity, further investigations are needed to prove the influence of ABCA1 gene polymorphism on HDL level and to determine whether it could be a genetic determinant of obesity.
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ABCA1 p.Arg219Lys 17923263:15:65
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16 Ó 2007 IMSS. Published by Elsevier Inc. Key Words: ABCA1, Overweight/obese, SNP, Polymorphism, R219K.
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ABCA1 p.Arg219Lys 17923263:16:99
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32 Some of these ABCA1 polymorphisms such as R219K (10) and I883M (9) are associated with increased HDL levels.
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ABCA1 p.Arg219Lys 17923263:32:42
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34 Thus, we studied the prevalence of two frequently occurring common variants of the ABCA1 gene, R219K and I883M polymorphisms, and any association between these two polymorphisms and the lipid profiles of Thai overweight/obese subjects.
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ABCA1 p.Arg219Lys 17923263:34:95
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51 R219K (G1051A) The forward primer was 50 -GTATTT TTG CAA GGC TAC CAG TTA CAT TTG ACA A-30 and the reverse primer was 50 -GAT TGG CTT CAG GAT GTC CAT GTT GGA A-30 .
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ABCA1 p.Arg219Lys 17923263:51:0
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62 Obviously, carrier frequency was high, 60e65% for R219K and almost 90% for I883M.
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ABCA1 p.Arg219Lys 17923263:62:50
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64 To determine whether the presence of the mutant allele of the two variants (K allele for R219K and M allele for I883M) affects the HDL levels of overweight/obese subjects compared with the control, the HDL levels of the obese and control groups were compared according to their genotype, as shown in Table 3.
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ABCA1 p.Arg219Lys 17923263:64:70
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ABCA1 p.Arg219Lys 17923263:64:89
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65 A difference was observed in male subjects carrying the mutant allele R219K.
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ABCA1 p.Arg219Lys 17923263:65:70
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67 Bivariate logistic regression was used to test support for the suggestion that the low HDL levels found in overweight/obese men carrying the mutant R219K allele is the result of ABCA1 gene polymorphism.
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ABCA1 p.Arg219Lys 17923263:67:148
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ABCA1 p.Arg219Lys 17923263:67:190
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68 Table 4 shows the logistic regression and odds ratios for possible association between HDL at cutoff point 35 mg/dL and obesity, cholesterol, triglycerides, LDL, the two ABCA1 polymorphisms-R219K and I883M-and gender.
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ABCA1 p.Arg219Lys 17923263:68:190
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70 Accordingly, most of the overweight and obese men carrying the R219K mutant allele appeared to have HDL !50 mg/dL compared with the control (Figure 1), although they were smaller in number (22 vs. 63).
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ABCA1 p.Arg219Lys 17923263:70:63
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ABCA1 p.Arg219Lys 17923263:70:80
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71 Triglyceride was another parameter found to be higher in obese men carrying the R219K mutant allele.
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ABCA1 p.Arg219Lys 17923263:71:80
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77 Our result was 61.61% in overweight/obese and 66.67% for R219K; for I883M, it was 87.5% and 90.18% for overweight/obese and control, respectively.
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ABCA1 p.Arg219Lys 17923263:77:57
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79 However, this agrees with our result because the carrier frequency of R219K in Japanese is 74.6% (12).
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ABCA1 p.Arg219Lys 17923263:79:70
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ABCA1 p.Arg219Lys 17923263:79:105
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80 Both polymorphisms appear to be more common among populations of Asian ethnicity than Westerners because R219K carrier frequency in Europeans is 46% (10).
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ABCA1 p.Arg219Lys 17923263:80:105
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90 Frequency of the two ABCA1 SNPs-R219K and I883M-in overweight/obese and control subjects ABCA1 genotype Overweight/obese n (%) Control n (%) Odds ratio (95% CI) p value* R219K n 5 112 n 5 117 219RR 43 39 0.800 0.422 219RK þ KK 57þ12 (61.61%) 65þ13 (66.67%) (0.450e1.430) I883M n 5 112 n 5 112 883II 14 11 0.760 883IM þ MM 47þ51 (87.50%) 57þ44 (90.18%) (0.310e1.890) 0.520 *p value 0.05 or less was considered statistically significant.
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ABCA1 p.Arg219Lys 17923263:90:32
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ABCA1 p.Arg219Lys 17923263:90:170
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92 Although several reports have confirmed that the K allele of R219K is associated with a slightly higher HDL concentration (10,15), this is not consistent with our finding in overweight/obese subjects.
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ABCA1 p.Arg219Lys 17923263:92:34
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ABCA1 p.Arg219Lys 17923263:92:61
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93 The overweight/obese men carrying R219K had significantly lower HDL concentrations than their controls, although a small number of individuals was tested.
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ABCA1 p.Arg219Lys 17923263:93:34
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101 Lipid profiles of noncarriers and carriers of the K allele of the R219K polymorphism in overweight/obese and control subjects by gender Genotype RR RK þ KK Obese Control p value* Obese Control p value* Men n 5 18 n 5 33 n 5 22 n 5 63 Cholesterol 211.00 203.00 0.937 220.50 202.00 0.177 (103.00e374.00) (127.00e284.00) (136.00e276.00) (129.00e279.00) HDL 50.50 44.00 0.206 45.00 50.00 0.006* (31.00e64.00) (28.00e64.00) (33.00e69.00) (33.00e86.00) LDL 133.90 138.20 0.460 129.00 117.40 0.748 (26.00e291.00) (55.00e210.00) (75.00e193.00) (50.00e205.00) Triglycerides 137.50 138.00 0.261 188.50 118.00 0.000 (62.00e269.00) (47.00e269.00) (71.00e342.00) (35.00e327.00) Women n 5 25 n 5 6 n 5 47 n 5 15 Cholesterol 211.00 182.00 0.937 223.00 212.00 0.406 (139.00e427.00) (159.00e352.00) (136.00e388.00) (167.00e319.00) HDL 51.00 59.50 0.423 50.00 43.00 0.097 (29.00e78.00) (27.00e71.00) (34.00e79.00) (31.00e61.00) LDL 138.80 119.60 0.726 145.00 139.00 0.824 (44.00e359.00) (85.00e259.00) (50.00e284.00) (107.00e236.00) Triglycerides 133.00 110.50 0.516 117.00 88.00 0.565 (48.00e351.00) (45.00e307.00) (48.00e397.00) (50.00e355.00) *Mann-Whitney U Test (two-tailed).
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ABCA1 p.Arg219Lys 17923263:101:66
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104 Logistic regression results for relationship between HDL at cutoff point 35 mg/dL and obesity, cholesterol, triglycerides, LDL, ABCA1 polymorphisms at R219K and I883M, and gender Variables Odds ratio 95% CI p value* Obesity 0.365 0.027e4.971 0.449 Cholesterol 2.775 1.502e5.129 0.001 Triglycerides 0.817 0.724e0.920 0.001 LDL 0.358 0.192e0.665 0.001 R219K 0.824 0.089e7.622 0.864 I883M 0.634 0.027e14.942 0.777 Gender 1.816 0.173e19.111 0.619 *p value 0.05 or less was considered statistically significant.
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ABCA1 p.Arg219Lys 17923263:104:151
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ABCA1 p.Arg219Lys 17923263:104:350
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112 In conclusion, our study showed that the R219K variant allele was associated with low levels of HDL in Thai overweight/obese men compared with their controls.
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ABCA1 p.Arg219Lys 17923263:112:41
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31 Some of these ABCA1 polymorphisms such as R219K (10) and I883M (9) are associated with increased HDL levels.
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ABCA1 p.Arg219Lys 17923263:31:42
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33 Thus, we studied the prevalence of two frequently occurring common variants of the ABCA1 gene, R219K and I883M polymorphisms, and any association between these two polymorphisms and the lipid profiles of Thai overweight/obese subjects.
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ABCA1 p.Arg219Lys 17923263:33:95
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50 R219K (G1051A) The forward primer was 50 -GTATTT TTG CAA GGC TAC CAG TTA CAT TTG ACA A-30 and the reverse primer was 50 -GAT TGG CTT CAG GAT GTC CAT GTT GGA A-30 .
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ABCA1 p.Arg219Lys 17923263:50:0
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61 Obviously, carrier frequency was high, 60e65% for R219K and almost 90% for I883M.
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ABCA1 p.Arg219Lys 17923263:61:50
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63 To determine whether the presence of the mutant allele of the two variants (K allele for R219K and M allele for I883M) affects the HDL levels of overweight/obese subjects compared with the control, the HDL levels of the obese and control groups were compared according to their genotype, as shown in Table 3.
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ABCA1 p.Arg219Lys 17923263:63:89
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66 Bivariate logistic regression was used to test support for the suggestion that the low HDL levels found in overweight/obese men carrying the mutant R219K allele is the result of ABCA1 gene polymorphism.
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ABCA1 p.Arg219Lys 17923263:66:148
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69 Accordingly, most of the overweight and obese men carrying the R219K mutant allele appeared to have HDL !50 mg/dL compared with the control (Figure 1), although they were smaller in number (22 vs. 63).
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ABCA1 p.Arg219Lys 17923263:69:63
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76 Our result was 61.61% in overweight/obese and 66.67% for R219K; for I883M, it was 87.5% and 90.18% for overweight/obese and control, respectively.
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ABCA1 p.Arg219Lys 17923263:76:57
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78 However, this agrees with our result because the carrier frequency of R219K in Japanese is 74.6% (12).
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ABCA1 p.Arg219Lys 17923263:78:70
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89 Frequency of the two ABCA1 SNPs-R219K and I883M-in overweight/obese and control subjects ABCA1 genotype Overweight/obese n (%) Control n (%) Odds ratio (95% CI) p value* R219K n 5 112 n 5 117 219RR 43 39 0.800 0.422 219RK &#fe; KK 57&#fe;12 (61.61%) 65&#fe;13 (66.67%) (0.450e1.430) I883M n 5 112 n 5 112 883II 14 11 0.760 883IM &#fe; MM 47&#fe;51 (87.50%) 57&#fe;44 (90.18%) (0.310e1.890) 0.520 *p value 0.05 or less was considered statistically significant.
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ABCA1 p.Arg219Lys 17923263:89:32
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ABCA1 p.Arg219Lys 17923263:89:170
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91 Although several reports have confirmed that the K allele of R219K is associated with a slightly higher HDL concentration (10,15), this is not consistent with our finding in overweight/obese subjects.
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ABCA1 p.Arg219Lys 17923263:91:61
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100 Lipid profiles of noncarriers and carriers of the K allele of the R219K polymorphism in overweight/obese and control subjects by gender Genotype RR RK &#fe; KK Obese Control p value* Obese Control p value* Men n 5 18 n 5 33 n 5 22 n 5 63 Cholesterol 211.00 203.00 0.937 220.50 202.00 0.177 (103.00e374.00) (127.00e284.00) (136.00e276.00) (129.00e279.00) HDL 50.50 44.00 0.206 45.00 50.00 0.006* (31.00e64.00) (28.00e64.00) (33.00e69.00) (33.00e86.00) LDL 133.90 138.20 0.460 129.00 117.40 0.748 (26.00e291.00) (55.00e210.00) (75.00e193.00) (50.00e205.00) Triglycerides 137.50 138.00 0.261 188.50 118.00 0.000 (62.00e269.00) (47.00e269.00) (71.00e342.00) (35.00e327.00) Women n 5 25 n 5 6 n 5 47 n 5 15 Cholesterol 211.00 182.00 0.937 223.00 212.00 0.406 (139.00e427.00) (159.00e352.00) (136.00e388.00) (167.00e319.00) HDL 51.00 59.50 0.423 50.00 43.00 0.097 (29.00e78.00) (27.00e71.00) (34.00e79.00) (31.00e61.00) LDL 138.80 119.60 0.726 145.00 139.00 0.824 (44.00e359.00) (85.00e259.00) (50.00e284.00) (107.00e236.00) Triglycerides 133.00 110.50 0.516 117.00 88.00 0.565 (48.00e351.00) (45.00e307.00) (48.00e397.00) (50.00e355.00) *Mann-Whitney U Test (two-tailed).
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ABCA1 p.Arg219Lys 17923263:100:66
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103 Logistic regression results for relationship between HDL at cutoff point 35 mg/dL and obesity, cholesterol, triglycerides, LDL, ABCA1 polymorphisms at R219K and I883M, and gender Variables Odds ratio 95% CI p value* Obesity 0.365 0.027e4.971 0.449 Cholesterol 2.775 1.502e5.129 0.001 Triglycerides 0.817 0.724e0.920 0.001 LDL 0.358 0.192e0.665 0.001 R219K 0.824 0.089e7.622 0.864 I883M 0.634 0.027e14.942 0.777 Gender 1.816 0.173e19.111 0.619 *p value 0.05 or less was considered statistically significant.
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ABCA1 p.Arg219Lys 17923263:103:151
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111 In conclusion, our study showed that the R219K variant allele was associated with low levels of HDL in Thai overweight/obese men compared with their controls.
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ABCA1 p.Arg219Lys 17923263:111:41
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PMID: 17368464 [PubMed] Jensen MK et al: "Common genetic variation in the ATP-binding cassette transporter A1, plasma lipids, and risk of coronary heart disease."
No. Sentence Comment
23 Only the R1587K and the -565C/T promoter variant were found associated with apolipoprotein AI levels, the R219K SNP was associated with risk of myocardial infarction, and none of the 16 identified promoter SNPs were significantly associated with risk [7].
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ABCA1 p.Arg219Lys 17368464:23:106
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166 Moreover, we did not have information on the R219K SNP that has consistently been associated with lower CHD risk previously [7-9].
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ABCA1 p.Arg219Lys 17368464:166:45
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PMID: 17510946 [PubMed] Rodriguez-Rodriguez E et al: "Association of genetic variants of ABCA1 with Alzheimer's disease risk."
No. Sentence Comment
1 To evaluate the relationship between ABCA1 genetic variants and Alzheimer`s disease (AD), independently or in concert with the APOE e4 allele, we examined three ABCA1 polymorphisms located in the coding region (R219K, I883M, and R1587K) and two ABCA1 polymorphisms in the promoter region (CÀ14T and CÀ477T) in a group of 372 Spanish AD patients and 440 controls.
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ABCA1 p.Arg219Lys 17510946:1:211
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16 We focused on the ABCA1 I883M, R1587K, and R219K variants in the coding region since these give rise to amino acid changes [Singaraja et al., 2003], they are common in European populations [Singaraja et al., 2003], and have been reported to alter the susceptibility to AD [Katzov et al., 2004; Sundar et al., 2006]; in addition, we examined two potentially functional polymorphisms (CÀ14T and CÀ477T) in the promoter region of ABCA1 gene [Hodoglugil et al., 2005; Kyriakou et al., 2005].
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ABCA1 p.Arg219Lys 17510946:16:43
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35 Genotyping of ABCA1 I883M (rs 4149313), ABCA1 R1587K (rs 2230808), ABCA1 R219K (rs 2230806), ABCA1 CÀ14T (rs 1800977), and ABCA1 CÀ477T (rs 2422493) polymorphisms was performed by a Taq-Man single-nucleotide-polymorphism assay (Applied Biosystems, Warrington, Cheshire, UK) and an ABI PRISM 7000 sequence detection system (Applied Biosystems).
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ABCA1 p.Arg219Lys 17510946:35:73
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43 RESULTS Control groups for ABCA1 I883M (P ¼ 0.16), ABCA1 R1587K (P ¼ 0.47), ABCA1 R219K (P ¼ 0.29), ABCA1 CÀ14T (P ¼ 0.46), and ABCA1 CÀ477T (P ¼ 0.70) polymorphisms were within the range of Hardy-Weinberg equilibrium; the same occurred in case groups for ABCA1 I883M (P ¼ 0.74), ABCA1 R1587K (P ¼ 0.29), ABCA1 R219K (P ¼ 0.82), ABCA1 CÀ14T (P ¼ 0.82), and ABCA1 CÀ477T (P ¼ 0.26).
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ABCA1 p.Arg219Lys 17510946:43:92
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ABCA1 p.Arg219Lys 17510946:43:356
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44 As shown in Table I, the distribution of the allele and genotype frequencies of the ABCA1 polymorphisms did not differ significantly between AD and control groups, except for ABCA1 R219K: when compared to 219RR genotype, the 219RK and KK genotypes were associated with AD (age, sex and APOE e4 status-adjusted OR ¼ 1.50; 95% CI ¼ 1.10-2.04; P ¼ 0.009).
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ABCA1 p.Arg219Lys 17510946:44:181
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49 ABCA1 polymorphisms in the coding region were in linkage disequilibrium (LD): I883M and R1587K, D0 ¼ 0.2071, P ¼ 0.033; I883M and R219K, D0 ¼ 0.2616, P < 0.001; R1587K and R219K, D0 ¼ 0.2343, P < 0.001.
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ABCA1 p.Arg219Lys 17510946:49:140
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ABCA1 p.Arg219Lys 17510946:49:187
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62 We performed a meta-analysis for ABCA1 R219K polymorphism, and we pooled 10 case-control series [Wollmer et al., 2003; Katzov et al., 2004; Li et al., 2004; Ko¨lsch et al., 2006; Sundar et al., 2006] including the present study; the combined total of 3,162 patients and 2,725 controls from these studies were included in the meta-analysis, and using a random-effects model, the pooled OR (estimated by Der Simonian-Laird method) for AD associated with ABCA1 219RK and KK genotypes was 1.07 (95% CI ¼ 0.95-1.20), showing no association with AD risk.
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ABCA1 p.Arg219Lys 17510946:62:39
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67 Distribution of ABCA1 Polymorphisms in Patients and Controls Stratified by APOE e4 Allele Polymorphism APOE e4 allele carriers APOE e4 allele noncarriers Total sample Patients Controls Patients Controls Patients Controls I883M II 121 (0.63) 47 (0.59) 117 (0.65) 237 (0.66) 238 (0.64) 284 (0.65) IM 64 (0.34) 33 (0.41) 57 (0.31) 110 (0.31) 121 (0.33) 143 (0.33) MM 6 (0.03) 0 (0.00) 7 (0.04) 11 (0.03) 13 (0.03) 11 (0.02) Total 191 80 181 358 372 438 Allele frequency I/M 0.80/0.20 0.79/0.21 0.80/0.20 0.82/0.18 0.80/0.20 0.81/0.19 R1587K RR 109 (0.58) 44 (0.57) 110 (0.63) 228 (0.65) 219 (0.60) 272 (0.64) RK 72 (0.38) 30 (0.39) 62 (0.35) 109 (0.31) 134 (0.36) 139 (0.32) KK 8 (0.04) 3 (0.04) 6 (0.02) 17 (0.04) 14 (0.04) 20 (0.04) Total 189 77 178 354 367 431 Allele frequency R/K 0.77/0.23 0.77/0.23 0.79/0.21 0.80/0.20 0.78/0.22 0.79/0.21 R219K RR 83 (0.43) 40 (0.51) 82 (0.45) 192 (0.54) 165 (0.44) 232 (0.53) RK 82 (0.43) 30 (0.38) 85(0.48) 136 (0.38) 167 (0.45) 166 (0.38) KK 26 (0.14) 9(0.11) 13 (0.07) 29 (0.08) 39 (0.11) 38 (0.09) Total 191 79 180 357 371 436 Allele frequency R/K 0.65/0.35 0.70/0.30 0.69/0.31 0.73/0.27 0.67/0.33 0.72/0.28 CÀ14T CC 81 (0.42) 34 (0.42) 67 (0.37) 147 (0.42) 148 (0.40) 181 (0.42) CT 79 (0.41) 42 (0.53) 96 (0.53) 161 (0.46) 175 (0.47) 203 (0.47) TT 31 (0.17) 4 (0.05) 18 (0.10) 44 (0.12) 49 (0.13) 48 (0.11) Total 191 80 181 352 372 432 Allele frequency C/T 0.63/0.37 0.69/0.31 0.64/0.36 0.65/0.35 0.63/0.37 0.65/0.35 CÀ477T CC 50 (0.26) 19 (0.24) 43 (0.24) 103 (0.29) 93 (0.25) 122 (0.28) CT 88 (0.46) 47 (0.59) 87 (0.48) 177 (0.49) 175 (0.47) 224 (0.51) TT 53 (0.28) 14 (0.17) 51 (0.28) 80 (0.22) 104 (0.28) 94 (0.21) Total 191 80 181 360 372 440 Allele frequency C/T 0.49/0.51 0.53/0.47 0.48/0.52 0.53/0.47 0.49/0.51 0.53/0.47 Figures in parentheses indicate frequencies; P > 0.05 for all comparisons except 219 RK and KK genotypes versus RR: age, sex and APOE e4 status-adjusted OR ¼ 1.50 (95% CI ¼ 1.10-2.04; P ¼ 0.009).
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ABCA1 p.Arg219Lys 17510946:67:842
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76 Similarly, in a family-based association study using a set of Caribbean Hispanics, a possible interaction was found between ABCA1 R1587K and R219K polymorphisms and APOE [Shibata et al., 2006].
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ABCA1 p.Arg219Lys 17510946:76:141
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81 Distribution of ABCA1 Polymorphisms in Patients and Controls Stratified by Age Groups Polymorphism 72 yearsa >72 yearsa Patients Controls Patients Controls I883M II 123 (0.68) 47 (0.69) 115 (0.61) 237 (0.64) IM 52 (0.28) 18 (0.27) 69 (0.36) 125 (0.34) MM 7 (0.04) 3 (0.04) 6 (0.03) 8 (0.02) Total 182 68 190 370 Allele frequency I/M 0.82/0.18 0.82/0.18 0.79/0.21 0.81/0.19 R1587K RR 101 (0.57) 44 (0.65) 118 (0.63) 228 (0.63) RK 69 (0.39) 21 (0.31) 65 (0.34) 118 (0.32) KK 8 (0.04) 3 (0.04) 6 (0.03) 19 (0.05) Total 178 68 189 365 Allele frequency R/K 0.76/0.24 0.80/0.20 0.80/0.20 0.79/0.21 R219K RR 86 (0.47) 41 (0.60) 79 (0.42) 191 (0.52) RK 74 (0.41) 23 (0.34) 93 (0.49) 143 (0.39) KK 21 (0.12) 4 (0.06) 18 (0.09) 34 (0.09) Total 181 68 190 368 Allele frequency R/K 0.68/0.32 0.77/0.23 0.66/0.34 0.71/0.29 CÀ14T CC 65 (0.36) 31 (0.48) 83 (0.44) 150 (0.41) CT 96 (0.53) 28 (0.43) 79 (0.41) 175 (0.47) TT 21 (0.11) 6 (0.09) 28 (0.15) 43 (0.12) Total 182 65 190 368 Allele frequency C/T 0.62/0.38 0.69/0.31 0.64/0.36 0.65/0.35 CÀ477T CC 42 (0.23) 22 (0.32) 51 (0.27) 100 (0.27) CT 90 (0.49) 33 (0.49) 85 (0.45) 191 (0.51) TT 50 (0.28) 13 (0.19) 54 (0.28) 81 (0.22) Total 182 68 190 372 Allele frequency C/T 0.48/0.52 0.57/0.43 0.49/0.51 0.53/0.47 a Median age at AD onset (72 years) was set as cut-off; figures in parentheses indicate frequencies; P > 0.05 for all comparisons except 219 RK and KK genotypes versus RR: age, sex and APOE (4 status-adjusted OR ¼ 1.90 (95% CI ¼ 0.99-3.64; P ¼ 0.05) in the 72 years subgroup, and adjusted OR ¼ 1.51 (95% CI ¼ 1.02-2.23; P ¼ 0.04) in the >72 years subgroup.
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ABCA1 p.Arg219Lys 17510946:81:592
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83 Odds Ratios for Alzheimer`s Disease Risk According to the Haplotype Frequencies of the ABCA1 Gene Coding Region Polymorphisms Among Patients and Controls R219K I883M R1587K Frequency in AD patients (n ¼ 369) Frequency in controls (n ¼ 435) ORa (95% CI) P* R I R 0.4794 0.5218 1 (reference) K I R 0.1402 0.1100 1.78 (1.17-2.70) 0.0073 R I K 0.0939 0.0995 0.83 (0.52-1.33) 0.43 K I K 0.0887 0.0808 1.27 (0.79-2.05) 0.31 R M R 0.0743 0.0869 0.92 (0.52-1.62) 0.78 K M R 0.0859 0.0701 1.49 (0.92-2.41) 0.11 R M K 0.0238 0.0147 4.85 (0.83-28.49) 0.081 K M K 0.0139 0.0163 1.13 (0.24-5.26) 0.88 a Odds ratios adjusting by age, sex and APOE genotype.
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ABCA1 p.Arg219Lys 17510946:83:154
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PMID: 17070530 [PubMed] Nebel A et al: "Common coding polymorphisms in the ABCA1 gene and risk of early-onset coronary heart disease in northern Germany."
No. Sentence Comment
7 In the present study, we have examined the potential association between the five known coding polymorphisms R219K, V771M, I883M, E1172D and R1587K in the ABCA1 gene and early-onset CHD in a large ethnically homogeneous sample from the northernmost province in Germany.
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ABCA1 p.Arg219Lys 17070530:7:109
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21 Marker R219K showed marginal association (P = 0.066).
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ABCA1 p.Arg219Lys 17070530:21:7
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25 We examined the five known ABCA1 polymorphisms R219K, V771M, I883M, E1172D and R1587K in early-onset 0021-9150/$ - see front matter (c) 2006 Elsevier Ireland Ltd.
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ABCA1 p.Arg219Lys 17070530:25:47
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27 doi:10.1016/j.atherosclerosis.2006.09.022 Letter to the Editor / Atherosclerosis 193 (2007) 458-460 Table 1 Summary association statistics for common ABCA1 coding SNPs in German CHD patients and controls ABCA1 variant MAFa CHD MAFa control Pallele Pgenotype Pcarrier b ORcarrier c 95% CIcarrier d R219K (rs2230806)e 0.265 0.258 0.656 0.582 0.438 1.08 0.89-1.30 V771M (rs2066718)e 0.026 0.034 0.188 0.255 0.222 0.78 0.53-1.16 I883M (rs4149313)e 0.138 0.112 0.023 0.068 0.021 1.31 1.04-1.64 E1172D (hCV25924149)e 0.025 0.025 0.914 0.714 0.983 1.00 0.65-1.55 R1587K (rs2230808)e 0.261 0.234 0.067 0.197 0.097 1.18 0.97-1.42 a MAF, minor allele frequency.
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ABCA1 p.Arg219Lys 17070530:27:299
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31 e R219K, V771M, I883M, E1172D and R1587K were typed using TaqMan® SNP Assays (Applied Biosystems, Foster City, USA).
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ABCA1 p.Arg219Lys 17070530:31:2
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36 However, additional studies have indicated no relevant effects for the I883M genotype on CHD or HDH-C levels [8,10,11].
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ABCA1 p.Arg219Lys 17070530:36:20
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37 The other four SNPs R219K, V771M, E1172D and R1587K exhibited no clear effects in the German CHD samples investigated here.
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ABCA1 p.Arg219Lys 17070530:37:20
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46 Table 2 Logistic regression analysis for five coding SNPs in the ABCA1 gene in German CHD patients and controls Predictora ORb 95% CIc P Gender 1.05 0.81-1.36 0.721 R219K 1.20 0.99-1.47 0.066 V771M 0.90 0.57-1.41 0.645 I883M 1.28 1.02-1.61 0.034 E1172D 0.78 0.52-1.19 0.253 R1587K 1.10 0.90-1.34 0.361 a Each marker binary classified for carriership of rare allele, gender was included as a predictive variable, logistic regression analysis was performed with the R-package [14].
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ABCA1 p.Arg219Lys 17070530:46:165
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26 doi:10.1016/j.atherosclerosis.2006.09.022 Letter to the Editor / Atherosclerosis 193 (2007) 458-460 Table 1 Summary association statistics for common ABCA1 coding SNPs in German CHD patients and controls ABCA1 variant MAFa CHD MAFa control Pallele Pgenotype Pcarrier b ORcarrier c 95% CIcarrier d R219K (rs2230806)e 0.265 0.258 0.656 0.582 0.438 1.08 0.89-1.30 V771M (rs2066718)e 0.026 0.034 0.188 0.255 0.222 0.78 0.53-1.16 I883M (rs4149313)e 0.138 0.112 0.023 0.068 0.021 1.31 1.04-1.64 E1172D (hCV25924149)e 0.025 0.025 0.914 0.714 0.983 1.00 0.65-1.55 R1587K (rs2230808)e 0.261 0.234 0.067 0.197 0.097 1.18 0.97-1.42 a MAF, minor allele frequency.
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ABCA1 p.Arg219Lys 17070530:26:299
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30 e R219K, V771M, I883M, E1172D and R1587K were typed using TaqMan&#ae; SNP Assays (Applied Biosystems, Foster City, USA).
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ABCA1 p.Arg219Lys 17070530:30:2
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45 Table 2 Logistic regression analysis for five coding SNPs in the ABCA1 gene in German CHD patients and controls Predictora ORb 95% CIc P Gender 1.05 0.81-1.36 0.721 R219K 1.20 0.99-1.47 0.066 V771M 0.90 0.57-1.41 0.645 I883M 1.28 1.02-1.61 0.034 E1172D 0.78 0.52-1.19 0.253 R1587K 1.10 0.90-1.34 0.361 a Each marker binary classified for carriership of rare allele, gender was included as a predictive variable, logistic regression analysis was performed with the R-package [14].
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ABCA1 p.Arg219Lys 17070530:45:165
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PMID: 16879828 [PubMed] Benton JL et al: "Associations between two common polymorphisms in the ABCA1 gene and subclinical atherosclerosis: Multi-Ethnic Study of Atherosclerosis (MESA)."
No. Sentence Comment
0 Atherosclerosis 193 (2007) 352-360 Associations between two common polymorphisms in the ABCA1 gene and subclinical atherosclerosis: Multi-Ethnic Study of Atherosclerosis (MESA) Jeana L. Bentonb, Jingzhong Dingi, Michael Y. Tsaid, Steven Sheae,f, Jerome I. Rotterg, Gregory L. Burkeh, Wendy Posta,c,* a Division of Cardiology, Department of Medicine, The Johns Hopkins University School of Medicine, Blalock 910H, 600 N. Wolfe Street, Baltimore, MD 21287, United States b The Johns Hopkins University School of Medicine, Baltimore, MD, United States c Department of Epidemiology, The Johns Hopkins University Bloomberg School of Public Health, Baltimore, MD, United States d Department of Laboratory Medicine and Pathology, University of Minnesota Medical School, Minneapolis, MN, United States e Department of Medicine, Columbia University, New York, NY, United States f Department of Epidemiology, Columbia University, New York, NY, United States g Medical Genetics Institute, Cedars-Sinai Medical Center, Los Angeles, CA, United States h Department of Public Health Sciences, Wake Forest University, Winston-Salem, NC, United States i Department of Internal Medicine/Geriatrics, Wake Forest University, Winston-Salem, NC, United States Received 15 February 2006; received in revised form 9 May 2006; accepted 9 June 2006 Available online 1 August 2006 Abstract Objective: ABCA1 controls the first step in reverse cholesterol transport. The potential associations between G1051A (R219K) and -565C/T genetic polymorphisms in the ABCA1 gene, high-density lipoprotein cholesterol (HDL-C) and subclinical cardiovascular disease in the general population remains unclear.
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ABCA1 p.Arg219Lys 16879828:0:1481
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24 Two common SNPs are G1051A (R219K, rs2230806) and -565C/T (previously designated as -477, rs2422493).
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ABCA1 p.Arg219Lys 16879828:24:28
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88 G1051A (R219K) Demographic characteristics, laboratory values and subclinical disease measures for subjects stratified by G1051A genotype are presented in Table 3.
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ABCA1 p.Arg219Lys 16879828:88:8
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25 Two common SNPs are G1051A (R219K, rs2230806) and -565C/T (previously designated as -477, rs2422493).
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ABCA1 p.Arg219Lys 16879828:25:28
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89 G1051A (R219K) Demographic characteristics, laboratory values and subclinical disease measures for subjects stratified by G1051A genotype are presented in Table 3.
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ABCA1 p.Arg219Lys 16879828:89:8
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PMID: 17556888 [PubMed] Klos KL et al: "Genetic determinants of HDL: monogenic disorders and contributions to variation."
No. Sentence Comment
64 Increased HDL-C in rare allele carriers of the ABCA1 R219K polymorphism have now been reported for several samples of European extraction [28,29 ] and most recently in the Multi-Ethnic Study of Atherosclerosis (MESA) [30 ].
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ABCA1 p.Arg219Lys 17556888:64:53
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65 For other samples, a lack of association between HDL-C and R219K has been reported (e.g. [31,32 ]).
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ABCA1 p.Arg219Lys 17556888:65:59
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66 Interestingly, haplotype analysis in a sample of healthy Pakistani people revealed that the effect of a V825L polymorphism in ABCA1 on HDL-C was dependent on allelic state at R219K [32 ] and, in Turkish people, an effect of R219K on HDL-C was only seen when in combination with the I883M polymorphism [33].
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ABCA1 p.Arg219Lys 17556888:66:175
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ABCA1 p.Arg219Lys 17556888:66:225
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81 Sequence analyses, most notably of the ABCA1 region, suggest that both common variants and rare mutations contribute to interindividual variation in Genetic determinants of HDL Klos and Kullo 347 Table1Commonpolymorphisms(minorallelefrequency>5%)reportedtobeassociatedwithplasmaHDL-Cinmorethanonestudy;thereporteddirectionofeffectoftheless commonallele,andtheircontributionstocovariate-adjustedHDL-Cvariationaloneandincombinationwithotherpolymorphismsofthesamegene GenesymbolGenenamePolymorphismEffecta Single-sitevariationMultisitevariation ABCA1ATP-bindingcassette,sub-familyA (ABC1),member1 596G>A"HDL-C[52,53]4%[52] R219K"HDL-C[28,29 ,30 ]6%[54] V771M"HDL-C[30 ,33] V825I/V825L"HDL-C[30 ];#HDL-C[32 ] APOA5ApolipoproteinA-VÀ1131T>C#HDL-C[55-57] APOC3ApolipoproteinC-III482C>T#HDL-C[55,58 ]0.2-1.4%[58 ]1-6%[58 ,59] SstIS2allelewith#HDL-C[60,61] APOEApolipoproteinEÀ219G>T#HDL-C[27 ,62] e2/e3/e40.8-6.5%[63,64 ]8.3-15.3%[65] ARAndrogenreceptorEx1CAGrepeat"HDL-Cwithlength[66] CETPCholesterol-estertransferproteinÀ1946VNTR"HDL-Cwiththeshortallele[36,67] À629C>A"HDL-C[36,38,39,67-69]4.6-5.2%[39,64 ]5.5-9.8%[39,68] Taq1B"HDL-C[35]3.9%[39]5.5-15%[39,54] MspIin8#HDL-C[36,67] A373P/R451Q#HDL-C[67,68]8%[70] I405V"HDL-C[35] LIPCHepaticlipaseÀ514C>T"HDL-C[45]Upto31%[54] À250G>A"HDL-C[41,43]4.7%[67] LIPGEndotheliallipaseT111I"HDL-C[72,73 ];#HDL-C[74] LPLLipoproteinlipaseHindIII#HDL-CwiththeHþallele[49,75] N291S#HDL-C[50 ] S447X"HDL-C[48,75]0.8%[64 ]3%[35] PON1Paraoxonase1À107T>C"HDL-C[76-78] Q192R"HDL-C[77,79 ];#HDL-C[79 ] PPARDPeroxisomeproliferatorsactivatedreceptordelta294T>C#HDL-C[80] PPARGPeroxisomeproliferatorsactivatedreceptorgammaPro12Ala"HDL-C[81,82] SCARB1ScavengerreceptorclassB,member1A350A"HDL-C[64 ,83]1.3%[64 ] IVS5/A350A(/IVS10)haplotype#HDL-C[84 ] a Citationsrepresentaselectionofavailablestudiesprioritizedbasedonmeta-analysesofassociationresultsinnumerousstudygroups,andrecentstudiescontainingcomprehensivereviewsofpreviously reportedassociations.
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ABCA1 p.Arg219Lys 17556888:81:623
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PMID: 17412755 [PubMed] Kyriakou T et al: "Functional polymorphism in ABCA1 influences age of symptom onset in coronary artery disease patients."
No. Sentence Comment
74 Coefficients (D 0 ) of pair-wise linkage disequilibrium between ABCA1 SNPs 21801 21652 21506 21395 21252 21217 21034 2940 2803 2565 2407 2302 2278 299 214 R219K V825I I883M 21652A.G 20.97 Ã 21506G.C 20.97 Ã 20.86 Ã 21395C.T 0.94 Ã 20.94 Ã 20.91 Ã 21252G.A 20.90 Ã 0.89 Ã 20.64 † 20.95 Ã 21217C.T 21.00 Ã 0.96 Ã 20.94 Ã 20.97 Ã 20.91 † 21034ATins/del 20.91 Ã 20.90 Ã 0.89 Ã 20.94 Ã 20.80 Ã 20.94 Ã 2940T.G 20.95 Ã 0.40 Ã 0.90 Ã 20.95 Ã 20.79 Ã 0.96 Ã 0.84 Ã 2803G.A 0.93 Ã 20.91 Ã 20.95 Ã 0.96 Ã 20.83 † 21.00 Ã 20.95 Ã 20.98 Ã 2565C.T 20.95 Ã 20.42 Ã 0.71 Ã 20.97 Ã 20.81 Ã 1.00 Ã 0.74 Ã 0.92 Ã 20.98 Ã 2407G.C 20.87 Ã 0.39 Ã 0.71 Ã 20.86 Ã 20.74 Ã 0.88 Ã 0.73 Ã 0.86 Ã 20.95 Ã 0.92 Ã 2302C.T 20.85 Ã 20.90 Ã 0.87 Ã 20.88 Ã 20.77 Ã 20.87 Ã 0.90 Ã 0.84 Ã 20.89 Ã 0.94 Ã 0.98 Ã 2278G.C 20.94 Ã 0.41 Ã 0.72 Ã 20.94 Ã 20.83 Ã 0.96 Ã 0.77 Ã 0.93 Ã 20.98 Ã 0.99 Ã 0.91 Ã 0.92 Ã 299G.C 0.79 Ã 20.81 Ã 20.84 Ã 0.82 Ã 20.96 Ã 20.88 Ã 20.80 Ã 20.82 Ã 20.96 Ã 20.85 Ã 20.75 Ã 20.88 Ã 20.85 Ã 214C.T 20.93 Ã 0.10 † 0.78 Ã 20.94 Ã 20.81 Ã 20.89 Ã 0.77 Ã 0.91 Ã 21.00 Ã 0.98 Ã 0.90 Ã 0.84 Ã 0.98 Ã 20.86 Ã R219K 0.14 † 20.17 † 20.18 ‡ 0.14 † 20.62 Ã 0.01 ‡ 20.16 ‡ 0.00 ‡ 0.09 ‡ 20.11 † 0.10 ‡ 20.17 ‡ 0.11 ‡ 0.04 ‡ 0.05 ‡ V825I 20.03 ‡ 20.39 † 0.14 † 0.19 ‡ 20.35 ‡ 20.62 ‡ 0.17 † 20.06 ‡ 0.02 ‡ 0.12 ‡ 0.15 ‡ 0.03 ‡ 20.12 ‡ 0.09 ‡ 0.04 ‡ 20.88 Ã I883M 0.08 ‡ 20.38 † 0.09 † 0.05 ‡ 20.24 ‡ 20.18 ‡ 0.11 † 0.02 ‡ 20.05 ‡ 0.04 ‡ 20.04 ‡ 0.04 ‡ 0.02 ‡ 20.12 ‡ 0.01 ‡ 0.25 Ã 0.81 Ã R1587K 0.00 ‡ 0.03 ‡ 20.04 ‡ 20.05 ‡ 0.06 ‡ 0.00 ‡ 0.01 ‡ 20.04 ‡ 20.08 ‡ 20.07 ‡ 20.08 ‡ 20.08 † 20.06 ‡ 0.01 ‡ 20.03 ‡ 0.14 † 20.27 ‡ 20.01 ‡ Ã P , 0.001.
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ABCA1 p.Arg219Lys 17412755:74:155
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ABCA1 p.Arg219Lys 17412755:74:1625
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95 A G/G 59.94 (9.79), 708 0.57 299G.C (rs2740483) G/G 60.41 (9.90), 505 0.12 G/A 59.80 (9.88), 180 G/C 59.41 (9.68), 363 A/A 57.80 (8.82), 15 C/C 59.18 (9.35), 78 21217C.T (rs10991420) C/C 59.47 (9.82), 769 0.05 214C.T (rs1800977) C/C 59.80 (9.69), 460 0.54 C/T 61.11 (9.48), 209 C/T 59.74 (9.80), 401 T/T 59.82 (11.39), 11 T/T 60.68 (10.5), 113 21034ATins/del (rs34669957) AT/AT 59.63 (9.71), 621 0.37 R219K (rs2230806) R/R 60.07 (9.94), 503 0.52 AT/ 2 60.14 (9.73), 350 R/K 59.82 (9.84), 392 2/2 60.49 (11.13), 43 K/K 59.33 (8.81), 78 2940T.G (rs2980083) T/T 59.11 (9.51), 273 0.03 V825I (rs28587567) V/V 59.70 (9.86), 866 0.24 T/G 59.85 (9.68), 430 V/I 60.75 (9.52), 100 G/G 61.07 (9.86), 200 I/I 63.46 (9.07), 4 2803G.A (rs10991419) G/G 59.83 (9.74), 812 0.79 I883M (rs4149313) I/I 60.38 (9.66), 644 0.23 G/A 59.73 (9.91), 192 I/M 59.10 (9.65), 217 A/A 58.94 (10.85), 14 M/M 62.12 (6.36), 19 R1587K (rs2230808) R/R 60.23 (9.95), 496 0.30 R/K 58.90 (9.50), 301 K/K 60.93 (9.12), 41 1416 association was detected between the R219K SNP and plasma level of HDL.
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ABCA1 p.Arg219Lys 17412755:95:401
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ABCA1 p.Arg219Lys 17412755:95:1026
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119 Plasma HDL levels (mmol/L) according to ABCA1 genotypes Polymorphism Genotype Mean (SD), n P-value Polymorphism Genotype Mean (SD), n P-value 21801C.T (rs2487046) C/C 1.26 (0.31), 93 0.88 2565C.T (rs2422493) C/C 1.25 (0.32), 81 0.78 C/T 1.23 (0.31), 122 C/T 1.24 (0.30), 137 T/T 1.29 (0.33), 40 T/T 1.23 (0.28), 54 21652A.G (rs10124728) A/A 1.22 (0.29), 99 0.37 2407G.C (rs2246293) G/G 1.24 (0.32), 76 0.80 A/G 1.25 (0.31), 131 G/C 1.23 (0.30), 123 G/G 1.29 (0.35), 30 C/C 1.24 (0.27), 52 21506G.C (rs2487047) G/G 1.26 (0.33), 156 0.47 2302C.T (rs2246298) C/C 1.26 (0.32), 165 0.67 G/C 1.21 (0.28), 90 C/T 1.21 (0.27), 68 C/C 1.24 (0.29), 14 T/T 1.27 (0.26), 13 21395C.T (rs2487048) C/C 1.26 (0.31), 96 0.83 2278G.C (rs1800976) G/G 1.25 (0.32), 80 0.79 C/T 1.22 (0.29), 115 G/C 1.24 (0.30), 126 T/T 1.26 (0.32), 45 C/C 1.23 (0.28), 51 21252G.A G/G 1.23 (0.29), 193 0.13 299G.C (rs2740483) G/G 1.25 (0.29), 139 0.83 G/A 1.27 (0.29), 44 G/C 1.23 (0.31), 93 A/A 1.27 (0.34), 7 C/C 1.30 (0.28), 21 21217C.T (rs10991420) C/C 1.25 (0.32), 202 0.64 214C.T (rs1800977) C/C 1.25 (0.31), 126 0.59 C/T 1.23 (0.28), 56 C/T 1.25 (0.32), 99 T/T 0.97 (2), 1 T/T 1.20 (0.23), 30 21034ATins/del (rs34669957) AT/AT 1.27 (0.33), 157 0.36 R219K (rs2230806) R/R 1.26 (0.30), 129 0.58 AT/ 2 1.21 (0.26), 89 R/K 1.23 (0.30), 104 2/2 1.24 (0.29), 14 K/K 1.25 (0.34), 18 2940T.G (rs2980083) T/T 1.24 (0.32), 70 0.77 V825I (rs28587567) V/V 1.23 (0.30), 232 0.01 T/G 1.24 (0.31), 117 V/I 1.34 (0.31), 26 G/G 1.22 (0.29), 53 I/I 1.54 (0.07), 3 2803G.A (rs10991419) G/G 1.26 (0.31), 208 0.40 I883M (rs4149313) I/I 1.20 (0.27), 172 0.0004 G/A 1.20 (0.28), 51 I/M 1.39 (0.36), 56 A/A 1.32 (0.47), 4 M/M 1.34 (0.34), 9 R1587K (rs2230808) R/R 1.27 (0.31), 142 0.39 R/K 1.24 (0.30), 84 K/K 1.18 (0.20), 9 Figure 2.
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ABCA1 p.Arg219Lys 17412755:119:1219
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126 Single nucleotide polymorphism selection and determination of genotypes The subjects of this study were genotyped for 15 common SNPs in the proximal promoter region, i.e. 21801C.T (rs2487046), 21652A.G (rs10124728), 21506G.C (rs2487047), 21395C.T (rs2487048), 21252G.A (rs number unavailable), 21217C.T (rs10991420), 21034A Tins/del (rs34669957), 2940T.G (rs2980083), 2803G.A (rs10991419), 2565C.T (rs2422493), 2407G.C (rs2246293), 2302C.T (rs2246298), 2278G.C (rs1800976), 299G.C (rs2740483) and 214C.T (rs1800977), respectively, and four common non-synonymous SNPs, i.e. R219K (rs2230806), V825I (rs28587567), I883M (rs4149313) and R1587K (rs2230808) (Fig. 1).
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ABCA1 p.Arg219Lys 17412755:126:573
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76 Coefficients (D 0 ) of pair-wise linkage disequilibrium between ABCA1 SNPs 21801 21652 21506 21395 21252 21217 21034 2940 2803 2565 2407 2302 2278 299 214 R219K V825I I883M 21652A.G 20.97  21506G.C 20.97  20.86  21395C.T 0.94  20.94  20.91  21252G.A 20.90  0.89  20.64 ߤ 20.95  21217C.T 21.00  0.96  20.94  20.97  20.91 ߤ 21034ATins/del 20.91  20.90  0.89  20.94  20.80  20.94  2940T.G 20.95  0.40  0.90  20.95  20.79  0.96  0.84  2803G.A 0.93  20.91  20.95  0.96  20.83 ߤ 21.00  20.95  20.98  2565C.T 20.95  20.42  0.71  20.97  20.81  1.00  0.74  0.92  20.98  2407G.C 20.87  0.39  0.71  20.86  20.74  0.88  0.73  0.86  20.95  0.92  2302C.T 20.85  20.90  0.87  20.88  20.77  20.87  0.90  0.84  20.89  0.94  0.98  2278G.C 20.94  0.41  0.72  20.94  20.83  0.96  0.77  0.93  20.98  0.99  0.91  0.92  299G.C 0.79  20.81  20.84  0.82  20.96  20.88  20.80  20.82  20.96  20.85  20.75  20.88  20.85  214C.T 20.93  0.10 ߤ 0.78  20.94  20.81  20.89  0.77  0.91  21.00  0.98  0.90  0.84  0.98  20.86  R219K 0.14 ߤ 20.17 ߤ 20.18 ߥ 0.14 ߤ 20.62  0.01 ߥ 20.16 ߥ 0.00 ߥ 0.09 ߥ 20.11 ߤ 0.10 ߥ 20.17 ߥ 0.11 ߥ 0.04 ߥ 0.05 ߥ V825I 20.03 ߥ 20.39 ߤ 0.14 ߤ 0.19 ߥ 20.35 ߥ 20.62 ߥ 0.17 ߤ 20.06 ߥ 0.02 ߥ 0.12 ߥ 0.15 ߥ 0.03 ߥ 20.12 ߥ 0.09 ߥ 0.04 ߥ 20.88  I883M 0.08 ߥ 20.38 ߤ 0.09 ߤ 0.05 ߥ 20.24 ߥ 20.18 ߥ 0.11 ߤ 0.02 ߥ 20.05 ߥ 0.04 ߥ 20.04 ߥ 0.04 ߥ 0.02 ߥ 20.12 ߥ 0.01 ߥ 0.25  0.81  R1587K 0.00 ߥ 0.03 ߥ 20.04 ߥ 20.05 ߥ 0.06 ߥ 0.00 ߥ 0.01 ߥ 20.04 ߥ 20.08 ߥ 20.07 ߥ 20.08 ߥ 20.08 ߤ 20.06 ߥ 0.01 ߥ 20.03 ߥ 0.14 ߤ 20.27 ߥ 20.01 ߥ  P , 0.001.
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ABCA1 p.Arg219Lys 17412755:76:155
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ABCA1 p.Arg219Lys 17412755:76:1116
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96 A G/G 59.94 (9.79), 708 0.57 299G.C (rs2740483) G/G 60.41 (9.90), 505 0.12 G/A 59.80 (9.88), 180 G/C 59.41 (9.68), 363 A/A 57.80 (8.82), 15 C/C 59.18 (9.35), 78 21217C.T (rs10991420) C/C 59.47 (9.82), 769 0.05 214C.T (rs1800977) C/C 59.80 (9.69), 460 0.54 C/T 61.11 (9.48), 209 C/T 59.74 (9.80), 401 T/T 59.82 (11.39), 11 T/T 60.68 (10.5), 113 21034ATins/del (rs34669957) AT/AT 59.63 (9.71), 621 0.37 R219K (rs2230806) R/R 60.07 (9.94), 503 0.52 AT/ 2 60.14 (9.73), 350 R/K 59.82 (9.84), 392 2/2 60.49 (11.13), 43 K/K 59.33 (8.81), 78 2940T.G (rs2980083) T/T 59.11 (9.51), 273 0.03 V825I (rs28587567) V/V 59.70 (9.86), 866 0.24 T/G 59.85 (9.68), 430 V/I 60.75 (9.52), 100 G/G 61.07 (9.86), 200 I/I 63.46 (9.07), 4 2803G.A (rs10991419) G/G 59.83 (9.74), 812 0.79 I883M (rs4149313) I/I 60.38 (9.66), 644 0.23 G/A 59.73 (9.91), 192 I/M 59.10 (9.65), 217 A/A 58.94 (10.85), 14 M/M 62.12 (6.36), 19 R1587K (rs2230808) R/R 60.23 (9.95), 496 0.30 R/K 58.90 (9.50), 301 K/K 60.93 (9.12), 41 association was detected between the R219K SNP and plasma level of HDL.
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ABCA1 p.Arg219Lys 17412755:96:401
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ABCA1 p.Arg219Lys 17412755:96:1022
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120 Plasma HDL levels (mmol/L) according to ABCA1 genotypes Polymorphism Genotype Mean (SD), n P-value Polymorphism Genotype Mean (SD), n P-value 21801C.T (rs2487046) C/C 1.26 (0.31), 93 0.88 2565C.T (rs2422493) C/C 1.25 (0.32), 81 0.78 C/T 1.23 (0.31), 122 C/T 1.24 (0.30), 137 T/T 1.29 (0.33), 40 T/T 1.23 (0.28), 54 21652A.G (rs10124728) A/A 1.22 (0.29), 99 0.37 2407G.C (rs2246293) G/G 1.24 (0.32), 76 0.80 A/G 1.25 (0.31), 131 G/C 1.23 (0.30), 123 G/G 1.29 (0.35), 30 C/C 1.24 (0.27), 52 21506G.C (rs2487047) G/G 1.26 (0.33), 156 0.47 2302C.T (rs2246298) C/C 1.26 (0.32), 165 0.67 G/C 1.21 (0.28), 90 C/T 1.21 (0.27), 68 C/C 1.24 (0.29), 14 T/T 1.27 (0.26), 13 21395C.T (rs2487048) C/C 1.26 (0.31), 96 0.83 2278G.C (rs1800976) G/G 1.25 (0.32), 80 0.79 C/T 1.22 (0.29), 115 G/C 1.24 (0.30), 126 T/T 1.26 (0.32), 45 C/C 1.23 (0.28), 51 21252G.A G/G 1.23 (0.29), 193 0.13 299G.C (rs2740483) G/G 1.25 (0.29), 139 0.83 G/A 1.27 (0.29), 44 G/C 1.23 (0.31), 93 A/A 1.27 (0.34), 7 C/C 1.30 (0.28), 21 21217C.T (rs10991420) C/C 1.25 (0.32), 202 0.64 214C.T (rs1800977) C/C 1.25 (0.31), 126 0.59 C/T 1.23 (0.28), 56 C/T 1.25 (0.32), 99 T/T 0.97 (2), 1 T/T 1.20 (0.23), 30 21034ATins/del (rs34669957) AT/AT 1.27 (0.33), 157 0.36 R219K (rs2230806) R/R 1.26 (0.30), 129 0.58 AT/ 2 1.21 (0.26), 89 R/K 1.23 (0.30), 104 2/2 1.24 (0.29), 14 K/K 1.25 (0.34), 18 2940T.G (rs2980083) T/T 1.24 (0.32), 70 0.77 V825I (rs28587567) V/V 1.23 (0.30), 232 0.01 T/G 1.24 (0.31), 117 V/I 1.34 (0.31), 26 G/G 1.22 (0.29), 53 I/I 1.54 (0.07), 3 2803G.A (rs10991419) G/G 1.26 (0.31), 208 0.40 I883M (rs4149313) I/I 1.20 (0.27), 172 0.0004 G/A 1.20 (0.28), 51 I/M 1.39 (0.36), 56 A/A 1.32 (0.47), 4 M/M 1.34 (0.34), 9 R1587K (rs2230808) R/R 1.27 (0.31), 142 0.39 R/K 1.24 (0.30), 84 K/K 1.18 (0.20), 9 Figure 2.
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ABCA1 p.Arg219Lys 17412755:120:1219
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127 Single nucleotide polymorphism selection and determination of genotypes The subjects of this study were genotyped for 15 common SNPs in the proximal promoter region, i.e. 21801C.T (rs2487046), 21652A.G (rs10124728), 21506G.C (rs2487047), 21395C.T (rs2487048), 21252G.A (rs number unavailable), 21217C.T (rs10991420), 21034A Tins/del (rs34669957), 2940T.G (rs2980083), 2803G.A (rs10991419), 2565C.T (rs2422493), 2407G.C (rs2246293), 2302C.T (rs2246298), 2278G.C (rs1800976), 299G.C (rs2740483) and 214C.T (rs1800977), respectively, and four common non-synonymous SNPs, i.e. R219K (rs2230806), V825I (rs28587567), I883M (rs4149313) and R1587K (rs2230808) (Fig. 1).
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ABCA1 p.Arg219Lys 17412755:127:573
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PMID: 17553166 [PubMed] Pasdar A et al: "The effect of ABCA1 gene polymorphisms on ischaemic stroke risk and relationship with lipid profile."
No. Sentence Comment
7 Methods: We studied four common polymorphisms in ABCA1 gene: G/A-L158L, G/A-R219K, G/ A-G316G and G/A-R1587K in 400 Caucasian ischaemic stroke patients and 487 controls.
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ABCA1 p.Arg219Lys 17553166:7:76
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9 Results: Genotype and allele frequencies of all polymorphisms were similar in cases and controls, except for a modest difference in the ABCA1 R219K allele frequency (P-value = 0.05).
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14 Individuals who had R219K "22" genotype had a higher LDL level (p = 0.001).
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ABCA1 p.Arg219Lys 17553166:14:20
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33 The only published study in ischaemic stroke on 244 Hungarian patients [25] suggests a protective role for the ABCA1-R219K and V771M polymorphisms.
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ABCA1 p.Arg219Lys 17553166:33:117
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46 We used different sets of primers for each SNP as follows: 1- ABCA1-rs2230805 (G/A; L158L); designated as [ABCA1-6] ABCA1-2230805F: 5'-biotin-TAGACTTTGGGAGAGA- GAGGTTGT-3' ABCA1-2230805R: 5'-AATGAAACCTTCTCTGGGTTCC-3' 2- ABCA1-rs2234884 (G1051A; R219K); designated as [ABCA1-3] ABCA1-2234884F: 5'-biotin-AATTTCTGAGCTTTGT- GGACTA-3' ABCA1-2234884R: 5'-GCTCTGCTGCAGTCATTTTCTC-3' 3- ABCA1-rs2246841 (G888A; G316G); designated as [ABCA1-5] ABCA1-2246841F: 5'-biotin-TACCAGTTGAGAGACTT- GATCTTC-3' ABCA1-2246841R: 5'-TCTCGTATTGTCTGTGGGCATC-3' 4- ABCA1-rs1997618 (c/t, T1555I) ABCA1-1997618F: 5'-biotin-CCGAGTCAAGAAGTTAAT- GATGC-3' ABCA1-1997618R: 5'-GCTTTAGGTGTTTCTTCATTT- GTTT-3' 5- ABCA1-rs2234886 (G5155A; R1587K); designated as [ABCA1-4] ABCA1-2234886F: 5'-biotin-CAGCGGTTTACCTTGACAT- TATT-3' ABCA1-2234886R: 5'-GAAGATTTATGACAGGACT- GGACAC-3' 6- ABCA1-rs1883024 (c/t, P1648L) ABCA1-1883024F: 5'-biotin-TATACA- GACACAGCCACACTTA-3' ABCA1-1883024R: 5'-ATCTCACCAAGCAGCAGTTCTC-3' Of the six ABCA1 SNPs, only four SNPs (G/A-L158L, G/A-R219K, G/A-G316G and G/A-R1587K) were polymorphic in the Scottish population.
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ABCA1 p.Arg219Lys 17553166:46:242
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60 Haplotype frequencies for the four loci (G/A-L158L, G/A-R219K, G/A-G316G and G/A-R1587K) were estimated for cases and controls, using PHASE Ver.2.11 [28].
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ABCA1 p.Arg219Lys 17553166:60:56
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63 ABCA1-3 (G1051A; R219K) "G" allele frequency (R variant) was 68.2% in cases and 73.2% in controls (p = 0.05; OR = 0.79, 95%CI: 0.62-1.00), ABCA1-5 (G/A; G316G) "G" allele frequency (G variant) was 88% in cases and 86.7% in controls (p = 0.42; OR = 1.13, 95%CI: 0.84-1.52); ABCA1-4 (G5155A; R1587K) "G" allele frequency (R variant) was 77.4% in cases and 75.9% in controls (p = 0.47; OR = 1.09, 95%CI: 0.86-1.37).
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65 In addition to a trend to lower ABCA1-3 (G1051A; R219K) "G" allele frequency in all cases (p = 0.05), especially in males (p = 0.04), the "22" genotype was higher in LVD cases (p = 0.04) and also in patients over 65 years (p Table 2: Different stroke subtypes based on TOAST classification Subtype All Stroke Samples Number % Large Vessel Disease (LVD) 141 35.3% Small Vessel Disease (SVD) 98 24.5% Cardioembolic 76 19% Other/Unclear 85 21.3% Hemorrhagic Stroke 0 0 TOTAL 400 100% Table 1: Specifications of cases and controls Cases (n = 400) Controls (n = 487) Mean age (± SD)§ 66 (± 11) 64.2(± 12.3) Sex (M:F Ratio)§ 1.4 0.97 Hypertension*§ 41% 18% Diabetes Mellitus**§ 12.2% 3.2% Total Cholesterol mmol/l (Ave., SD)§ 5.6 (± 1.3) 5.8 (± 1.2) HDL mmol/l (Ave., SD)§ 1.2 (± 0.4) 1.4 (± 0.4) LDL mmol/l (Ave., SD) 3.5 (± 1.2) 3.5 (± 1.1) Total Triglyceride mmol/l (Ave., SD) 1.7 (± 1.1) 1.8 (± 1.1) Glucose mmol/l§ 6.4 (± 2.4) 5.9 (± 1.2) * Hypertension defined as blood pressure > 160/90 mmHg or history of hypertension/on hypertensive therapy ** History of diabetes or confirmed laboratory diagnosis §Significant difference (P < 0.05) between cases and controls = 0.01), compared to controls.
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ABCA1 p.Arg219Lys 17553166:65:49
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70 Cases with ABCA1-3 (G1051A; R219K) "22" genotype had a higher LDL level compared to controls which remained significant after Bonferroni correction (p = 0.003).
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ABCA1 p.Arg219Lys 17553166:70:28
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72 However, in this subgroup, females with ABCA1-3 (G1051A; R219K) "11" and ABCA1-4 (G5155A; R1587K) "22" genotypes had a higher level of IDL (p = 0.01 and p = 0.02) respectively.
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ABCA1 p.Arg219Lys 17553166:72:57
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ABCA1 p.Arg219Lys 17553166:72:149
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73 Effects of alleles on lipid profile Comparing the lipid profiles in carriers of different ABCA1 alleles revealed that individuals who were the ABCA1-R219K carrier (K allele) had a lower TG level than non carriers (p = 0.005).
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84 Other works have reported that CAD patients who are carriers of R219K allele had less severe atherosclerosis [31] and overall lower risk of CAD [36].
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ABCA1 p.Arg219Lys 17553166:84:58
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ABCA1 p.Arg219Lys 17553166:84:64
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85 Andrikovics et al recently reported a higher frequency of R219K in controls than in Hungarian stroke patients and suggested a protective role for this polymorphism [25].
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ABCA1 p.Arg219Lys 17553166:85:58
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89 While the R219K -G1051A- (A or "K" variant) has been associated with decreased TG, increased HDL and subsequently a lower risk for atherosclerotic progression, in contrast the R allele has been associated with vascular disease [31].
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ABCA1 p.Arg219Lys 17553166:89:10
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ABCA1 p.Arg219Lys 17553166:89:87
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90 This has not been confirmed in our study, although in our stroke population those with R219K "22" genotype (AA) had a higher level of LDL and the "K allele" carriers had a lower TG.
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ABCA1 p.Arg219Lys 17553166:90:87
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92 The HDL level showed no significant difference among different R219K genotypes.
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102 Other studies have shown an association between the R219K polymorphism and MI, but no association between haplotype arrangements and MI.
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ABCA1 p.Arg219Lys 17553166:102:52
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112 Among the studied ABCA1 gene polymorphisms, R219K has the greatest impact on lipid profile especially LDL and TG.
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59 Haplotype frequencies for the four loci (G/A-L158L, G/A-R219K, G/A-G316G and G/A-R1587K) were estimated for cases and controls, using PHASE Ver.2.11 [28].
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62 ABCA1-3 (G1051A; R219K) "G" allele frequency (R variant) was 68.2% in cases and 73.2% in controls (p = 0.05; OR = 0.79, 95%CI: 0.62-1.00), ABCA1-5 (G/A; G316G) "G" allele frequency (G variant) was 88% in cases and 86.7% in controls (p = 0.42; OR = 1.13, 95%CI: 0.84-1.52); ABCA1-4 (G5155A; R1587K) "G" allele frequency (R variant) was 77.4% in cases and 75.9% in controls (p = 0.47; OR = 1.09, 95%CI: 0.86-1.37).
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64 In addition to a trend to lower ABCA1-3 (G1051A; R219K) "G" allele frequency in all cases (p = 0.05), especially in males (p = 0.04), the "22" genotype was higher in LVD cases (p = 0.04) and also in patients over 65 years (p Table 2: Different stroke subtypes based on TOAST classification Subtype All Stroke Samples Number % Large Vessel Disease (LVD) 141 35.3% Small Vessel Disease (SVD) 98 24.5% Cardioembolic 76 19% Other/Unclear 85 21.3% Hemorrhagic Stroke 0 0 TOTAL 400 100% Table 1: Specifications of cases and controls Cases (n = 400) Controls (n = 487) Mean age (&#b1; SD)&#a7; 66 (&#b1; 11) 64.2(&#b1; 12.3) Sex (M:F Ratio)&#a7; 1.4 0.97 Hypertension*&#a7; 41% 18% Diabetes Mellitus**&#a7; 12.2% 3.2% Total Cholesterol mmol/l (Ave., SD)&#a7; 5.6 (&#b1; 1.3) 5.8 (&#b1; 1.2) HDL mmol/l (Ave., SD)&#a7; 1.2 (&#b1; 0.4) 1.4 (&#b1; 0.4) LDL mmol/l (Ave., SD) 3.5 (&#b1; 1.2) 3.5 (&#b1; 1.1) Total Triglyceride mmol/l (Ave., SD) 1.7 (&#b1; 1.1) 1.8 (&#b1; 1.1) Glucose mmol/l&#a7; 6.4 (&#b1; 2.4) 5.9 (&#b1; 1.2) * Hypertension defined as blood pressure > 160/90 mmHg or history of hypertension/on hypertensive therapy ** History of diabetes or confirmed laboratory diagnosis &#a7;Significant difference (P < 0.05) between cases and controls = 0.01), compared to controls.
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69 Cases with ABCA1-3 (G1051A; R219K) "22" genotype had a higher LDL level compared to controls which remained significant after Bonferroni correction (p = 0.003).
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71 However, in this subgroup, females with ABCA1-3 (G1051A; R219K) "11" and ABCA1-4 (G5155A; R1587K) "22" genotypes had a higher level of IDL (p = 0.01 and p = 0.02) respectively.
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ABCA1 p.Arg219Lys 17553166:71:57
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83 Other works have reported that CAD patients who are carriers of R219K allele had less severe atherosclerosis [31] and overall lower risk of CAD [36].
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88 While the R219K -G1051A- (A or "K" variant) has been associated with decreased TG, increased HDL and subsequently a lower risk for atherosclerotic progression, in contrast the R allele has been associated with vascular disease [31].
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91 The HDL level showed no significant difference among different R219K genotypes.
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ABCA1 p.Arg219Lys 17553166:91:63
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101 Other studies have shown an association between the R219K polymorphism and MI, but no association between haplotype arrangements and MI.
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ABCA1 p.Arg219Lys 17553166:101:52
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111 Among the studied ABCA1 gene polymorphisms, R219K has the greatest impact on lipid profile especially LDL and TG.
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PMID: 17372331 [PubMed] Soro-Paavonen A et al: "Common ABCA1 variants, HDL levels, and cellular cholesterol efflux in subjects with familial low HDL."
No. Sentence Comment
5 Cholesterol-loaded macrophages from low-HDL subjects showed significantly increased levels of ABCA1 mRNA but not of ABCG1 mRNA and were more often carriers of the rare ABCA1 alleles L158 and R219K.
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ABCA1 p.Arg219Lys 17372331:5:191
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137 Three SNPs differed significantly between the low-HDL family members and control subjects [L158 (rs2230805), P 5 0.004; R219K (rs2230806), P 5 0.005; and rs2297409, P 5 0.006], so that the rare alleles of each of these SNPs were overrepresented among low-HDL subjects (Table 3).
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ABCA1 p.Arg219Lys 17372331:137:22
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ABCA1 p.Arg219Lys 17372331:137:120
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138 The variants L158 and R219K showed significant association with low HDL-C levels (P 5 0.009 and P 5 0.007, respectively), and T1427 showed association with high HDL-C (P 5 0.028).
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ABCA1 p.Arg219Lys 17372331:138:22
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140 We constructed allelic haplotypes of the three SNPs that showed association with either high or low HDL-C levels (L158, R219K, and T1427T) using PHASE version 2.0 software.
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ABCA1 p.Arg219Lys 17372331:140:120
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146 Comparisons of the ABCA1 allele frequencies between 47 low-HDL family members (19 unaffected and 28 affected subjects) and 25 control subjects, and ABCA1 genotype effects on cholesterol efflux, HDL-C, and mean IMT in the pooled study group (n 5 72) Single-Nucleotide Polymorphism Identification Number Amino Acid Residue Allele Frequencies and P Value in Low-HDL Family Members Versus Control Subjectsa HDL-C Pb Mean IMT Pc rs2472459 - NS NS NS rs2246293 - NS NS NS rs2515616 - NS NS NS rs1800978 - NS NS NS rs2740492 - NS NS NS rs3858075 - NS NS NS rs1929842 - NS NS NS rs2230805 L158 (0.45 vs. 0.12) 0.004 0.009 NS rs2230806 R219K (0.40 vs. 0.08) 0.005 0.007 NS rs2487037 - NS NS NS rs2297409 - (0.30 vs. 0.04) 0.006 NS NS rs2066716 T1427 (0.11 vs. 0.32) 0.053 0.003 NS rs2230808 R1587K NS NS NS rs2066881 - NS NS NS rs4149341 - NS NS 0.025 a For statistically significant differences, the corresponding allele frequencies are given in parentheses (in low-HDL family members vs. control subjects), followed by Chi-square P value, with Fisher`s exact test for the differences in allele frequencies between low-HDL family members and control subjects.
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ABCA1 p.Arg219Lys 17372331:146:627
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158 Interestingly, the carrier status of the haplotype containing the R219K variant was not associated with the cholesterol efflux activity, implying that this particular variant does not result in the disturbed function of ABCA1 in macrophages but rather tags the allelic variant related to serum HDL-C level regulation, possibly at the hepatic level.
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ABCA1 p.Arg219Lys 17372331:158:66
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162 The efflux (%) was not changed significantly between carriers and noncarriers of the rare alleles in R219K.
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191 In turn, in healthy subjects and CHD patients of European 1414 Journal of Lipid Research Volume 48, 2007 atHealthScienceLibraryCB#7585,onSeptember24,2012www.jlr.orgDownloadedfrom 0.DC1.html and French-Canadian origin, the common variant R219K was associated with increased levels of HDL, decreased TGs, and reduced severity of atherosclerosis (42, 43).
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ABCA1 p.Arg219Lys 17372331:191:238
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194 Of these, T1427 gave corresponding results in both data sets, showing association with increased HDL-C. The variant R219K showed association with low serum HDL levels but not with the cholesterol efflux in our study sample.
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204 In summary, based on our data, we conclude that 1) macrophages derived from Finnish subjects with familial low HDL displayed similar cholesterol-loading capacity but decreased cholesterol efflux to apoA-I via the ABCA1 pathway after loading; 2) familial low HDL in these families is not caused by rare mutations in ABCA1; rather, the common allelic variants are associated with HDL-C levels, as indicated by the dose-dependent contribution of the haplotype carrying the common R219K change in these subjects; and 3) relative ABCA1 mRNA expression in cholesterol-loaded macrophages was increased significantly in the low-HDL group.
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ABCA1 p.Arg219Lys 17372331:204:477
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136 Three SNPs differed significantly between the low-HDL family members and control subjects [L158 (rs2230805), P 5 0.004; R219K (rs2230806), P 5 0.005; and rs2297409, P 5 0.006], so that the rare alleles of each of these SNPs were overrepresented among low-HDL subjects (Table 3).
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139 We constructed allelic haplotypes of the three SNPs that showed association with either high or low HDL-C levels (L158, R219K, and T1427T) using PHASE version 2.0 software.
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145 Comparisons of the ABCA1 allele frequencies between 47 low-HDL family members (19 unaffected and 28 affected subjects) and 25 control subjects, and ABCA1 genotype effects on cholesterol efflux, HDL-C, and mean IMT in the pooled study group (n 5 72) Single-Nucleotide Polymorphism Identification Number Amino Acid Residue Allele Frequencies and P Value in Low-HDL Family Members Versus Control Subjectsa HDL-C Pb Mean IMT Pc rs2472459 - NS NS NS rs2246293 - NS NS NS rs2515616 - NS NS NS rs1800978 - NS NS NS rs2740492 - NS NS NS rs3858075 - NS NS NS rs1929842 - NS NS NS rs2230805 L158 (0.45 vs. 0.12) 0.004 0.009 NS rs2230806 R219K (0.40 vs. 0.08) 0.005 0.007 NS rs2487037 - NS NS NS rs2297409 - (0.30 vs. 0.04) 0.006 NS NS rs2066716 T1427 (0.11 vs. 0.32) 0.053 0.003 NS rs2230808 R1587K NS NS NS rs2066881 - NS NS NS rs4149341 - NS NS 0.025 a For statistically significant differences, the corresponding allele frequencies are given in parentheses (in low-HDL family members vs. control subjects), followed by Chi-square P value, with Fisher`s exact test for the differences in allele frequencies between low-HDL family members and control subjects.
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157 Interestingly, the carrier status of the haplotype containing the R219K variant was not associated with the cholesterol efflux activity, implying that this particular variant does not result in the disturbed function of ABCA1 in macrophages but rather tags the allelic variant related to serum HDL-C level regulation, possibly at the hepatic level.
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161 The efflux (%) was not changed significantly between carriers and noncarriers of the rare alleles in R219K.
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190 In turn, in healthy subjects and CHD patients of European 1414 Journal of Lipid Research Volume 48, 2007 at SEMMELWEIS EGYETEM NET KORELET, on December , and French-Canadian origin, the common variant R219K was associated with increased levels of HDL, decreased TGs, and reduced severity of atherosclerosis (42, 43).
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193 Of these, T1427 gave corresponding results in both data sets, showing association with increased HDL-C. The variant R219K showed association with low serum HDL levels but not with the cholesterol efflux in our study sample.
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203 In summary, based on our data, we conclude that 1) macrophages derived from Finnish subjects with familial low HDL displayed similar cholesterol-loading capacity but decreased cholesterol efflux to apoA-I via the ABCA1 pathway after loading; 2) familial low HDL in these families is not caused by rare mutations in ABCA1; rather, the common allelic variants are associated with HDL-C levels, as indicated by the dose-dependent contribution of the haplotype carrying the common R219K change in these subjects; and 3) relative ABCA1 mRNA expression in cholesterol-loaded macrophages was increased significantly in the low-HDL group.
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PMID: 16725228 [PubMed] Sundar PD et al: "Gender-specific association of ATP-binding cassette transporter 1 (ABCA1) polymorphisms with the risk of late-onset Alzheimer's disease."
No. Sentence Comment
4 In the present study, we examined the role of two ABCA1 polymorphisms, R219K (rs2230806) and G-17C (rs2740483) in modifying the risk of late-onset AD (LOAD) in a large American white cohort of 992 AD cases and 699 controls.
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5 We observed significant gender × R219K interaction (p = 0.00008).
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8 The risk associated with the R219K polymorphism was independent of the recently reported significant association in the ubiquilin (UBQLN1) gene in this region on chromosome 9q.
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9 Our data suggest a gender-specific and APOE and UBQLN1 independent association between the ABCA1/R219K polymorphism and LOAD.
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31 In the present case-control association study, we examined the role of two ABCA1 polymorphisms: R219K (rs2230806) located in exon 7 resulting in a G to A nucleotide change at position 1051 and G-17C (rs2740483) located in the promoter region with LOAD risk.
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32 Previously R219K has been found to be associated with HDL-C levels and coronary artery disease (CAD) risk [5,8] but has shown inconsistent association with AD [17,22,32].
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43 The R219K and G-17C genotypes were determined by pyrosequencing on the PSQTM HS 96 system (Biotage, Uppsala, Sweden).
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44 Duplex pyrosequencing assay was performed using the following PCR (F, R) and sequencing (S) primers for R219K: F-5 -/5Bio/TGCAAGGCTACCAGTT- ACATT-3 ; R-5 -TAGGCTTCAGGATGTCCATGTT-3 ; S-5 -GCAGCCAGTTTCTCC-3 and G-17C: F-5 -CGTG- CTTTCTGCTGAGTGACTG-3 ; R-5 -/5Bio/CGAGCGCA- GAGGTTACTATC-3 ; S-5 -ACAGAGGCCGGGA-3 according to the previously described procedure [7].
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ABCA1 p.Arg219Lys 16725228:44:104
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53 For the simultaneous analysis of ABCA1 and UBQLN1, we included the ABCA1/R219K SNP and three UBQLN1 SNPs (intron 6 A → C, intron 8 T → C and intron 9 A → G).
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58 Associations between ABCA1 polymorphisms and late-onset AD We genotyped 1691 subjects for the R219K SNP (992 cases and 699 controls) and 1379 subjects for the G-17C Table 1 Distribution of ABCA1 polymorphisms in American white LOAD cases and controls Genotype Total Female Male AD Controls AD Controls AD Controls n (%) n (%) n (%) n (%) n (%) n (%) R219K RR 489 49.3 374 53.5 306 46.4 249 57.64a 183 55.0 125 46.82b RK 424 42.7 274 39.2 296 44.9 151 35.0 128 38.4 123 46.1 KK 79 8.0 51 7.3 57 8.7 32 7.4 22 6.6 19 7.1 Total 992 699 659 432 333 267 Allele frequency R/K 70.7/29.3 73.1/26.9 68.9/31.1 75.1/24.9c 74.2/25.8 69.9/30.1 G-17C GG 422 50.4 291 53.8 280 50.0 174 52.4 142 51.1 117 56.0 CG 319 38.1 203 37.5 216 38.6 125 37.7 103 37.1 78 37.3 CC 97 11.6 47 8.7 64 11.4 33 9.9 33 11.9 14 6.7 Total 838 541 560 332 278 209 Allele frequency G/C 69.4/30.6 72.6/27.4 69.3/30.7 71.2/28.8 69.6/30.4 74.6/25.4 a Significantly different between female AD cases and controls (RR vs. RK + KK; p = 0.0003).
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ABCA1 p.Arg219Lys 16725228:58:94
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62 The genotype distributions of the R219K polymorphism followed HWE in both AD cases and controls.
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65 The genotype and allele frequencies for the R219K and G-17C polymorphisms were comparable between AD cases and controls in the total sample (Table 1).
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67 Since the (gender × R219K) interaction term in the regression model was highly significant (p = 0.00008), we further examined the data stratified by gender.
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71 To exclude the possibility if the additional 312 individuals that were genotyped for the R219K SNP but not for the G-17C SNP could have impacted the result of the R219K SNP, we reanalyzed the data on 1370 individuals having genotypes for both SNPs.
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ABCA1 p.Arg219Lys 16725228:71:89
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72 The results for the R219K SNP were essentially the same as shown in Table 1.
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73 Both AD and controls were in HWE for the R219K SNP.
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76 Estimated haplotypes and late-onset AD risk The R219K and G-17C polymorphisms were not in linkage disequilibrium with each other (D = 0.084; p = 0.43).
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85 We fit a logistic regression model with the following independent variables: age, Table 2 Estimated haplotype frequencies among American white LOAD cases and controls Subjects Haplotype SNPs Haplotype frequency (%) p-Value R219K G-17C Total AD C Total n = 1370 n = 833 n = 537 1 R C 19.9 20.7 18.7 2 R G 52.0 50.3 54.7 3 K C 9.3 9.8 8.6 4 K G 18.7 19.2 18.0 ln(L) -2524.12 -1554.79 -966.69 0.15a Female n = 884 n = 555 n = 329 1 R C 20.2 20.1 20.3 2 R G 51.7 49.2 55.8 3 K C 9.6 10.5 8.1 4 K G 18.5 20.1 15.8 ln(L) -1636.2 -1042.6 -588.48 0.017a Male n = 486 n = 278 n = 208 1 R C 19.5 21.9 16.0 2 R G 52.6 52.4 53.2 3 K C 8.8 8.5 9.5 4 K G 19.0 17.2 21.3 ln(L) -887.54 -509.96 -374.35 0.09a a Calculated from the T5 statistic: 2[ln(L)case + ln(L)control - ln(L)case + control]; d.f. = 3. gender, APOE*4, ABCA1, UBQLN1 joint genotype at three sites (intron 6, intron 8 and intron 9), gender × ABCA1 interaction, and UBQLN1 × ABCA1 interaction (see Section 2 for precise definitions of these variables).
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92 Initial stud- Table 3 Logistic regression results for UBQLN1 3-site joint genotypes (Intron 6, Intron 8, Intron 9) and ABCA1/R219K OR 95% CI p-Value Baselinea 1.00 Sex 1.05 0.72-1.53 0.813 APOE*4 carriers 5.00 3.79-6.61 <0.0001 UBQLN1/haplotype H5 carriers 0.22 0.06-0.81 0.023 UBQLN1/one copy of haplotype H4 1.36 1.01-1.82 0.040 UBQLN1/two copies of haplotype H4 6.45 2.05-20.26 0.0014 ABCA1 1.57 1.13-2.19 0.0077 Sex × ABCA1 0.0135 a Female non-APOE*4, ABCA1/RR, UBQLN1/haplotypes non-H4 and H5-UBQLN1 haplotype H4 and haplotype H5 are described in Kamboh et al. [16].
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100 In the current study, we examined the role of two ABCA1 polymorphisms, R219K and G-17C, with the risk of AD in a large case-control cohort of American whites.
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101 We found a significant interaction with the R219K polymorphism and gender (p = 0.00008).
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103 The R219K association was confirmed in the two-site haplotype analysis, where the overall haplotype distribution was significant in females only (p = 0.017).
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105 Intriguingly, male AD cases and controls showed an opposite trend in R219K allele and haplotype frequency distribution compared to females.
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106 The underlying mechanism for the gender-specific differences in frequency and effect on AD risk for the R219K polymorphism in our study is unclear.
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107 Although both male and female controls in our study appeared to be in HWE for the R219K polymorphism, it needs to be taken into account that theirR219Kfrequenciesmaynotberepresentativeofthegen- eral population at large because this control group selectively included older, non-demented individuals.
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113 We do not know if different frequencies of the R219K SNP between our older normal males and females represent a survival effect because reported AD case-control studies have not presented gender-stratified genotype data for comparison.
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114 Most of the earlier studies with the R219K SNP were carried out in relation to CAD risk and with the exception of one study all other studies presented gender-combined data.
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123 Previous studies have not investigated the gender-specific effect of the R219K polymorphism on AD risk.
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124 Wollmer et al. [32] did not observe any effect of either the R219K SNP or another ABCA1 SNP, rs2230808 (R1587K), on LOAD risk, but reported a significant association of the 219K allele in delaying the AAO of AD.
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127 In contrast to our findings, Katzov et al. [17] found a significantly higher frequency of the R219K/KK genotype among 185 Swedish controls compared to 390 LOAD subjects (p = 0.014), however, the controls in their study were not in HWE showing an unusually inflated frequency of the R219K/KK genotype.
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128 While Li et al. [22] did not observe any effect of R219K on LOAD, the rs2230808 SNP was associated with significant protective effect against LOAD.
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131 The obvious difference between our study and those reported previously is that we used a very large LOAD case-control cohort from a single geographical location (1691 subjects) that is more than double than the previously reported largest LOAD case-control series of 796 individuals for the R219K SNP [22].
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132 Similar to the previous studies, the R219K SNP in our study did not show significant difference between cases and controls in the gender-combined total sample.
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133 The other difference between our study and other studies is that we analyzed gender-specific effect of the R219K SNP in our large case-control cohort and found opposite association of the same allele in males and females.
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136 To our knowledge, the functional significance of the R219K SNP has not been evaluated.
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137 However, a recent study by Katzov et al. [18] has shown that the R219K SNP could affect the Abeta metabolism in an allele-specific manner such that the 219K allele carriers were associated with significantly higher CSF Abeta42 levels than the RR homozygotes (p = 0.0007).
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150 In summary, we report a significant association for the ABCA1/R219K polymorphism with LOAD risk in American white subjects, with a more pronounced effect in females.
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PMID: 17335784 [PubMed] Wang F et al: "Polymorphisms of cholesterol metabolism genes CYP46 and ABCA1 and the risk of sporadic Alzheimer's disease in Chinese."
No. Sentence Comment
2 The purpose of this case-control study was to determine whether single nucleotide polymorphisms (SNPs) A→G in the intron 2 of CYP46 gene and G→A (R219K) in the exon 7 of ABCA1 gene are associated with sporadic AD in the Chinese Han population.
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ABCA1 p.Arg219Lys 17335784:2:158
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29 Among the examined sites, single nucleotide polymorphisms (SNPs) A→G in the intron 2 of CYP46 gene (rs754203) and G→A (R219K) in the exon 7 of ABCA1 gene (rs2230806) were most promising., We have therefore performed a case-control study to evaluate the association between these two SNPs and sporadic AD in the Chinese Han population.
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ABCA1 p.Arg219Lys 17335784:29:131
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52 Recently, there were a few studies about the R219K polymorphism of ABCA1 gene in AD patients and their results were inconsistent (Table 3).
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63 The R219K among them predicts a G to A exchange in exon 7 resulting in an arginine to lysine exchange at amino acid 219 which occurs in the first extracellular loop of the ABCA1 protein.
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73 In conclusion, our study does not support an association between the genetic variability in CYP46 gene and the risk of AD. However, our data revealed that ABCA1 KK genotype and Table 3 - Studies about R219K polymorphism within ABCA1 gene in AD patients Studies Number (cases/controls) Race K allele (%) (cases/controls) Conclusion Wollmer et al., 2003 169/166 Caucasian 29.9/27.7 A delayed age-at-onset Katzov et al., 2004 390/185 Swedish 21.5/27.5 Positive Li et al., 2004 419/377 Caucasian 27.4/27.4 Negative Shibata et al., 2006 218/195 Caucasian 26.0/22.0 Negative 118 AD families Hispanic origin 36.5 A possible interaction between ABCA1 and APOE Sundar et al., 2006 992/699 American whites Total: 29.3/26.9 Positive in female Female: 31.1/24.9 Male: 25.8/30.1 Table 2 - Genotype and allele distributions of R219K polymorphism within ABCA1 gene in AD patients and controls by stratifying for gender or APOE ε4 status Group n Allele (%) Genotype (%) R K RR RK KK Male AD 74 88 (59.5) 60 (40.5) 27 (36.5) 34 (45.9) 13 (17.6) Control 89 94 (52.8) 84 (47.2) 27 (30.3) 40 (44.9) 22 (24.7) χ2 =1.449, P=0.229 χ2 =1.433, P=0.489 Female AD 94 121 (64.4) 67 (35.6) 38 (40.4) 45 (47.9) 11 (11.7) Control 126 129 (51.2) 123 (48.8) 30 (23.8) 69 (54.8) 27 (21.4) χ2 =7.613, P=0.006 χ2 =8.251, P=0.016 ε4 allele carrier AD 42 47 (56.0) 37 (44.0) 12 (28.6) 23 (54.8) 7 (16.7) Control 21 20 (47.6) 22 (52.4) 5 (23.8) 10 (47.6) 6 (28.6) χ2 =0.781, P=0.377 χ2 =1.216, P=0.545 Non-ε4 carrier AD 126 162 (64.3) 90 (35.7) 53 (42.1) 56 (44.4) 17 (13.5) Control 194 203 (52.3) 185 (47.7) 52 (26.8) 99 (51.0) 43 (22.)
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ABCA1 p.Arg219Lys 17335784:73:201
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198 R219K polymorphism of the ABCA1 gene and its modulation of the variations in serum high-density lipoprotein cholesterol and triglycerides related to age and adiposity in white versus black young adults.
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197 R219K polymorphism of the ABCA1 gene and its modulation of the variations in serum high-density lipoprotein cholesterol and triglycerides related to age and adiposity in white versus black young adults.
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PMID: 17303779 [PubMed] Kiss RS et al: "Genetic etiology of isolated low HDL syndrome: incidence and heterogeneity of efflux defects."
No. Sentence Comment
47 In ABCA1, a total of 19 nonsynonymous coding sequence variants; some of these we reported previously.22 Of these, 9 sequence variants were common polymorphisms (ie, reported in the literature as common or of similar prevalence in control subjects): P85L, P85A, R219K, V399A, V771M, V825I, I883M, E1172D, R1587K.14,32-35 Another 5 sequence variants, identified here, were previously reported to be disease causing: W590L (reported as W590S)14; C1477F (reported as C1477R)13; S1731C (only found in French-Canadian populations)36; N1800H32; and 1851X.37 Five sequence variants were novel: K199F, H551D, R965C, E1386Q, and D1706N.
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42 In ABCA1, a total of 19 nonsynonymous coding sequence variants; some of these we reported previously.22 Of these, 9 sequence variants were common polymorphisms (ie, reported in the literature as common or of similar prevalence in control subjects): P85L, P85A, R219K, V399A, V771M, V825I, I883M, E1172D, R1587K.14,32-35 Another 5 sequence variants, identified here, were previously reported to be disease causing: W590L (reported as W590S)14; C1477F (reported as C1477R)13; S1731C (only found in French-Canadian populations)36; N1800H32; and 1851X.37 Five sequence variants were novel: K199F, H551D, R965C, E1386Q, and D1706N.
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PMID: 17430597 [PubMed] Wahrle SE et al: "Apolipoprotein E levels in cerebrospinal fluid and the effects of ABCA1 polymorphisms."
No. Sentence Comment
40 In particular, studies have implicated the following SNPs in affecting levels of plasma HDL-C: rs2230806 (R219K) [33], rs2066718 (V771M) [31,32], rs2066715 (V825I) [31], rs4149313 (I883M) [34], rs2230808 (R1587K) [31].
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42 Additionally, studies by others have reported that the ABCA1 SNP rs2230806 (R219K) affects risk for AD [35-38].
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70 The subjects for whom we had CSF apoE data were genotyped for the following ABCA1 SNPs: rs2230806 (R219K), rs2066718 (V771M), rs2066715 (V825I), rs4149313 (I883M), rs2230808 (R1587K), rs1883025 (intron), rs2275544 (intron), rs2777799 (intron), rs3904999 (intron) and rs6479283 (intron).
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149 Genotyping The following SNPS in ABCA1 were genotyped in the Washington University sample of 168 subjects: rs2230806 (R219K), rs2066718 (V771M), rs2066715 (V825I), rs4149313 (I883M), rs2230808 (R1587K), rs1883025 (intron), rs2275544 (intron), rs2777799 (intron), rs3904999 (intron) and rs6479283 (intron).
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ABCA1 p.Arg219Lys 17430597:149:118
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PMID: 17324514 [PubMed] Wavrant-De Vrieze F et al: "ABCA1 polymorphisms and Alzheimer's disease."
No. Sentence Comment
20 doi:10.1016/j.neulet.2007.02.010 The SNPs used were rs2230806 (also designated as rs2234884) which encodes variant R219K (c.969A > G, numbering according to GenBank reference NM 005502) with a reported ~25% minor allele frequency in Caucasian populations [5,7], rs2066718 which is a V771M (c.2624A > G) variant with a reported ~3% minor allele frequency [5,7], rs2230808 which encodes a R1587K (c.5073A > G) variant with a reported 26% minor allele frequency [5,7] and finally rs2422493 which is a 5 UTR polymorphism located at -477 in the promoter with a reported 46% minor allele frequency [23,25].
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41 These previous findings emphasize the Table 1 Genotype frequency of ABCA1 polymorphisms in USA sibpair series SNP ID (function) Total (Nf = 331) ApoE-␧4- (Nf = 76) ApoE-␧4+ (Nf = 227) Fam Freq p-Value Fam Freq p-Value Fam Freq p-Value rs2422493 (promoter) C/C 45 0.266 0.62 5 0.245 N/A 25 0.284 0.62 T/C 79 0.494 0.17 14 0.494 0.29 38 0.489 0.35 T/T 44 0.241 0.02* 10 0.261 0.30 21 0.227 0.08 rs2230806 (R219K) A/A 17 0.095 0.93 2 0.058 N/A 10 0.111 0.86 A/G 66 0.399 0.23 12 0.483 0.01* 31 0.388 0.70 G/G 56 0.507 0.21 11 0.459 0.02* 25 0.500 0.59 rs2066718 (V771M) A/A 0 0 N/A 0 0 N/A 0 0 N/A A/G 14 0.100 0.69 2 0.162 N/A 6 0.102 N/A G/G 14 0.900 0.69 2 0.838 N/A 6 0.898 N/A rs2230808 (R1587K) A/A 15 0.066 0.06 5 0.044 N/A 8 0.064 N/A A/G 62 0.426 0.69 14 0.505 0.64 32 0.420 0.90 G/G 56 0.509 0.55 13 0.451 0.57 29 0.515 0.67 Fam, number of informative families; Freq, frequency; Nf, number of nuclear families; N/A, non-applicable.
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PMID: 17383594 [PubMed] Mantaring M et al: "Genotypic variation in ATP-binding cassette transporter-1 (ABCA1) as contributors to the high and low high-density lipoprotein-cholesterol (HDL-C) phenotype."
No. Sentence Comment
3 Carrier frequencies of common ABCA1 polymorphisms, R219K, V771M, V825I, I883M, E1172D, and R1587K were also assessed.
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8 Of the 6 common ABCA1 polymorphisms, very high HDL-C was associated with a higher genotype frequency for R219K (Ptrend ‫؍‬ 0.04) and higher genotype and allelic frequency for E1172D (Ptrend ‫؍‬ 0.0004, Ptrend ‫؍‬ 0.0002, respectively) compared with lower HDL-C.
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ABCA1 p.Arg219Lys 17383594:8:105
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17 doi:10.1016/j.trsl.2006.11.007 itating the egress of cholesterol and phospholipids from interstitial macrophages.2 To date, numerous functional mutations or single nucleotide polymorphisms in ABCA1 have been associated with low HDL-C.3,4 Structural mutations causing ABCA1 deficiency have been implicated in Tangler disease, a co-dominant disorder characterized by yellowish-orange engorgement of tonsils, hepatosplenomegaly, and very low HDL.5 A milder clinical phenotype, familial hypoalphalipoproteinemia (FHA), results from a single defective ABCA1 allele and occurs in the general population at the lower end of the HDL-C spectrum.6,7 Alternatively, at least 1 common ABCA1 polymorphism (ie, R219K) has been associated with a modified risk of CVD without significantly impacting HDL-C levels.8-11 In contrast, fewer data are available evaluating the extent to which variation in ABCA1 contributes to the high HDL-C phenotype,7,12 as previously characterized by reduced CVD risk.13 Therefore, this study evaluated subjects at the upper and lower tails of the HDL-C spectrum to assess the relative impact of novel mutations and common polymorphisms in ABCA1 on the HDL-C phenotype.
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ABCA1 p.Arg219Lys 17383594:17:699
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36 DNA was PCR amplified and digested using standard methods and the frequency of the 6 common polymorphisms (R219K, V771M, V825I, I883M, E1172D, and R1587K) in ABCA1, which was determined as described by Clee et al.8 Sequencing of PCR-amplified DNA.
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54 The prevalence of 6 common ABCA1 polymorphisms, R219K, V771M, V825I, I883M, E1172D, and R1587K was also evaluated.
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57 Very high HDL-C was associated with a higher genotype frequency of R219K (RK and KK, 68.2%; Ptrend ϭ 0.04) although allele frequency was not materially different.
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76 Finally, although this small sample size did not permit assessment of CVD risk for the R219K variant, a higher prevalence of the K allele was found among subjects with very high HDL-C, suggesting that carriers Table III.
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77 Genotype and allele frequencies for 6 common ABCA1 polymorphisms in subgroups with HDL-C defined as very high (n ϭ 22), high (n ϭ 34), average (n ϭ 36), or low (n ϭ 32) R219K Genotype frequencies P value Allele frequencies P valueR/R R/K K/K R K Very high 31.8% 45.5% 22.7% 0.04 0.55 0.45 0.20 High 45.7% 51.4% 2.9% 0.71 0.29 Average 43.2% 56.8% 0.0% 0.72 0.28 Low 50.0% 40.0% 10.0% 0.70 0.30 V771M V/V V/M M/M V M Very high 59.0% 36.0% 4.5% 0.11 0.77 0.23 0.04 High 85.7% 14.3% 0.0% 0.93 0.07 Average 86.1% 13.9% 0.0% 0.93 0.07 Low 80.0% 20.0% 0.0% 0.90 0.10 V825I V/V V/I I/I V I Very high 77.3% 22.7% 0.0% 0.58 0.89 0.11 0.62 High 88.6% 11.4% 0.0% 0.94 0.06 Average 88.9% 11.1% 0.0% 0.94 0.06 Low 82.8% 17.2% 0.0% 0.92 0.08 I883M I/I I/M M/M I M Very high 40.9% 45.5% 13.6% 0.29 0.64 0.36 0.05 High 60.0% 34.3% 5.7% 0.78 0.22 Average 73.0% 24.3% 2.7% 0.85 0.15 Low 66.7% 26.7% 6.7% 0.80 0.20 E1172D E/E E/D D/D E D Very high 68.2% 31.8% 0.0% 0.0004 0.82 0.18 0.0002 High 94.3% 5.7% 0.0% 0.97 0.03 Average 94.6% 5.4% 0.0% 0.97 0.03 Low 100.00% 0.0% 0.0% 1.00 0.00 R1587K R/R R/K K/K R K Very high 31.8% 50.0% 18.2% 0.16 0.57 0.43 0.07 High 65.6% 25.0% 9.4% 0.78 0.22 Average 55.6% 41.7% 2.8% 0.76 0.24 Low 51.9% 33.3% 14.8% 0.69 0.31 of R219K may have a basis for reduced CVD risk as previously suggested.8-11,24 CONCLUSION The data extend previous findings that novel mutations in ABCA1 are associated with the low rather than the high HDL-C (FHA) phenotype.
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16 doi:10.1016/j.trsl.2006.11.007 itating the egress of cholesterol and phospholipids from interstitial macrophages.2 To date, numerous functional mutations or single nucleotide polymorphisms in ABCA1 have been associated with low HDL-C.3,4 Structural mutations causing ABCA1 deficiency have been implicated in Tangler disease, a co-dominant disorder characterized by yellowish-orange engorgement of tonsils, hepatosplenomegaly, and very low HDL.5 A milder clinical phenotype, familial hypoalphalipoproteinemia (FHA), results from a single defective ABCA1 allele and occurs in the general population at the lower end of the HDL-C spectrum.6,7 Alternatively, at least 1 common ABCA1 polymorphism (ie, R219K) has been associated with a modified risk of CVD without significantly impacting HDL-C levels.8-11 In contrast, fewer data are available evaluating the extent to which variation in ABCA1 contributes to the high HDL-C phenotype,7,12 as previously characterized by reduced CVD risk.13 Therefore, this study evaluated subjects at the upper and lower tails of the HDL-C spectrum to assess the relative impact of novel mutations and common polymorphisms in ABCA1 on the HDL-C phenotype.
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ABCA1 p.Arg219Lys 17383594:16:699
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35 DNA was PCR amplified and digested using standard methods and the frequency of the 6 common polymorphisms (R219K, V771M, V825I, I883M, E1172D, and R1587K) in ABCA1, which was determined as described by Clee et al.8 Sequencing of PCR-amplified DNA.
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ABCA1 p.Arg219Lys 17383594:35:107
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53 The prevalence of 6 common ABCA1 polymorphisms, R219K, V771M, V825I, I883M, E1172D, and R1587K was also evaluated.
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56 Very high HDL-C was associated with a higher genotype frequency of R219K (RK and KK, 68.2%; Ptrend afd; 0.04) although allele frequency was not materially different.
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PMID: 16806540 [PubMed] Saleheen D et al: "A novel haplotype in ABCA1 gene effects plasma HDL-C concentration."
No. Sentence Comment
7 R219K, A399V and V771M polymorphisms did not show any association with levels of HDL-C, LDL-C, cholesterol and triglycerides.
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8 Haplotype analysis between R219K and V825L polymorphisms showed a unique interaction between R219 allele and L825 allele.
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50 Subjects were classified as having diabetes mellitus if he or she already Table 1 Methods for restriction fragment length polymorphism for screening of ABCA1 SNPs Variant Forward oligo (5VY3V), reverse oligo (5VY3V) Annealing temperature Enzyme Product (bp), wild-type allele, variant allele R219K (G1051A) ''aaagacttcaaggacccagctt``, ''cctcacattccgaaagcatta`` 62.5 -C EcoNI 309, 184, 125 V399A (T1591C) ''ctcattgtctgtgcttctcctc``, ''gtgaccagaaactcacctctcc`` 64.0 -C HphI 117, 71, 48, 188, 48 V771M (G2706A) ''tacaagtgagtgcttgggattg``, ''cccattggaaaagacaatcatc`` 60.0 -C BsaAI 254, 137, 391 V825L (G2868A) ''ttctgcaccttatgattgatcc``, ''agcacaaagaaaggacatcagc`` 62.5 -C BsaI 265, 127, 392 Polymerase chain reaction (PCR) was carried out using a Perkin Elmer GeneAmp PCR system 2400 (Perkin Elmer Corp., Applied Biosystems Division, USA).
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77 R219K, V399A and V771M polymorphisms did not show any association with levels of HDL-C, LDL-C, cholesterol and triglycerides.
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80 R219K, V399A and T774P polymorphisms followed the HWE however V825L and V771M showed a departure from HWE.
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82 Linkage disequilibrium and haplotype analysis R219K polymorphism was in significant linkage disequilibrium (LD) with V825L and V771M (DV=0.50; P-value<10À3 ).
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ABCA1 p.Arg219Lys 16806540:82:46
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92 On two-point haplotype analysis, the haplotype model between R219K and V825L polymorphisms showed RL haplotype to be associated with decreased levels of HDL-C. Importantly, this association remained significant when age, gender, hypertension and diabetes mellitus were introduced in to the haplotype model.
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ABCA1 p.Arg219Lys 16806540:92:61
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97 South Asian populations (from Pakistan, India, Bangladesh and Sri Lanka) represent a quarter of the developing world and harbor thirty percent of the global Table 4 Haplotype association analysis of the ABCA1 gene polymorphisms in relation with the HDL-C levels Haplotype Haplotype frequencies Haplotypic additive effects [95% CI] P-value R219K RV 0.47 + V825L RL 0.18 À0.12 [À0.22 to À0.03] 0.001 KV 0.28 À0.04 [À0.10 to 0.01] 0.15 KL 0.06 0.08 [À0.06 to 0.22] 0.25 T774P TV 0.21 0.03 [À0.05 to 0.12] 0.41 V825L TL 0.09 0.10 [À0.06 to 0.27] 0.22 PV 0.47 + PL 0.21 À0.06 [À0.14 to 0.02] 0.15 R219K RM 0.55 + V771M RV 0.07 À0.13 [À0.45 to 0.19] 0.41 KM 0.34 À0.02 [À0.09 to 0.05] 0.54 KV 0.04 0.07 [À0.12 to 0.27] 0.46 Table 3 Mean HDL-C levels (S.D.) for the genotypes and alleles of the studied polymorphisms Frequencies HDL-C (S.D.) b (95% CI) P-value R219K RR 39.8 1.06 (0.30) À0.02 (À0.16 to 0.13) 0.85 RK 46.0 1.10 (0.28) 0.00 (À0.14 to 0.14) 0.99 KK 14.3 1.10 (0.31) + R 62.7 1.08 (0.26) 0.01 (À0.05 to 0.07) 0.79 K 37.3 1.09 (0.31) V399A AA 6.0 1.01 (0.23) À0.03 (À0.24 to 0.16) 0.70 AV 34.7 1.11 (0.28) 0.10 (À0.04 to 0.16) 0.22 VV 59.3 1.04 (0.31) + A 23.3 1.09 (0.28) À0.03 (À0.10 to 0.05) 0.58 V 76.7 1.04 (0.31) T774P PP 9.6 1.10 (0.31) 0.20 (0.01 to 0.40) 0.03 PT 37.5 1.03 (0.32) 0.13 (À0.03 to 0.20) 0.14 TT 52.9 0.97 (0.28) + P 28.4 1.05 (0.32) À0.15 (À0.18 to À0.02) 0.01 T 71.6 0.99 (0.29) V771M MM 6.1 1.09 (0.30) 0.01 (À0.24 to 0.25) VM 10.1 0.98 (0.24) À0.07 (À0.27 to 0.12) 0.46 VV 83.8 1.07 (0.29) + 0.94 M 11.1 1.04 (0.27) 0.03 (À0.10 to 0.15) 0.71 V 88.9 1.07 (0.29) V825L LL 9.8 0.89 (0.299) À0.17 (À0.32 to À0.19) 0.02 LV 32.8 1.06 (0.265) À0.03 (À0.11 to 0.076) 0.70 VV 57.5 1.07 (0.30) + L 26.1 1.07 (0.29) 0.10 (À0.00 to .13) 0.05 V 73.9 1.00 (0.28) P-values are adjusted for age and gender.
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ABCA1 p.Arg219Lys 16806540:97:339
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ABCA1 p.Arg219Lys 16806540:97:588
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ABCA1 p.Arg219Lys 16806540:97:848
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107 On haplotype analysis, the RL haplotype generated from the R219K and V825L polymorphisms was strongly associated with decreased levels of HDL-C. Importantly, association of this haplotype was stronger than the association observed for V825L polymorphism.
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ABCA1 p.Arg219Lys 16806540:107:59
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113 R219K is the most widely studied polymorphism in association with coronary artery disease, atherosclerosis and HDL-C levels [21,23,24,28].
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PMID: 17135600 [PubMed] Porchay I et al: "ABCA1 single nucleotide polymorphisms on high-density lipoprotein-cholesterol and overweight: the D.E.S.I.R. study."
No. Sentence Comment
6 The aim of this study was to assess the effect of three polymorphisms, C69T, G378C, and G1051A (R219K), on HDL-C levels and their interaction with BMI in more than 5000 French whites from the D.E.S.I.R. (Data from an Epidemiological Study on the Insulin Resistance syndrome) cohort study.
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27 We analyzed two SNPs with a potential regulating role located in 5Ј-untranslated regions, C69T (rs1800977) and G378C (rs1800978) (5), and one SNP G1051A (rs2230806) (6) leading to an amino acid substitution, R219K, in a large cohort from the D.E.S.I.R. (Data from an Epidemiological Study on the Insulin Resistance syndrome) Study (18).
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ABCA1 p.Arg219Lys 17135600:27:214
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74 The G1051A SNP controls the substitution of arginine 219 by a lysine in the first extracellular domain of ABCA1.
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PMID: 16313984 [PubMed] Martin M et al: "ABCA1 polymorphisms and prognosis after myocardial infarction in young patients."
No. Sentence Comment
9 In order to know whether there is a relationship between ABCA1 polymorphisms and prognosis after myocardial infarction in young patients, we have analysed three polymorphisms in ABCA1 gene (À477C/T, R219K, I883M) in a cohort of young male survivors of first myocardial infarction.
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ABCA1 p.Arg219Lys 16313984:9:199
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19 Table 1 Frequency of genotypes of ABCA1 gene in study and control group Genotypes Patients (%) Controls (%) p ABCA1 R219K RR 48 49 ns RK 42 40 KK 10 11 ABCA1 À477C/T CC 24 30 ns TC 50 50 TT 26 20 ABCA1 I883M AA 69 80 ns AG/GG 31 20 International Journal of Cardiology 110 (2006) - 268 www.elsevier.com/locate/ijcard Fasting blood samples were drawn for measurements of total plasma cholesterol, HDL-C and triglycerides in the first 24 h after admission.
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PMID: 16540294 [PubMed] Kaminski WE et al: "ABC A-subfamily transporters: structure, function and disease."
No. Sentence Comment
80 On the other hand, one dimorphism in the ABCA1 gene, R219K, appears to exert atheroprotective effects [30].
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PMID: 16157450 [PubMed] Shibata N et al: "Association studies of cholesterol metabolism genes (CH25H, ABCA1 and CH24H) in Alzheimer's disease."
No. Sentence Comment
71 In a previous study, investigating sporadic AD patients, the A-allele of the non-synonymous R219K SNP (rs2230806) in ABCA1 was associated with a reduction of total cholesterol in cerebrospinal fluid and a delay in age-at-onset [17].
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72 However, the current study failed to detect a significant effect of the R219K variation on age-at-onset.
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PMID: 16704350 [PubMed] Brunham LR et al: "Variations on a gene: rare and common variants in ABCA1 and their impact on HDL cholesterol levels and atherosclerosis."
No. Sentence Comment
605 Many of these variants have been studied in relationship to their association with HDL cholesterol levels and atherosclerosis (11, 15, 22, 27, 28, 38, TABLE 4 Nonsynonymous single-nucleotide polymorphisms (SNPs) in ABCA1 SNP id Nucleotidea Amino acidb Observed heterozygosity rs2230806 G969A R219K 0.488 rs9282541 C1001T R230C 0.029 rs9282543 T1509C V399A 0.020 rs4131108 A1556C M415L - rs13306068 A1949G I546V - rs2066718 G2624A V771M 0.074 rs2472458 G2804A D831N - rs4149313 A2962G I883M - rs2482437 C3326T E1005K - rs13306072 G3473A V1054I - rs13306073 G3599A V1096I - rs1997618 T4977C I1555T - rs2230808 A5073G K1587R 0.480 rs1883024 T5256C L1648P - - C5505G S1731C - a Nucleotide position is with respect to NM 005502. b Amino acid position is with respect to NP 005493.
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ABCA1 p.Arg219Lys 16704350:605:295
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622 Notably, only two of the 15 common ABCA1 nonsynonymous SNPs, I883M and R219K,arerepresentedintheHapMapdataset,whichisanincompletedataset(the phaseIprojecthavingsetouttoidentify1SNPevery5000basepairs)(7).However, it is apparent from the haplotypes in which I883M and R219K reside that the minor alleles of each of these are unique to one particular, different haplotype, which may explain in part why these two SNPs have been consistently found to be associated with HDL levels and atherosclerosis risk.
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763 The association of the R219K polymorphism in the ATP-binding cassette transporter 1 (ABCA1) gene with coronary artery disease and hyperlipidemia.
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974 R219K polymorphism of the ABCA1 gene and its modulation of the variations in serum high-density lipoprotein cholesterol and triglycerides related to age and adiposity in white versus black young adults.
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PMID: 16446539 [PubMed] Andrikovics H et al: "Decreased frequencies of ABCA1 polymorphisms R219K and V771M in Hungarian patients with cerebrovascular and cardiovascular diseases."
No. Sentence Comment
0 Fax +41 61 306 12 34 E-Mail karger@karger.ch www.karger.com Original Paper Cerebrovasc Dis 2006;21:254-259 DOI: 10.1159/000091223 Decreased Frequencies of ABCA1 Polymorphisms R219K and V771M in Hungarian Patients with Cerebrovascular and Cardiovascular Diseases Hajnalka Andrikovicsa Endre Pongráczb Ákos Kalinac Anikó Szilvásia Charalampos Aslanidisd Gerd Schmitzd Attila Tordaia a Department of Molecular Genetics, National Medical Center, b Neurology Department, Central Hospital, Ministry of Interior, and c Hospital of the National Railways, Budapest, Hungary; d Institute for Clinical Chemistry and Laboratory Medicine, University of Regensburg, Germany and 0 8 1.6%, respectively) were decreased.
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1 V771M was almost exclusively (35/36) found in individuals carrying the R219K allele.
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ABCA1 p.Arg219Lys 16446539:1:71
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2 Conclusions: Our data confirm earlier observations that ABCA1 R219K and V771M polymorphisms may be associated with a protective role against CHD and extend those to another important pathologic condition, namely stroke.
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7 Methods: We investigated 244 unrelated, consecutively enrolled patients with ischemic stroke, 150 patients with coronary heart disease (CHD) and 193 blood donors for allele frequencies (AFs) of three common ABCA1 polymorphisms (R219K, V771M and I883M).
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ABCA1 p.Arg219Lys 16446539:7:228
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8 Results: Compared to controls (30.8 8 4.7 and 4.9 8 2.2%, respectively), decreased AFs were found in both patient groups for R219K and V771M (28.7 8 4.1 and 3.1 8 1.6% in stroke, and 25.7 8 5.0%; 1.3 8 1.3% in CHD patients, respectively).
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10 Similarly, among CHD patients younger than 60, AFs of R219K and V771M (22.6 8 7.5 Received: July 25, 2005 Accepted: October 12, 2005 Published online: January 27, 2006 Attila Tordai Department of Molecular Genetics National Medical Center, Diószegi út 64 HU-1113 Budapest (Hungary) Tel./Fax +36 1 385 2255, E-Mail tordai@biomembrane.hu (c) 2006 S. Karger AG, Basel 1015-9770/06/0214-$23.50/0 Accessible online at: www.karger.com/ced To date, the ABCA1 gene proved to be highly polymorphic with large numbers of sequence variations leading to amino acid changes or affecting the putative promoter region [8] (see also http://www.abca1 mutants.all.at).
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28 DNA Isolation and Detection of ABCA1 R219K, V771M and I883M Alleles with LightCycler Hybridization Probe Technique DNA isolation was performed from anticoagulated peripheral blood with the standard 'salting-out` procedure.
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ABCA1 p.Arg219Lys 16446539:28:37
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29 The following ABCA1sequencevariantswerestudied:R219K(exon7,c.969A]G, substitution of Arg219 by Lys); V771M (exon 16, c.2624G]A, substitution of Val771 by Met), and I883M (exon 18, c.2962A]G, substitution of Ile883 by Met).
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53 2006;21:254-259256 Results Genotyping for R219K, V771M and I883M ABCA1 Allelic Variants Using genomic DNA samples, simultaneous genotyping was carried out in the control blood donor and the stroke- and CHD-affected patient groups by PCR and fluorescent allelic discrimination techniques.
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55 In the control group, AF figures (30.8 8 4.7, 4.9 8 2.2 and 12.4 8 4.5%) were found in the expected range for R219K, V771M and I883M, respectively.
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ABCA1 p.Arg219Lys 16446539:55:110
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56 Decreased AFs were found in both patient groups for R219K and V771M variants (28.9 8 4.1 and 3.3 8 1.6% in stroke, and 25.7 8 5.0% and 1.3 8 1.3% in CHD, respectively).
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59 In a subset of stroke patients with disease onset before 50 (n = 114), both variants occurred in significantly lower frequencies compared to the control group [R219K: 22.4 8 5.5%, p = 0.013, crude OR = 0.55 (0.34-0.88); V771M: 1.8 8 1.7%, p = 0.045, crude OR = 0.33 (0.111.00)].
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60 A similar tendency was observed in the CHD group in a subset of patients younger than 60 (n = 62) for R219K and V771M, but only the V771M AF decrease was significant [22.6 8 3.6%, p 1 0.05; and 0 8 1.6%, p = 0.005, crude OR = 0.07 (0.004-1.2)].
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ABCA1 p.Arg219Lys 16446539:60:102
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62 Figure 1 further illustrates the tendency of R219K and V771M AF decreases following stratification of the patient groups by age at onset.
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63 Multivariate analyses (logistic regression) also showed that the R219K and V771M variants are protective factors against stroke, independently from age and sex [R219K: p = 0.032, adjusted OR: 0.68 (0.48-0.97); V771M: p = 0.017, adjusted OR: 0.34 (0.14-0.82)].
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ABCA1 p.Arg219Lys 16446539:63:65
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ABCA1 p.Arg219Lys 16446539:63:161
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66 Similarly to results of the entire stroke group, R219K AF reduction was 27.4 8 4.9%, p = 0.015, adjusted OR: 0.59 (0.39-0.91), and V771M AF reduction was 3.3 8 2.0%, p = 0.042, adjusted OR: 0.36 (0.13-0.97) compared to control.
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67 We also observed significant R219K and V771M AF reduction in patients with CT-proven ischemic stroke [n = 124; R219K: 24.6 8 5.5%, p = 0.049, adjusted OR: 0.64 (0.41-0.99), and V771M: 1.2 8 1.4%, p = 0.021, adjusted OR: 0.19 (0.05-0.78)] compared to control.
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ABCA1 p.Arg219Lys 16446539:67:29
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70 Genotyping results and statistical analyses for three common ABCA1 polymorphisms (R219K, V771M and I883M) in the control and patient groups Polymorphism AF % (895% CI) Heterozygous individuals n (%) Homozygous individuals n (%) p value Adjusted OR (95% CI) R219K Controls (n = 193) 30.8 (4.7) 73 (37.8) 23 (11.9) Patients with stroke (n = 244) 28.9 (4.1) 84 (34.1) 29 (11.8) 0.032 0.68 (0.48-0.97) Patients with CHD (n = 150) 25.7 (5.0) 55 (36.7) 11 (7.3) NS NS V771M Controls (n = 193) 4.9 (2.2) 19 (9.8) 0 Patients with stroke (n = 244) 3.3 (1.6) 14 (5.7) 1 (0.4) 0.017 0.34 (0.14-0.82) Patients with CHD (n = 150) 1.3 (1.3) 4 (2.7) 0 0.027 0.08 (0.01-0.75) I883M Controls (n = 105) 12.4 (4.5) 24 (22.9) 1 (1.0) Patients with stroke (n = 244) 15.2 (3.2) 61 (24.8) 7 (2.9) NS NS Patients with CHD (n = 150) 12.3 (3.8) 29 (19.3) 4 (2.6) NS NS AF = Allele frequency; CI = confidence interval; NS = nonsignificant.
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ABCA1 p.Arg219Lys 16446539:70:82
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72 showed that R219K and V771M variants also play a protective role against stroke independently from age and sex in the stroke patient subgroup without ischemic heart disease [R219K: p = 0.040, adjusted OR: 0.69 (0.48-0.98), and V771M: p = 0.034, adjusted OR: 0.39 (0.16-0.93)].
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ABCA1 p.Arg219Lys 16446539:72:12
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73 These results indicate that the protective role of R219K and V771M in the stroke group cannot be explained with the frequent coexistence of CHD.
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78 We observed lower R219K and V771M AFs in the low-risk group (R219K: 27.4 8 5.2 vs. 30.6 8 6.6%, and V771M: 2.1 8 1.7 vs. 4.6 8 3.0%, respectively), but the differences were not significant.
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ABCA1 p.Arg219Lys 16446539:78:18
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81 However, the genotype distribution of R219K showed a significant (p = 0.00465) alteration from HWE exclusively in the stroke-affected patient group.
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84 The V771M allele was almost exclusively found in individuals carrying the R219K allele (36/37 V771M carriers were positive for R219K).
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ABCA1 p.Arg219Lys 16446539:84:74
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86 0.0005 by the Arlequin software) was observed between V771M and R219K.
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87 Moreover, a similar, non-random allelic association was observed between R219K and I883M variants (p !
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89 Combining all genotyping results, 94/135 (69.6%) of I883M carriers were also positive for R219K, while only 148/374 (39.6%) of I883M wild-type individuals were positive for R219K.
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ABCA1 p.Arg219Lys 16446539:89:90
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90 The distribution of double-positive (R219K and I883M carriers) and single-positive (only I883M carriers) individuals was similar in the control, in the stroke and in the CHD-affected groups.
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91 These results suggest that the R219K and I883M polymorphisms are also in linkage disequilibrium in our population, although the common occurrence of these variants in the same individual is not likely to be related to disease development.
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94 Comparisons of AFs of the ABCA1 R219K and V771M variants in the control and patient groups.
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96 AF values and 95% CIs (bars) are presented for the R219K (a) and V771M (b) variants.
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106 The most common missense polymorphism in the coding region of the ABCA1 gene is R219K with an AF of the K allele of 25-46% in the Caucasian population.
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107 Two large studies investigating 2,028 and 794 individuals came to contradictory conclusions about the possible role of R219K in arteriosclerosis.
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108 Brousseau et al. [15] reported an elevated R219K AF in patients with CHD and a low HDL level compared to disease-free individuals, suggesting that the mutant allele may cause a decrease in the HDL level, subsequently promoting arteriosclerosis and the development of CHD.
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109 In their study, no correlation between R219K genotypes and the plasma lipid parameters could be observed either in the control group (mean age: 53 years) or in the CHD patient group (mean age: 64 years).
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110 In another study, primarily focusing on ABCA1 haplotype analyses, R219K was also found to be associated with an increased risk for myocardial infarction [16].
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111 In contrast, Clee et al. [9] found that R219K carrier patients have reduced severity of CHD, decreased focal and diffuse arteriosclerosis and fewer coronary events than wild-type CHD patients.
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112 They showed decreased triglyceride and increased HDL levels in their R219K carrier patients, although this difference existed only in the individuals younger than 57 years.
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113 They concluded that R219K alone is an independent protective factor against CHD.
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114 Further studies also described a putative protective effect of the R219K variant [18-20].
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117 Moreover, the mean age of R219K homozygous and heterozygous patients with stroke was significantly higher than the age of R219K wild-type patients (58.2 8 13.0, 55.4 8 13.8 vs. 51.2 8 14.9 years, respectively).
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118 In our CHD patient group, the mean age of the patients with different R219K genotype did not differ significantly.
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ABCA1 p.Arg219Lys 16446539:118:70
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119 However, upon subgroup analyses, among patients affected by both diseases with younger ages at onset, both variants R219K and V771M showed significantly decreased AFs (fig. 1).
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121 They explained this observation with the linkage disequilibrium between the R219K and V771M variants.
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122 In our study, the V771M variant, or compound heterozygosity for V771M and R219K, showed significant AF reduction in the patient groups, in spite of the fact that our controls were relatively younger than our patients with stroke or CHD.
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128 Our data confirm earlier observations that ABCA1 R219K and V771M polymorphisms may play a protective role against CHD and extend those to another frequently occurring pathologic condition, namely stroke.
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PMID: 16372134 [PubMed] Katzov H et al: "Quantitative trait loci in ABCA1 modify cerebrospinal fluid amyloid-beta 1-42 and plasma apolipoprotein levels."
No. Sentence Comment
1 Here, genetic association of the common R219K variant of ABCA1 is shown with cerebrospinal fluid (CSF) Ab1-42 levels, reinforcing emerging evidence of a connection between lipid and Ab metabolism.
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7 No other genetic markers in ABCA1 exhibit effects as large as R219K, although a modest independent effect of R1587K was observed.
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40 Genotyping Information on the R219K, I883M, and R1587K variants [representing cDNA (GenBank accession number NM_005502.2) rs2230806, c.658 G>A; rs4149313, c.2650 A>G; rs2230808, c.4762 G>A, respectively] may be found at dbSNP (http://www.ncbi.nlm.nih.gov/ SNP/).
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70 We focussed on the R219K, I883M, and R1587K variants since these give rise to amino acid changes and because they are common in European populations (Clee et al. 2001).
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72 A significant effect of the R219K variant on CSF Ab1-42 levels was observed whereby RK heterozygotes had the highest trait levels (547±19.2, n=141; 658±35.1, n=71; 443±60.6, n=4; F2,212=6.2, P=0.0024, for RR, RK, and KK genotype classes, respectively; pg/ ml ±SEM).
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ABCA1 p.Arg219Lys 16372134:72:19
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88 In an initial screen, we tested the R219K variant using ANOVA for effects upon these selected traits in the entire set of samples.
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96 To begin exploring this latter possibility in the CVD sample (since it affords the most power to detect such effects), genotyping of the I883M and R1587K variants was performed, and ANOVA used to model the potential independent main effects in a joint analysis of all three markers (including R219K).
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98 In smokers, the main effect for R219K improved when adjusting for the other sites from F2,943=8.4, P=0.00024 in isolation to F2,898=9.9, P=0.000055 when all three markers were included.
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ABCA1 p.Arg219Lys 16372134:98:32
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100 The I883M variant was not associated with the APOB trait either in isolation or in the full model.
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122 To explore the possible functional effects of ABCA1 variants, we used the PolyPhen tool (http://www.bor Table 1 Quantitative trait analyses for the R219K variant.
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126 HDL-C High density lipoprotein cholesterol, LDL-C low density lipoprotein cholesterol, TC total cholesterol, TG triglycerides Table 2 Phenotypic effects of the R219K variant in smokers and non-smokers ApoB KK RK RR F value P value Non-smokers 1.56±0.04 (102) 1.51±0.02 (573) 1.50±0.01 (878) 1.1 0.32 Smokers 1.80±0.06 (53) 1.56±0.02 (366) 1.62±0.02 (527) 8.4 0.00024 TC Non-smokers 6.06±0.11 (102) 5.97±0.04 (574) 5.93±0.04 (879) 0.84 0.43 Smokers 6.62±0.16 (53) 6.14±0.06 (367) 6.15±0.05 (526) 4.0 0.019 LDL-C Non-smokers 4.14±0.10 (102) 4.03±0.04 (568) 3.99±0.03 (868) 1.34 0.26 Smokers 4.54±0.16 (50) 4.13±0.05 (355) 4.17±0.05 (516) 3.5 0.031 Values are the mean ± SEM according to R219K genotype.
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127 The number of individuals in each category is shown in parenthesis. Comparisons were performed by ANOVATC total cholesterol, LDL-C low density lipoprotein cholesterol Traits KK RK RR F value P value APOA1a (g/l) 1.46±0.02 (157) 1.48±0.01 (966) 1.47±0.01 (1,439) 0.23 0.79 APOB (g/l) 1.64±0.03 (157) 1.53±0.01 (966) 1.55±0.01 (1,439) 5.4 0.0046 HDL-C (mmol/l) 1.16±0.26 (156) 1.20±0.01 (961) 1.20±0.01 (1,427) 1.1 0.34 LDL-C (mmol/l) 4.26±0.86 (154) 4.08±0.03 (951) 4.05±0.03 (1,415) 0.26 0.038 TC (mmol/l) 6.24±0.09 (157) 6.04±0.04 (969) 6.01±0.03 (1,439) 3.02 0.049 TGa (mmol/l) 1.87±0.11 (157) 1.71±0.04 (969) 1.72±0.03 (1,441) 1.38 0.25 a Log-transformed traits k.embl-heidelberg.de/PolyPhen/) (Ramensky et al. 2002) for five coding SNPs (cSNPs) in ABCA1 (R219K rs2230806; V771M rs2066718; V825I rs4149312; I883M rs2066714; R1587K rs2230808) (Frikke-Schmidt et al. 2004).
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128 As a control we also tested the APOE-e4 (R130C rs428358) variant.
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153 MI Myocardial infarction R219K (rs2230806) KK RK RR P value Smokers MI 29 (0.05) 205 (0.39) 293 (0.56) 0.98 Controls 24 (0.06) 162 (0.38) 236 (0.56) Non-smokers MI 35 (0.06) 198 (0.36) 314 (0.57) 0.87 Controls 67 (0.67) 377 (0.37) 566 (0.56) I883M (rs4149313) II IM MM Smokers MI 418 (0.76) 127 (0.23) 4 (0.01) 0.14 Controls 349 (0.81) 77 (0.18) 3 (0.01) Non-smokers MI 445 (0.78) 115 (0.2) 12(.02) 0.31 Controls 843 (0.81) 184 (0.18) 16 (0.02) R1587K (rs2230808) (rs2230808) KK RK RR Smokers MI 29 (0.05) 160 (0.30) 342 (0.64) 0.025 Controls 14 (0.03) 159 (0.38) 250 (0.59) Non-smokers MI 25 (0.04) 182 (0.33) 346 (0.62) 0.66 Controls 57 (0.05) 329 (0.32) 650 (0.63) also serve as a point to revisit in large published studies, such as that of Frikke-Schmidt et al. (2004).
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159 Fig. 2 Diplotype analysis of quantitative traits considering the joint contributions of the R219K and R1587K variants.
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160 Categories represent the diplotype configurations of each individual from among four possible haplotypes (RR, KK, RK, and KR, where R219K is at the first position).
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164 The highest trait levels occur in individuals that are homozygous for the K variant of R219K and homozygous for the R variant of R1587K.
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166 Among discovered and examined variable sites, the best evidence for potentially functional polymorphism is for the commonly studied R219K and R1587K variants (Tregouet et al. 2004).
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6 No other genetic markers in ABCA1 exhibit effects as large as R219K, although a modest independent effect of R1587K was observed.
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39 Genotyping Information on the R219K, I883M, and R1587K variants [representing cDNA (GenBank accession number NM_005502.2) rs2230806, c.658 G>A; rs4149313, c.2650 A>G; rs2230808, c.4762 G>A, respectively] may be found at dbSNP (http://www.ncbi.nlm.nih.gov/ SNP/).
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74 A significant effect of the R219K variant on CSF Ab1-42 levels was observed whereby RK heterozygotes had the highest trait levels (547&#b1;19.2, n=141; 658&#b1;35.1, n=71; 443&#b1;60.6, n=4; F2,212=6.2, P=0.0024, for RR, RK, and KK genotype classes, respectively; pg/ ml &#b1;SEM).
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90 In an initial screen, we tested the R219K variant using ANOVA for effects upon these selected traits in the entire set of samples.
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124 To explore the possible functional effects of ABCA1 variants, we used the PolyPhen tool (http://www.bor Table 1 Quantitative trait analyses for the R219K variant.
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129 The number of individuals in each category is shown in parenthesis. Comparisons were performed by ANOVATC total cholesterol, LDL-C low density lipoprotein cholesterol Traits KK RK RR F value P value APOA1a (g/l) 1.46&#b1;0.02 (157) 1.48&#b1;0.01 (966) 1.47&#b1;0.01 (1,439) 0.23 0.79 APOB (g/l) 1.64&#b1;0.03 (157) 1.53&#b1;0.01 (966) 1.55&#b1;0.01 (1,439) 5.4 0.0046 HDL-C (mmol/l) 1.16&#b1;0.26 (156) 1.20&#b1;0.01 (961) 1.20&#b1;0.01 (1,427) 1.1 0.34 LDL-C (mmol/l) 4.26&#b1;0.86 (154) 4.08&#b1;0.03 (951) 4.05&#b1;0.03 (1,415) 0.26 0.038 TC (mmol/l) 6.24&#b1;0.09 (157) 6.04&#b1;0.04 (969) 6.01&#b1;0.03 (1,439) 3.02 0.049 TGa (mmol/l) 1.87&#b1;0.11 (157) 1.71&#b1;0.04 (969) 1.72&#b1;0.03 (1,441) 1.38 0.25 a Log-transformed traits k.embl-heidelberg.de/PolyPhen/) (Ramensky et al. 2002) for five coding SNPs (cSNPs) in ABCA1 (R219K rs2230806; V771M rs2066718; V825I rs4149312; I883M rs2066714; R1587K rs2230808) (Frikke-Schmidt et al. 2004).
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155 MI Myocardial infarction R219K (rs2230806) KK RK RR P value Smokers MI 29 (0.05) 205 (0.39) 293 (0.56) 0.98 Controls 24 (0.06) 162 (0.38) 236 (0.56) Non-smokers MI 35 (0.06) 198 (0.36) 314 (0.57) 0.87 Controls 67 (0.67) 377 (0.37) 566 (0.56) I883M (rs4149313) II IM MM Smokers MI 418 (0.76) 127 (0.23) 4 (0.01) 0.14 Controls 349 (0.81) 77 (0.18) 3 (0.01) Non-smokers MI 445 (0.78) 115 (0.2) 12(.02) 0.31 Controls 843 (0.81) 184 (0.18) 16 (0.02) R1587K (rs2230808) (rs2230808) KK RK RR Smokers MI 29 (0.05) 160 (0.30) 342 (0.64) 0.025 Controls 14 (0.03) 159 (0.38) 250 (0.59) Non-smokers MI 25 (0.04) 182 (0.33) 346 (0.62) 0.66 Controls 57 (0.05) 329 (0.32) 650 (0.63) also serve as a point to revisit in large published studies, such as that of Frikke-Schmidt et al. (2004).
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161 Fig. 2 Diplotype analysis of quantitative traits considering the joint contributions of the R219K and R1587K variants.
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162 Categories represent the diplotype configurations of each individual from among four possible haplotypes (RR, KK, RK, and KR, where R219K is at the first position).
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168 Among discovered and examined variable sites, the best evidence for potentially functional polymorphism is for the commonly studied R219K and R1587K variants (Tregouet et al. 2004).
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PMID: 16207713 [PubMed] Koldamova R et al: "Lack of ABCA1 considerably decreases brain ApoE level and increases amyloid deposition in APP23 mice."
No. Sentence Comment
233 Wollmer et al. (20) found that the R219K variant of ABCA1, associated with increased HDL-cholesterol levels and a decreased risk of atherosclerosis (43), delayed the age of onset of LOAD.
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ABCA1 p.Arg219Lys 16207713:233:35
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229 Wollmer et al. (20) found that the R219K variant of ABCA1, associated with increased HDL-cholesterol levels and a decreased risk of atherosclerosis (43), delayed the age of onset of LOAD.
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PMID: 16207707 [PubMed] Hirsch-Reinshagen V et al: "The absence of ABCA1 decreases soluble ApoE levels but does not diminish amyloid deposition in two murine models of Alzheimer disease."
No. Sentence Comment
335 Wollmer et al. (74) reported that the R219K gain-of-function single nucleotide polymorphism in ABCA1 (R219K) has been suggested to delay the age of onset of AD by 1.6 years.
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ABCA1 p.Arg219Lys 16207707:335:38
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336 Katzov et al. (75) reported significant associations with the R219K, R1587K, and V771M on AD in single marker and haplotype analyses conducted on European subjects.
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ABCA1 p.Arg219Lys 16207707:336:38
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ABCA1 p.Arg219Lys 16207707:336:62
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337 Katzov et al. (75) reported significant associations with the R219K, R1587K, and V771M on AD in single marker and haplotype analyses conducted on European subjects.
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PMID: 15935359 [PubMed] Hodoglugil U et al: "Common polymorphisms of ATP binding cassette transporter A1, including a functional promoter polymorphism, associated with plasma high density lipoprotein cholesterol levels in Turks."
No. Sentence Comment
3 The rare alleles of C-14T and V771M polymorphisms were associated with higher HDL-C levels in men and, in combination with the rare alleles of R219K and I883M, respectively, with higher HDL-C in both sexes.
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8 The C-14T and R219K polymorphisms were on different haplotype blocks.
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11 In conclusion, we describe a functional promoter polymorphism (C-14T) and a coding sequence variant (V771M) of ABCA1 and their interactions with two other variants (R219K and I883M) on plasma HDL-C levels in Turks.
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21 Some common polymorphisms of ABCA1, including R219K 0021-9150/$ - see front matter (c) 2005 Elsevier Ireland Ltd. All rights reserved.
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31 In onestudy,wheremalesandfemaleswereanalyzedseparately, R219K and I883M were associated with elevated HDL-C levels in females only [9].
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104 The G-803A Table 2 ABCA1 polymorphisms Nucleotide changea Carrier of rare allele (%) Rare allele (%) nb Referencesc Frequency in 5 and promoter regions G-803A ~10 92/141 [19] T-564C 72.7 47.7 728/1268 [18] G-407C 62.5 40.7 220/233 [18] G-99C 42.2 24.2 875/1130 [46] C-14T 61.2 37.7 916/1416 [46] InsG 319 26.6 14.2 848/1288 [46] Nucleotide changed Amino acid change Exon Carrier of rare allele (%) Rare allele (%) nb Referencesc Frequency in coding sequence Nonsynonymous G(70943)A R219K 7 62.3 38.5 996/1466 db 2230806 G(102555)A V771M 16 10.0 5.1 981/1477 db 2066718 G(103777)A V825I 17 12.3 6.2 960/1145 db 4149312 A(105057)G I883M 18 38.1 21.8 1084/1448 db 4149313 G(112177)C E1172D 24 9.0 4.6 1001/1237 [12,13] A(116887)G Q1328R 28 0.003e 0.0015 172/156 NR G(129004)A R1587K 35 55.1 33.0 937/1351 db 2230808 T(133402)C Y1767H 39 ~1.0e 40/55 NR G(133420)A V1773M 39 ~1.0e 40/55 NR Synonymous C(100538)A I620I 15 ~4.0 40/55 NR C(109469)T V990V 21 ~3.0 87/90 [17] T(109861)G V1053V 22 ~1.0 90/90 [12] C(109868)T L1056L 22 ~5.0 90/90 NR C(109906)T R1068R 22 ~3.0 90/90 NR A(113280)G E1211E 25 ~4.0 40/55 [17] A(116879)G T1325T 28 ~1.0 40/55 NR T(137043)C Y1921Y 43 ~1.0 40/55 NR Nucleotide changed Intron Carrier of rare allele (%) Intronic location nb Referencesc Frequency in noncoding sequence G(23816)A 1 ~1.0 11 bp 5 exon 1b 94 NR G(23819)C 1 42 8 bp 5 exon 1b 94 NR A(22997)T 1 46 90 bp 5 exon 1d 91 NR A(23004)G 1 ~1.0 83 bp 5 exon 1d 91 NR G(23058)C 1 46 29 bp 5 exon 1d 91 NR G(40504)A 3 2.6 26 bp 3 of exon 3 192 NR C(45217)T 4 0.7 64 bp 3 of exon 4 142 NR T(98628)A 14 35-40 24 bp 3 of exon 14 190 db 4743763 C(100332)T 14 4.3 59 bp 5 of exon 15 90 db 2066717 C(108020)T 19 0.7 3 bp 5 of exon 20 144 NR DelTTT(134503-6) 39 7.0 20-23 bp 5 of exon 40 90 NR C(142026)T 46 8.6 34 bp 5 of exon 47 116 NR A(142751)G 48 15.9 13 bp 3 of exon 48 107 NR a Relative to transcriptional start.
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ABCA1 p.Arg219Lys 15935359:104:482
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109 Table 3 ABCA1 polymorphisms and mean plasma HDL-C levels (mg/dl ± S.D.) in a random Turkish population Females Males AAa AB BB AAa AB BB Promoter and 5 region T-564C 40.4 ± 8.4 (205) 41.0 ± 7.9 (365) 39.9 ± 7.6 (158) 35.6 ± 7.4 (339) 35.5 ± 6.5 (635) 34.9 ± 6.5 (294) G-407C 41.3 ± 11.2 (82) 40.7 ± 7.7 (101) 40.7 ± 12.2 (37) 35.7 ± 6.9 (88) 35.3 ± 6.7 (96) 35.4 ± 7.4 (49) G-99C 40.7 ± 7.5 (505) 41.0 ± 7.2 (317) 41.3 ± 8.4 (53) 35.1 ± 6.5 (654) 35.0 ± 6.3 (405) 34.9 ± 6.5 (71) C-14T 41.3 ± 9.0 (361) 41.0 ± 9.0 (417) 41.0 ± 9.4 (138) 34.8 ± 7.0b (547) 35.5 ± 7.5 (675) 36.7 ± 8.1b (194) InsG 319 41.3 ± 8.1 (641) 40.5 ± 7.7 (193) 43.1 ± 8.0 (14) 35.3 ± 6.4 (933) 34.7 ± 6.4 (332) 34.5 ± 6.5 (23) Nonsynonymous R219K 41.2 ± 9.4 (364) 40.8 ± 8.6 (480) 41.2 ± 10 (152) 35.2 ± 7.3 (574) 35.3 ± 7.3 (688) 35.2 ± 7.6 (204) V771M 40.9 ± 9.2 (896) 42.8 ± 9.3 (82) 38.7 ± 10 (3) 35.1 ± 7.2c (1330) 37.1 ± 8.0c (144) 45.7 ± 10.7 (3) V825I 40.6 ± 9.4 (842) 38.9 ± 8.5 (117) 42 (1) 35.8 ± 8.7 (1005) 37.1 ± 9.5 (140) (-) I883M 41.1 ± 9.5 (643) 40.8 ± 8.4 (372) 41.4 ± 9.1 (69) 35.0 ± 7.0 (922) 35.7 ± 8.0 (457) 35.6 ± 7.4 (69) E1172D 40.5 ± 8.8 (907) 40.5 ± 7.6 (93) 29 (1) 34.6 ± 7.3 (1129) 35.4 ± 7.6 (105) 30.7 ± 8.7 (3) R1587K 41.1 ± 9.4 (410) 40.8 ± 9.6 (433) 41.0 ± 10.1 (94) 35.9 ± 8.1 (617) 35.1 ± 7.6 (579) 35.3 ± 8.6 (155) Numbers of subjects are shown in parenthesis.
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116 Informative associations between HDL-C levels and the R219K, V771M, and I883M polymorphisms will be discussed.
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168 Effect of combined ABCA1 polymorphisms on HDL-C levels in a random Turkish population The R219K and I883M polymorphisms have been shown to affect lipid metabolism or CAD risk [9,10,12,15,43].
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170 In contrast, the combinations of C-14T with R219K and of V771M with I883M were associated with altered HDL-C levels.
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ABCA1 p.Arg219Lys 15935359:170:44
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171 As shown in Table 4, subjects were stratified according to their R219K genotype (RR, RK, or KK) versus C-14T (CC, CT, or TT).
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ABCA1 p.Arg219Lys 15935359:171:65
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181 Separate haplotype blocks of ABCA1 In order to assess whether the length of the ABCA1 locus could be treated as a single haplotype block, haplotypes were constructed and significant LDs between polymorphisms were calculated using 10 common ABCA1 polymorphisms Table 4 Interactive effects of ABCA1 polymorphisms on mean plasma HDL-C levels (mg/dl ± S.D.) R219K C-14T Females Males RR CC 41.4 ± 8.5 (128) 34.7 ± 6.7 (207) CT 41.6 ± 9.8 (150) 35.7 ± 7.6 (253) TT 41.3 ± 8.9 (55) 36.3 ± 7.8 (84) RK CC 41.8 ± 8.3 (169) 34.8 ± 7.4 (261) CT 39.9 ± 8.3 (203) 35.5 ± 6.8 (309) TT 39.5 ± 9.0 (60) 36.8 ± 8.5 (84) KK CC 39.8 ± 11.2 (60) 34.0 ± 6.2 (69) CT 41.1 ± 9.0 (60) 35.7 ± 8.4 (102) TT 44.7 ± 9.8a (22) 37.1 ± 7.8a (22) I883M V771M II VV 40.9 ± 9.8 (499) 34.8 ± 6.8 (797) VM 41.4 ± 8.3 (74) 36.7 ± 8.3b (112) IM VV 40.3 ± 8.0 (313) 35.1 ± 8.1 (427) VM 44.2 ± 11.5b (17) 37.3 ± 7.4b (26) MM VV 41.6 ± 9.2 (60) 35.6 ± 7.5 (67) Numbers of subjects are shown in parenthesis.
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ABCA1 p.Arg219Lys 15935359:181:359
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204 However, further analysis Table 5 Allele frequency and significant (P < 0.01) pair-wise linkage disequilibrium coefficients between the ABCA1 polymorphisms in a random Turkish population Position Allele % T-564C G-99C C-14T InsG 319 R219K V771M V825I I883M E1172D R1587K T-564C 52.3/47.7 - G-99C 75.8/24.2 0.36 - C-14T 62.3/37.7 -0.96 -0.98 - InsG 319 85.8/14.2 - - - - R219K 61.5/38.5 - - - - V771M 94.9/5.1 - - - 0.99 - V825I 93.8/6.2 -0.40 -0.69 - - -0.76 - - I883M 78.2/21.8 - -0.42 - - 0.20 -0.79 0.91 - E1172D 95.4/4.6 - - - - - 0.34 - - - R1587K 67.0/33.0 - - -0.23 - - 0.56 - - 0.87 - Table 6 Common haplotypes of promoter and coding regions of ABCA1 gene in a random Turkish population Promoter region haplotypes % T-564C G-99C C-14T InsG 319 1 31.7 0 0 1 0 2 20.1 1 1 0 0 3 19.9 1 0 0 0 4 12.7 0 0 0 0 5 4.6 0 0 1 1 6 4.2 1 1 0 1 7 3.2 1 0 0 1 8 2.5 0 0 0 1 Sum 98.9 Coding region haplotypes % R219K V771M V825I I883M E1172D R1587K 1 39.3 0 0 0 0 0 0 2 12.6 1 0 0 0 0 0 3 12.0 0 0 0 0 0 1 4 8.7 1 0 0 1 0 0 5 8.3 1 0 0 0 0 1 6 4.0 0 0 1 1 0 0 7 3.4 0 0 0 0 1 1 8 1.6 1 0 0 1 0 1 9 1.3 1 1 0 0 0 0 10 1.3 0 1 0 0 1 1 11 1.3 0 0 1 1 0 1 12 1.1 1 1 0 0 0 1 Sum 95.1 0: common allele; 1: rare allele.
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ABCA1 p.Arg219Lys 15935359:204:233
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ABCA1 p.Arg219Lys 15935359:204:370
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ABCA1 p.Arg219Lys 15935359:204:907
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209 We observed an interaction between the C-14T and R219K polymorphisms (Table 4).
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ABCA1 p.Arg219Lys 15935359:209:49
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ABCA1 p.Arg219Lys 15935359:209:156
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210 In an effort to construct haplotypes including these two polymorphisms, a haplotype block including five polymorphisms (T-564C, G-99C, C-14T, InsG 319, and R219K) was used for mapping.
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213 Therefore, haplotype-to-phenotype associations containing the C-14T and R219K polymorphisms within the same block could not be conducted.
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215 Haplotype structure and haplotype-phenotype association of polymorphisms in the coding region of ABCA1 When the haplotype structure of the coding region was constructed using six polymorphisms (R219K, V771M, V825I, I883M, E1172D, and R1587K; Table 6), 12 haplotypes with a frequency >1% accounted for 95.1% of all haplotypes.
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ABCA1 p.Arg219Lys 15935359:215:194
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231 There was negative LD (rare allele to common allele) between I883M and V771M as seen in Table 4.
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ABCA1 p.Arg219Lys 15935359:231:4
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232 The R219K, C-14T, and V771M polymorphisms were not in LD in the Turkish population.
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ABCA1 p.Arg219Lys 15935359:232:4
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279 In the analysis of covariance, where the sources of variance on plasma HDL-C levels were examined, introduction of interaction variables (smoking or alcohol consumption) × (C-14T or V771M) to the model showed that neither parameter modulated (P > 0.05) the effect of polymorphisms on HDL-C levels in males or females or when data for both genders were pooled.
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ABCA1 p.Arg219Lys 15935359:279:120
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280 However, we are able to see an association with elevated HDL-C in females through the combined effect between C-14T and R219K.
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ABCA1 p.Arg219Lys 15935359:280:120
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282 We tried to examine the combined effect of the C-14T and R219K polymorphisms by examining the haplotypes that contain these two rare allele genotypes; unfortunately, haplotype construction was complicated by an inability to predict a unique set of diplotypes.
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ABCA1 p.Arg219Lys 15935359:282:57
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283 This prevented further statistical association of haplotypes that include both the C-14T and the R219K polymorphisms in the same haplotype block.
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ABCA1 p.Arg219Lys 15935359:283:0
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ABCA1 p.Arg219Lys 15935359:283:97
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284 R219K by itself did not affect plasma lipid levels in Turks and Danes [17].
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ABCA1 p.Arg219Lys 15935359:284:0
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288 On the other hand, the R219K polymorphism did not affect the severity of coronary atherosclerosis in the Veterans Administration HDL Cholesterol Intervention Trial [13] or in Japanese CAD patients [14].
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ABCA1 p.Arg219Lys 15935359:288:23
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ABCA1 p.Arg219Lys 15935359:288:39
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289 In Turks, the interaction of C-14T and R219K may play a role in altering plasma HDL-C levels and possibly CAD risk.
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ABCA1 p.Arg219Lys 15935359:289:39
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304 A functional promoter polymorphism, C-14T, and a coding sequence polymorphism, V771M, in the ABCA1 gene appeared to affect HDL-C levels in Turks and these results could be replicated when our entire data set was randomly divided in two different subsets (Supplemental Table II).
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ABCA1 p.Arg219Lys 15935359:304:44
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305 Two combinations of rare alleles-C-14T with R219K and V771M with I883M-were associated with high HDL-C in both males and females.
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103 The G-803A Table 2 ABCA1 polymorphisms Nucleotide changea Carrier of rare allele (%) Rare allele (%) nb Referencesc Frequency in 5 and promoter regions G-803A ~10 92/141 [19] T-564C 72.7 47.7 728/1268 [18] G-407C 62.5 40.7 220/233 [18] G-99C 42.2 24.2 875/1130 [46] C-14T 61.2 37.7 916/1416 [46] InsG 319 26.6 14.2 848/1288 [46] Nucleotide changed Amino acid change Exon Carrier of rare allele (%) Rare allele (%) nb Referencesc Frequency in coding sequence Nonsynonymous G(70943)A R219K 7 62.3 38.5 996/1466 db 2230806 G(102555)A V771M 16 10.0 5.1 981/1477 db 2066718 G(103777)A V825I 17 12.3 6.2 960/1145 db 4149312 A(105057)G I883M 18 38.1 21.8 1084/1448 db 4149313 G(112177)C E1172D 24 9.0 4.6 1001/1237 [12,13] A(116887)G Q1328R 28 0.003e 0.0015 172/156 NR G(129004)A R1587K 35 55.1 33.0 937/1351 db 2230808 T(133402)C Y1767H 39 ~1.0e 40/55 NR G(133420)A V1773M 39 ~1.0e 40/55 NR Synonymous C(100538)A I620I 15 ~4.0 40/55 NR C(109469)T V990V 21 ~3.0 87/90 [17] T(109861)G V1053V 22 ~1.0 90/90 [12] C(109868)T L1056L 22 ~5.0 90/90 NR C(109906)T R1068R 22 ~3.0 90/90 NR A(113280)G E1211E 25 ~4.0 40/55 [17] A(116879)G T1325T 28 ~1.0 40/55 NR T(137043)C Y1921Y 43 ~1.0 40/55 NR Nucleotide changed Intron Carrier of rare allele (%) Intronic location nb Referencesc Frequency in noncoding sequence G(23816)A 1 ~1.0 11 bp 5 exon 1b 94 NR G(23819)C 1 42 8 bp 5 exon 1b 94 NR A(22997)T 1 46 90 bp 5 exon 1d 91 NR A(23004)G 1 ~1.0 83 bp 5 exon 1d 91 NR G(23058)C 1 46 29 bp 5 exon 1d 91 NR G(40504)A 3 2.6 26 bp 3 of exon 3 192 NR C(45217)T 4 0.7 64 bp 3 of exon 4 142 NR T(98628)A 14 35-40 24 bp 3 of exon 14 190 db 4743763 C(100332)T 14 4.3 59 bp 5 of exon 15 90 db 2066717 C(108020)T 19 0.7 3 bp 5 of exon 20 144 NR DelTTT(134503-6) 39 7.0 20-23 bp 5 of exon 40 90 NR C(142026)T 46 8.6 34 bp 5 of exon 47 116 NR A(142751)G 48 15.9 13 bp 3 of exon 48 107 NR a Relative to transcriptional start.
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ABCA1 p.Arg219Lys 15935359:103:483
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108 Table 3 ABCA1 polymorphisms and mean plasma HDL-C levels (mg/dl &#b1; S.D.) in a random Turkish population Females Males AAa AB BB AAa AB BB Promoter and 5 region T-564C 40.4 &#b1; 8.4 (205) 41.0 &#b1; 7.9 (365) 39.9 &#b1; 7.6 (158) 35.6 &#b1; 7.4 (339) 35.5 &#b1; 6.5 (635) 34.9 &#b1; 6.5 (294) G-407C 41.3 &#b1; 11.2 (82) 40.7 &#b1; 7.7 (101) 40.7 &#b1; 12.2 (37) 35.7 &#b1; 6.9 (88) 35.3 &#b1; 6.7 (96) 35.4 &#b1; 7.4 (49) G-99C 40.7 &#b1; 7.5 (505) 41.0 &#b1; 7.2 (317) 41.3 &#b1; 8.4 (53) 35.1 &#b1; 6.5 (654) 35.0 &#b1; 6.3 (405) 34.9 &#b1; 6.5 (71) C-14T 41.3 &#b1; 9.0 (361) 41.0 &#b1; 9.0 (417) 41.0 &#b1; 9.4 (138) 34.8 &#b1; 7.0b (547) 35.5 &#b1; 7.5 (675) 36.7 &#b1; 8.1b (194) InsG 319 41.3 &#b1; 8.1 (641) 40.5 &#b1; 7.7 (193) 43.1 &#b1; 8.0 (14) 35.3 &#b1; 6.4 (933) 34.7 &#b1; 6.4 (332) 34.5 &#b1; 6.5 (23) Nonsynonymous R219K 41.2 &#b1; 9.4 (364) 40.8 &#b1; 8.6 (480) 41.2 &#b1; 10 (152) 35.2 &#b1; 7.3 (574) 35.3 &#b1; 7.3 (688) 35.2 &#b1; 7.6 (204) V771M 40.9 &#b1; 9.2 (896) 42.8 &#b1; 9.3 (82) 38.7 &#b1; 10 (3) 35.1 &#b1; 7.2c (1330) 37.1 &#b1; 8.0c (144) 45.7 &#b1; 10.7 (3) V825I 40.6 &#b1; 9.4 (842) 38.9 &#b1; 8.5 (117) 42 (1) 35.8 &#b1; 8.7 (1005) 37.1 &#b1; 9.5 (140) (-) I883M 41.1 &#b1; 9.5 (643) 40.8 &#b1; 8.4 (372) 41.4 &#b1; 9.1 (69) 35.0 &#b1; 7.0 (922) 35.7 &#b1; 8.0 (457) 35.6 &#b1; 7.4 (69) E1172D 40.5 &#b1; 8.8 (907) 40.5 &#b1; 7.6 (93) 29 (1) 34.6 &#b1; 7.3 (1129) 35.4 &#b1; 7.6 (105) 30.7 &#b1; 8.7 (3) R1587K 41.1 &#b1; 9.4 (410) 40.8 &#b1; 9.6 (433) 41.0 &#b1; 10.1 (94) 35.9 &#b1; 8.1 (617) 35.1 &#b1; 7.6 (579) 35.3 &#b1; 8.6 (155) Numbers of subjects are shown in parenthesis.
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ABCA1 p.Arg219Lys 15935359:108:838
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115 Informative associations between HDL-C levels and the R219K, V771M, and I883M polymorphisms will be discussed.
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167 Effect of combined ABCA1 polymorphisms on HDL-C levels in a random Turkish population The R219K and I883M polymorphisms have been shown to affect lipid metabolism or CAD risk [9,10,12,15,43].
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ABCA1 p.Arg219Lys 15935359:167:90
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169 In contrast, the combinations of C-14T with R219K and of V771M with I883M were associated with altered HDL-C levels.
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180 Separate haplotype blocks of ABCA1 In order to assess whether the length of the ABCA1 locus could be treated as a single haplotype block, haplotypes were constructed and significant LDs between polymorphisms were calculated using 10 common ABCA1 polymorphisms Table 4 Interactive effects of ABCA1 polymorphisms on mean plasma HDL-C levels (mg/dl &#b1; S.D.) R219K C-14T Females Males RR CC 41.4 &#b1; 8.5 (128) 34.7 &#b1; 6.7 (207) CT 41.6 &#b1; 9.8 (150) 35.7 &#b1; 7.6 (253) TT 41.3 &#b1; 8.9 (55) 36.3 &#b1; 7.8 (84) RK CC 41.8 &#b1; 8.3 (169) 34.8 &#b1; 7.4 (261) CT 39.9 &#b1; 8.3 (203) 35.5 &#b1; 6.8 (309) TT 39.5 &#b1; 9.0 (60) 36.8 &#b1; 8.5 (84) KK CC 39.8 &#b1; 11.2 (60) 34.0 &#b1; 6.2 (69) CT 41.1 &#b1; 9.0 (60) 35.7 &#b1; 8.4 (102) TT 44.7 &#b1; 9.8a (22) 37.1 &#b1; 7.8a (22) I883M V771M II VV 40.9 &#b1; 9.8 (499) 34.8 &#b1; 6.8 (797) VM 41.4 &#b1; 8.3 (74) 36.7 &#b1; 8.3b (112) IM VV 40.3 &#b1; 8.0 (313) 35.1 &#b1; 8.1 (427) VM 44.2 &#b1; 11.5b (17) 37.3 &#b1; 7.4b (26) MM VV 41.6 &#b1; 9.2 (60) 35.6 &#b1; 7.5 (67) Numbers of subjects are shown in parenthesis.
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ABCA1 p.Arg219Lys 15935359:180:358
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203 However, further analysis Table 5 Allele frequency and significant (P < 0.01) pair-wise linkage disequilibrium coefficients between the ABCA1 polymorphisms in a random Turkish population Position Allele % T-564C G-99C C-14T InsG 319 R219K V771M V825I I883M E1172D R1587K T-564C 52.3/47.7 - G-99C 75.8/24.2 0.36 - C-14T 62.3/37.7 -0.96 -0.98 - InsG 319 85.8/14.2 - - - - R219K 61.5/38.5 - - - - V771M 94.9/5.1 - - - 0.99 - V825I 93.8/6.2 -0.40 -0.69 - - -0.76 - - I883M 78.2/21.8 - -0.42 - - 0.20 -0.79 0.91 - E1172D 95.4/4.6 - - - - - 0.34 - - - R1587K 67.0/33.0 - - -0.23 - - 0.56 - - 0.87 - Table 6 Common haplotypes of promoter and coding regions of ABCA1 gene in a random Turkish population Promoter region haplotypes % T-564C G-99C C-14T InsG 319 1 31.7 0 0 1 0 2 20.1 1 1 0 0 3 19.9 1 0 0 0 4 12.7 0 0 0 0 5 4.6 0 0 1 1 6 4.2 1 1 0 1 7 3.2 1 0 0 1 8 2.5 0 0 0 1 Sum 98.9 Coding region haplotypes % R219K V771M V825I I883M E1172D R1587K 1 39.3 0 0 0 0 0 0 2 12.6 1 0 0 0 0 0 3 12.0 0 0 0 0 0 1 4 8.7 1 0 0 1 0 0 5 8.3 1 0 0 0 0 1 6 4.0 0 0 1 1 0 0 7 3.4 0 0 0 0 1 1 8 1.6 1 0 0 1 0 1 9 1.3 1 1 0 0 0 0 10 1.3 0 1 0 0 1 1 11 1.3 0 0 1 1 0 1 12 1.1 1 1 0 0 0 1 Sum 95.1 0: common allele; 1: rare allele.
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ABCA1 p.Arg219Lys 15935359:203:233
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ABCA1 p.Arg219Lys 15935359:203:370
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ABCA1 p.Arg219Lys 15935359:203:907
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208 We observed an interaction between the C-14T and R219K polymorphisms (Table 4).
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212 Therefore, haplotype-to-phenotype associations containing the C-14T and R219K polymorphisms within the same block could not be conducted.
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ABCA1 p.Arg219Lys 15935359:212:72
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214 Haplotype structure and haplotype-phenotype association of polymorphisms in the coding region of ABCA1 When the haplotype structure of the coding region was constructed using six polymorphisms (R219K, V771M, V825I, I883M, E1172D, and R1587K; Table 6), 12 haplotypes with a frequency >1% accounted for 95.1% of all haplotypes.
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ABCA1 p.Arg219Lys 15935359:214:194
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281 We tried to examine the combined effect of the C-14T and R219K polymorphisms by examining the haplotypes that contain these two rare allele genotypes; unfortunately, haplotype construction was complicated by an inability to predict a unique set of diplotypes.
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ABCA1 p.Arg219Lys 15935359:281:57
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287 On the other hand, the R219K polymorphism did not affect the severity of coronary atherosclerosis in the Veterans Administration HDL Cholesterol Intervention Trial [13] or in Japanese CAD patients [14].
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ABCA1 p.Arg219Lys 15935359:287:23
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PMID: 16429166 [PubMed] Brunham LR et al: "Accurate prediction of the functional significance of single nucleotide polymorphisms and mutations in the ABCA1 gene."
No. Sentence Comment
45 À;3), R219K, V771M, I883M, D1289N, and P2150L, four had cholesterol efflux values that were not statistically different from wild-type ABCA1.
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ABCA1 p.Arg219Lys 16429166:45:5
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46 This included two variants, D1289N and P2150L, that have been previously reported to be disease-causing mutations [4,8,9], as well as two cSNPs, R219K and V771M.
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ABCA1 p.Arg219Lys 16429166:46:145
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48 This SNP has been reported to be associated with decreased HDL cholesterol and increased severity of atherosclerosis in Table 1. subPSEC Scores and Probability of Functional Impairment (Pdeleterious) for ABCA1 Mutations and SNPs Mutations SNPs Variant SubPSEC Pdeleterious Variant subPSEC Pdeleterious P85L À4.62 0.83 R219K À0.57 0.08 H160F À2.79 0.45 V399A À2.26 0.32 R230C À4.27 0.78 V771M À2.86 0.46 A255T À1.81 0.23 T774P À1.99 0.27 E284K À2.34 0.34 K776N À3.53 0.63 Y482C À4.21 0.77 V825I À1.06 0.13 R587W À6.04 0.95 I883M À1.38 0.17 W590S À5.19 0.9 E1172D À1.96 0.26 W590L À4.48 0.82 R1587K À0.58 0.08 Q597R À7.15 0.98 S1731C À4.21 0.77 T929I À4.29 0.78 N935H À8.54 1 N935S À7.53 0.99 A937V À6.6 0.97 A1046D À7.52 0.99 M1091T À3.56 0.64 D1099Y À6.09 0.96 D1289N À2.48 0.37 L1379F À3.81 0.69 C1477R À5.44 0.92 S1506L À5.17 0.9 N1611D À5.69 0.94 R1680W À6.02 0.95 V1704D À3.21 0.55 N1800H À4.23 0.77 R1901S À5.06 0.89 F2009S À2.73 0.43 R2081W À8.08 0.99 P2150L À2.88 0.47 Q2196H À2.74 0.43 DOI: 10.1371/journal.pgen.0010083.t001 PLoS Genetics | www.plosgenetics.org December 2005 | Volume 1 | Issue 6 | e83 0740 Accurate Prediction of ABCA1 Variants Synopsis A major goal of human genetics research is to understand how genetic variation leads to differences in the function of genes.
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ABCA1 p.Arg219Lys 16429166:48:318
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75 Cholesterol Efflux Values for 293 Cells Transfected with ABCA1 Variants and subPSEC and PolyPhen Predictions of the Functional Impact of these Variants Variant Variant Type subPSEC Cholesterol Efflux PolyPhen R2081W Mutation À8.08 21.1 6 21%* Probably damaging N935S Mutation À7.53 29.3 6 13%* Benign A1046D Mutation À7.52 16.8 6 7%* Possibly damaging Q597R Mutation À7.15 17.7 6 14%* Probably damaging R587W Mutation À6.04 31.7 6 33%* Probably damaging C1477R Mutation À5.44 20.5 6 10%* Probably damaging W590S Mutation À5.19 47.1 6 13%* Probably damaging S1506L Mutation À5.17 17.8 6 15%* Probably damaging T929I Mutation À4.29 69.9 6 11%* Possibly damaging N1800H Mutation À4.23 31.3 6 16%* Possibly damaging S1731C SNP À4.21 12.3 6 10%* Possibly damaging M1091T Mutation À3.56 6.9 6 20%* Probably damaging P2150L Mutation À2.88 88.4 6 21% Probably damaging V771M SNP À2.86 145.4 6 33% Benign D1289N Mutation À2.48 137.7 6 86% Benign I883M SNP À1.38 69.1 6 16%* Benign R219K SNP À0.57 103.7 6 21.05 Benign Wild-type - 0.0 100% - *p , 0.01 compared to wild-type ABCA1.
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ABCA1 p.Arg219Lys 16429166:75:972
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ABCA1 p.Arg219Lys 16429166:75:1052
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PMID: 16226177 [PubMed] Frikke-Schmidt R et al: "Mutation in ABCA1 predicted risk of ischemic heart disease in the Copenhagen City Heart Study Population."
No. Sentence Comment
107 However, at the individual level, K776N appears to have a marked impact on risk.
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ABCA1 p.Arg219Lys 16226177:107:951
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109 However, several arguments favor a true observation: 1) the involved amino acid residue is completely conserved between species and relatively conserved between 12 ABCAs with very different transport functions; 2) the amino acid substitution changes the charge of the side-chain, potentially leading to structural alterations of the protein, and consequently to altered protein interactions or transport properties; 3) in the CFTR (or ABCC7), a disease-causing mutation (R347P) has been identified at a site that corresponds to residue 764 in ABCA1 (15), and thus in close vicinity to K776N; 4) the present study is of a large cohort, and therefore includes only incident cases, avoiding the normal pitfalls of case reports and case-control studies (30); 5) we observed a similar trend on risk of IHD in a separate case-control study; 6) we have previously determined effects on lipids and lipoproteins of all non-synonymous SNPs identified in ABCA1 (R219K, V771M, V825I, I883M, E1172D, R1587K).
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ABCA1 p.Arg219Lys 16226177:109:951
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PMID: 16183915 [PubMed] Oram JF et al: "ATP-binding cassette transporter A1: a cell cholesterol exporter that protects against cardiovascular disease."
No. Sentence Comment
431 The most studied of these SNPs is the R219K variant, with the K allele being associated with higher levels of HDL (255).
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ABCA1 p.Arg219Lys 16183915:431:38
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430 The most studied of these SNPs is the R219K variant, with the K allele being associated with higher levels of HDL (255).
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ABCA1 p.Arg219Lys 16183915:430:38
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PMID: 15790791 [PubMed] Albrecht C et al: "A novel missense mutation in ABCA1 results in altered protein trafficking and reduced phosphatidylserine translocation in a patient with Scott syndrome."
No. Sentence Comment
115 The R1925Q variant was not found in 164 alleles of a control population of British origin,32 evidenced by WAVE analysis.
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ABCA1 p.Arg219Lys 15790791:115:68
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116 For comparison, the allele frequency of the polymorphism in exon 6 (R219K) in this population was 0.22, similar to that observed in other European populations (0.254).33 To investigate whether there was differential expression of the 2 alleles, a PCR product spanning the c.6064GϾA mutation was generated by RT-PCR from total RNA isolated from leukocytes of 544 ALBRECHT et al BLOOD, 15 JULY 2005 the SS patient.
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ABCA1 p.Arg219Lys 15790791:116:68
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PMID: 15829498 [PubMed] Zareparsi S et al: "Toll-like receptor 4 variant D299G is associated with susceptibility to age-related macular degeneration."
No. Sentence Comment
69 Interaction of TLR4-D299G with ABCA1-R219K and APOE variants Given that ABCA1 and APOE are downstream in TLR4 signaling pathway (48,49), participate in cholesterol metabolism and are associated with atherosclerosis (43,53), we determined whether ABCA1 and APOE variants interact with TLR4-D299G in contributing to AMD susceptibility.
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ABCA1 p.Arg219Lys 15829498:69:37
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70 The frequency of the K allele of ABCA1-R219K (associated with reduced risk of atherosclerosis) (53) was similar between AMD patients and controls (0.29 versus 0.29, P .
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ABCA1 p.Arg219Lys 15829498:70:39
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79 There was no significant interaction between TLR4-D299G, ABCA1-R219K and APOE on AMD susceptibility (Table 4).
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ABCA1 p.Arg219Lys 15829498:79:63
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80 Nevertheless, ABCA1-R219K further contributed to the additive effect and the risk of AMD was increased by 4-fold in carriers of the risk alleles for all three genes (Gþ, Kþ and 142) when compared with those without the risk alleles (G2, K2 and 14þ) (Table 4).
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ABCA1 p.Arg219Lys 15829498:80:20
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83 Age at diagnosis of AMD did not vary significantly in the presence of the TLR4-D299G-G allele (70.6 + 9.3 versus 71.4 + 8.7) or the ABCA1-R219K-K allele (71.7 + 8.7 versus 70.9 + 8.8).
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ABCA1 p.Arg219Lys 15829498:83:138
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107 Here, we show that the variants reported to correlate with reduced risk of atherogenesis (TLR4-D299G, ABCA1-R219K and APOE-12/3) are associated with increased risk of AMD.
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ABCA1 p.Arg219Lys 15829498:107:108
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137 APOE and ABCA1-R219K genotypes were obtained using previously described methods by PCR and restriction digestion (53,64).
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ABCA1 p.Arg219Lys 15829498:137:15
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148 Additive effects between the TLR4-D299G and/or APOE and/or ABCA1-R219K were analyzed by logistic regression, where those carrying the risk alleles for any given combination of SNPs were compared with those who lacked the risk alleles for those SNPs (e.g. TLR4-G and ABCA1-K carriers compared with TLR4-DD and TLR4-RR individuals).
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ABCA1 p.Arg219Lys 15829498:148:65
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71 Interaction of TLR4-D299G with ABCA1-R219K and APOE variants Given that ABCA1 and APOE are downstream in TLR4 signaling pathway (48,49), participate in cholesterol metabolism and are associated with atherosclerosis (43,53), we determined whether ABCA1 and APOE variants interact with TLR4-D299G in contributing to AMD susceptibility.
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ABCA1 p.Arg219Lys 15829498:71:37
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72 The frequency of the K allele of ABCA1-R219K (associated with reduced risk of atherosclerosis) (53) was similar between AMD patients and controls (0.29 versus 0.29, P .
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ABCA1 p.Arg219Lys 15829498:72:39
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82 Nevertheless, ABCA1-R219K further contributed to the additive effect and the risk of AMD was increased by 4-fold in carriers of the risk alleles for all three genes (G&#fe;, K&#fe; and 142) when compared with those without the risk alleles (G2, K2 and 14&#fe;) (Table 4).
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ABCA1 p.Arg219Lys 15829498:82:20
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85 Age at diagnosis of AMD did not vary significantly in the presence of the TLR4-D299G-G allele (70.6 + 9.3 versus 71.4 + 8.7) or the ABCA1-R219K-K allele (71.7 + 8.7 versus 70.9 + 8.8).
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ABCA1 p.Arg219Lys 15829498:85:138
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109 Here, we show that the variants reported to correlate with reduced risk of atherogenesis (TLR4-D299G, ABCA1-R219K and APOE-12/3) are associated with increased risk of AMD.
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ABCA1 p.Arg219Lys 15829498:109:108
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PMID: 15557325 [PubMed] Koldamova RP et al: "The liver X receptor ligand T0901317 decreases amyloid beta production in vitro and in a mouse model of Alzheimer's disease."
No. Sentence Comment
14 Wollmer et al. (15) found that the R219K variant of ABCA1, associated with increased HDL cholesterol levels and a decreased risk of atherosclerosis (16), delayed the age of onset of late onset Alzheimer`s disease.
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ABCA1 p.Arg219Lys 15557325:14:35
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PMID: 15528481 [PubMed] Kyriakou T et al: "Genotypic effect of the -565C>T polymorphism in the ABCA1 gene promoter on ABCA1 expression and severity of atherosclerosis."
No. Sentence Comment
87 An interaction between another ABCA1 gene polymorphism (ie, R219K) and smoking has been reported previously, although the underlying mechanisms remain unknown.16 TABLE 2.
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ABCA1 p.Arg219Lys 15528481:87:17
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ABCA1 p.Arg219Lys 15528481:87:60
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93 For example, the R219K polymorphism has been shown to be associated with risk of myocardial infarction and/or severity of atherosclerosis,15-19 the V825I, M883I, and R1587K polymorphisms with various cardiovascular traits,17,20,21 the -191GϾC, -17CϾG, and 69CϾT polymorphisms with risk of coronary events in patients with coronary atherosclerosis,22 and the 319insG polymorphism with severity of atherosclerosis.22 Taken together, these data suggest that the development and outcome of atherosclerosis might be influenced by a qualitative change of the ABCA1 protein caused by coding region variants and a quantitative change in ABCA1 expression caused by regulatory region variants.
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ABCA1 p.Arg219Lys 15528481:93:17
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95 For example, in a study of 465 Japanese patients with myocardial infarction or angina pectoris, Takagi et al23 did not find an association between severity of atherosclerosis and the -565CϾT polymorphism, nor did they find an association between severity of atherosclerosis and the ABCA1 gene R219K polymorphism, which has been shown to be associated with atherosclerosis severity in several other studies.15-19 Thus, it appears that the genotypic effects of ABCA1 may be influenced by other factors such as genetic backgrounds and environmental factors.
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ABCA1 p.Arg219Lys 15528481:95:299
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81 An interaction between another ABCA1 gene polymorphism (ie, R219K) and smoking has been reported previously, although the underlying mechanisms remain unknown.16 TABLE 2.
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ABCA1 p.Arg219Lys 15528481:81:60
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89 For example, in a study of 465 Japanese patients with myocardial infarction or angina pectoris, Takagi et al23 did not find an association between severity of atherosclerosis and the afa;565Cb0e;T polymorphism, nor did they find an association between severity of atherosclerosis and the ABCA1 gene R219K polymorphism, which has been shown to be associated with atherosclerosis severity in several other studies.15-19 Thus, it appears that the genotypic effects of ABCA1 may be influenced by other factors such as genetic backgrounds and environmental factors.
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ABCA1 p.Arg219Lys 15528481:89:305
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PMID: 15262183 [PubMed] Probst MC et al: "Screening for functional sequence variations and mutations in ABCA1."
No. Sentence Comment
188 The patient was also heterozygous for two known polymorphisms (R219K and I883M), but no second mutation could be identified so far.
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ABCA1 p.Arg219Lys 15262183:188:63
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197 Three other known sequence variations have been found (heterozygous R219K, heterozygous E1172D and homozygous R1587K).
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ABCA1 p.Arg219Lys 15262183:197:68
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PMID: 15218400 [PubMed] Miller M et al: "Genetic determinants of low high-density lipoprotein cholesterol."
No. Sentence Comment
32 During the past year, several but not all ABCA1 variants have been associated with reduced HDL-C and CHD [14•-16•,17,18]; in populations, one specific polymorphism (R219K) was associated with reduced CHD risk [19•,20•].
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ABCA1 p.Arg219Lys 15218400:32:179
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PMID: 15158913 [PubMed] Albrecht C et al: "Two novel missense mutations in ABCA1 result in altered trafficking and cause severe autosomal recessive HDL deficiency."
No. Sentence Comment
150 In comparison, the allele frequency of the R219K polymorphism was 0.22 (K allele), similar to that found in other European populations [31].
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ABCA1 p.Arg219Lys 15158913:150:43
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149 In comparison, the allele frequency of the R219K polymorphism was 0.22 (K allele), similar to that found in other European populations [31].
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ABCA1 p.Arg219Lys 15158913:149:43
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PMID: 15044381 [PubMed] Knoblauch H et al: "Haplotypes and SNPs in 13 lipid-relevant genes explain most of the genetic variance in high-density lipoprotein and low-density lipoprotein cholesterol."
No. Sentence Comment
77 SNP characteristics including SNP identification system, localization, allele frequencies, nucleotide exchange and pseudonym are shown Gene/SNP no. SNP Id. Localization Allele frequency Nucleotide exchange Pseudonym APOB apob.snp1 rs512535 Promotor 0.45 G/A G-837A apob.snp2 rs1367117 Exon/non-syn 0.32 C/T Thr71Ile apob.snp3 rs520354 Intron 0.44 T/C apob.snp4 rs679899 Exon/non-syn 0.44 C/T Ala618Val apob.snp5 rs673548 Intron 0.21 C/T apob.snp6 rs693 Exon/syn 0.50 T/C XbaI apob.snp7 rs1800479 Intron 0.16 C/G Gþ50/in27C apob.snp8 rs1801703 Exon/non-syn 0.01 C/T Val4101Met apob.snp9 rs1042034 Exon/non-syn 0.22 T/C Asn4311Ser APOE apoe.snp1 rs449647 Promotor 0.17 A/T t-491a apoe.snp2 rs405509 Promotor 0.48 C/A g-219t apoe.snp3 rs440446 Intron 0.36 G/C Variant 1163 apoe.snp4 rs769450 Intron 0.41 C/T Variant 2440 apoe.snp5 rs429358 Exon/non-syn 0.16 T/C Cys112Arg apoe.snp6 rs7412 Exon/non-syn 0.06 C/T Arg158Cys ABCA1 abca1.snp1 rs2422493 Promotor 0.45 G/A 2477c/t abca1.snp2 rs1800977 50 UTR 0.50 C/T t69c abca1.snp3 50 UTR 0.04 C/G c117g abca1.snp4 rs2575879 Intron 0.46 G/C abca1.snp5 rs1800978 50 UTR 0.01 G/C G378C abca1.snp6 rs1999429 Intron 0.03 G/T abca1.snp7 rs2230806 Exon/non-syn 0.26 C/T Arg219Lys abca1.snp8 rs2274873 Exon/syn 0.08 C/T Pro312Pro abca1.snp9 rs4149313 Exon/non-syn 0.13 T/C A3044G, Ile883Met abca1.snp10 Exon/non-syn 0.03 C/G G3911C, Glu1172Asp abca1.snp11 rs2066716 Exon/syn 0.08 G/A Thr1367Thr abca1.snp12 rs363717 30 UTR 0.20 A/G CETP cetp.snp1 rs4783961 Promotor 0.47 C/T 2971 g/a cetp.snp2 rs1800776 Promotor 0.07 G/T 2631 cetp.snp3 rs1800775 Promotor 0.49 G/T 2629 cetp.snp4 rs711752 Intron 0.45 C/T Gþ202/in1A cetp.snp5 rs708272 Intron 0.45 C/T Taq1B; Gþ279/in1A cetp.snp6 rs158478 Intron 0.46 C/A EcoNI cetp.snp7 rs1532625 Intron 0.43 G/A Cþ8/in7T cetp.snp8 rs289718 Intron 0.29 T/C cetp.snp9 rs289719 Intron 0.29 C/T cetp.snp10 rs5880 Exon/non-syn 0.04 C/G CETPu1, Ala373Pro cetp.snp11 rs5882 Exon/non-syn 0.35 A/G CETPu2 cetp.snp12 rs1801706 30 UTR 0.18 C/T Gþ84A LCAT lcat.snp1 rs1109166 Intron 0.17 A/G lcat.snp2 rs4986970 Exon/non-syn 0.04 A/T Ser232Thr lcat.snp3 rs5923 Exon/syn 0.04 G/A LCATu3 LIPC lipc.snp1 rs723967 50 regiona 0.46 G/A lipc.snp2 rs1800588 Promotor 0.28 G/A 2C480T lipc.snp3 rs1869144 Intron 0.39 A/G lipc.snp4 rs6078 Exon/non-syn 0.04 G/A LIPCu1; Val73Met lipc.snp5 rs690 Exon/syn 0.49 T/G LIPCu3; Val155Val lipc.snp6 rs6082 Exon/syn 0.08 A/G LIPCu5; Gly197Gly lipc.snp7 rs6083 Exon/non-syn 0.36 T/C LIPCu6; Asn193Ser lipc.snp8 rs6084 Exon/syn 0.44 C/G LIPCu8; Thr224Thr lipc.snp9 rs6074 Exon/syn 0.13 G/T Thr479Thr LPL lpl.snp1 Promotor 0.00 C/A G-95T lpl.snp2 rs1800590 Promotor 0.01 A/C G-93T lpl.snp3 rs1031045 Intron 0.01 C/T lpl.snp4 rs253 Intron 0.47 C/T Continued Human Molecular Genetics, 2004, Vol. 13, No. 10 995 13 candidate genes important to lipid metabolism.
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ABCA1 p.Arg219Lys 15044381:77:1211
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79 SNP characteristics including SNP identification system, localization, allele frequencies, nucleotide exchange and pseudonym are shown Gene/SNP no. SNP Id. Localization Allele frequency Nucleotide exchange Pseudonym APOB apob.snp1 rs512535 Promotor 0.45 G/A G-837A apob.snp2 rs1367117 Exon/non-syn 0.32 C/T Thr71Ile apob.snp3 rs520354 Intron 0.44 T/C apob.snp4 rs679899 Exon/non-syn 0.44 C/T Ala618Val apob.snp5 rs673548 Intron 0.21 C/T apob.snp6 rs693 Exon/syn 0.50 T/C XbaI apob.snp7 rs1800479 Intron 0.16 C/G G&#fe;50/in27C apob.snp8 rs1801703 Exon/non-syn 0.01 C/T Val4101Met apob.snp9 rs1042034 Exon/non-syn 0.22 T/C Asn4311Ser APOE apoe.snp1 rs449647 Promotor 0.17 A/T t-491a apoe.snp2 rs405509 Promotor 0.48 C/A g-219t apoe.snp3 rs440446 Intron 0.36 G/C Variant 1163 apoe.snp4 rs769450 Intron 0.41 C/T Variant 2440 apoe.snp5 rs429358 Exon/non-syn 0.16 T/C Cys112Arg apoe.snp6 rs7412 Exon/non-syn 0.06 C/T Arg158Cys ABCA1 abca1.snp1 rs2422493 Promotor 0.45 G/A 2477c/t abca1.snp2 rs1800977 50 UTR 0.50 C/T t69c abca1.snp3 50 UTR 0.04 C/G c117g abca1.snp4 rs2575879 Intron 0.46 G/C abca1.snp5 rs1800978 50 UTR 0.01 G/C G378C abca1.snp6 rs1999429 Intron 0.03 G/T abca1.snp7 rs2230806 Exon/non-syn 0.26 C/T Arg219Lys abca1.snp8 rs2274873 Exon/syn 0.08 C/T Pro312Pro abca1.snp9 rs4149313 Exon/non-syn 0.13 T/C A3044G, Ile883Met abca1.snp10 Exon/non-syn 0.03 C/G G3911C, Glu1172Asp abca1.snp11 rs2066716 Exon/syn 0.08 G/A Thr1367Thr abca1.snp12 rs363717 30 UTR 0.20 A/G CETP cetp.snp1 rs4783961 Promotor 0.47 C/T 2971 g/a cetp.snp2 rs1800776 Promotor 0.07 G/T 2631 cetp.snp3 rs1800775 Promotor 0.49 G/T 2629 cetp.snp4 rs711752 Intron 0.45 C/T G&#fe;202/in1A cetp.snp5 rs708272 Intron 0.45 C/T Taq1B; G&#fe;279/in1A cetp.snp6 rs158478 Intron 0.46 C/A EcoNI cetp.snp7 rs1532625 Intron 0.43 G/A C&#fe;8/in7T cetp.snp8 rs289718 Intron 0.29 T/C cetp.snp9 rs289719 Intron 0.29 C/T cetp.snp10 rs5880 Exon/non-syn 0.04 C/G CETPu1, Ala373Pro cetp.snp11 rs5882 Exon/non-syn 0.35 A/G CETPu2 cetp.snp12 rs1801706 30 UTR 0.18 C/T G&#fe;84A LCAT lcat.snp1 rs1109166 Intron 0.17 A/G lcat.snp2 rs4986970 Exon/non-syn 0.04 A/T Ser232Thr lcat.snp3 rs5923 Exon/syn 0.04 G/A LCATu3 LIPC lipc.snp1 rs723967 50 regiona 0.46 G/A lipc.snp2 rs1800588 Promotor 0.28 G/A 2C480T lipc.snp3 rs1869144 Intron 0.39 A/G lipc.snp4 rs6078 Exon/non-syn 0.04 G/A LIPCu1; Val73Met lipc.snp5 rs690 Exon/syn 0.49 T/G LIPCu3; Val155Val lipc.snp6 rs6082 Exon/syn 0.08 A/G LIPCu5; Gly197Gly lipc.snp7 rs6083 Exon/non-syn 0.36 T/C LIPCu6; Asn193Ser lipc.snp8 rs6084 Exon/syn 0.44 C/G LIPCu8; Thr224Thr lipc.snp9 rs6074 Exon/syn 0.13 G/T Thr479Thr LPL lpl.snp1 Promotor 0.00 C/A G-95T lpl.snp2 rs1800590 Promotor 0.01 A/C G-93T lpl.snp3 rs1031045 Intron 0.01 C/T lpl.snp4 rs253 Intron 0.47 C/T Continued 13 candidate genes important to lipid metabolism.
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ABCA1 p.Arg219Lys 15044381:79:1210
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PMID: 15135251 [PubMed] Bertolini S et al: "Genetic polymorphisms affecting the phenotypic expression of familial hypercholesterolemia."
No. Sentence Comment
2 We investigated Apo E (ε2, ε3, ε4), MTP (-493G/T), Apo B (-516C/T), Apo A-V (-1131T/C), HL (-514C/T and -250G/A), FABP-2 (A54T), LPL (D9N, N291S, S447X) and ABCA1 (R219K) polymorphisms in 221 unrelated FH index cases and 349 FH relatives with defined LDL-R gene mutations.
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ABCA1 p.Arg219Lys 15135251:2:179
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25 Finally, we investigated the R219K variant of the ABCA1 gene, since the K allele appeared to be protective against CAD in both FH and non-FH subjects [22,23].
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ABCA1 p.Arg219Lys 15135251:25:29
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42 The polymorphisms Apo E, MTP -493G/T, LPL N291S, Apo B -516C/T, HL -514C/T, FABP-2 A54T, Apo A-V -1131T/C, ABCA1 R219K and LPL S447X were studied using methods previously described [2,6,11,13,14,16,19,23,25].
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ABCA1 p.Arg219Lys 15135251:42:113
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119 The other polymorphisms we investigated (N291S and D9N of LPL gene and R219K of ABCA1 gene) were found to have no significant effect on plasma lipids (data not shown).
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ABCA1 p.Arg219Lys 15135251:119:71
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173 Several recent studies have investigated the role of the R219K polymorphism of ABCA1 transporter on plasma lipoprotein profile or CAD [40].
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ABCA1 p.Arg219Lys 15135251:173:57
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116 The other polymorphisms we investigated (N291S and D9N of LPL gene and R219K of ABCA1 gene) were found to have no significant effect on plasma lipids (data not shown).
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ABCA1 p.Arg219Lys 15135251:116:71
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170 Several recent studies have investigated the role of the R219K polymorphism of ABCA1 transporter on plasma lipoprotein profile or CAD [40].
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ABCA1 p.Arg219Lys 15135251:170:57
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PMID: 14962947 [PubMed] Tregouet DA et al: "In-depth haplotype analysis of ABCA1 gene polymorphisms in relation to plasma ApoA1 levels and myocardial infarction."
No. Sentence Comment
7 Two polymorphisms were associated with plasma levels of ApoA1, 1 in the promoter (C-564T) and 1 in the coding (R1587K) regions, whereas only 1 polymorphism (R219K) was associated with the risk of MI.
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ABCA1 p.Arg219Lys 14962947:7:157
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79 Strong LD was also present in the coding region for 1 cluster of polymorphisms (R219K, G316G, I680I, V771 M, V825I, I883 M) located in exons 8 to 17.
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ABCA1 p.Arg219Lys 14962947:79:80
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84 Description and Frequency of ABCA1 Gene Polymorphisms in the 2 Centers From the United Kingdom Sequence Allele Frequency† Name 5Ј Flanking Nucleotide Change 3Ј Flanking Belfast (Nϭ888) Glasgow (Nϭ725) A-1814G CAGCCTCCTG A/g GATAACAGGC 0.339 0.366 C-1801T TAACAGGCGC C/t CGCCACCACA 0.443 0.433 A-1652G CACTGCGCCC A/g GCTCAGATCC 0.350 0.364 G-1506C CTCTTCTATG G/c GTCTGTCCTG 0.203 0.205 C-1395T TGAATGTCTG C/t ATGCAGGTGG 0.428 0.425 G-1252A TGCCCTTCAA G/a GTGGCTACAA 0.095 0.088 C-1217T AGGTAGGAGA C/t CTTGTGGCCT 0.120 0.121 -1034ins/del ATATTTAGAC ϮAT ATGGTGTGTA 0.210 0.220 T-940G GGCAAACAGA T/g AAGTTGGAGG 0.486 0.483 G-803A AAATTAAAAG G/a GGGCTGGTCC 0.108 0.093 -777rpt/23nt* CTGTGTTTTTGTTTGTTTGTTTC 0.527 0.518 -777rpt/28nt CTGTGTTTTTGTTTGTTTTGTTTGTTTC 0.267 0.272 -777rpt/32nt CTGTGTTTTTGTTTGTTTGTTTTGTTTGTTTC 0.206 0.210 C-564T GAGGACTGTC C/t GCCTTCCCCT 0.456 0.472 G-407C GCGGAAAGCA G/c GATTTAGAGG 0.455 0.459 C-302T CGTCTTAGGC C/t GGCGGGCCCG 0.196 0.189 G-278C GGGGGAAGGG G/c ACGCAGACCG 0.435 0.424 C-14T GGAACTAGTC C/t CGGCAAAAAC 0.335 0.346 R219K GGCCTACCAA G/a GGAGAAACTG 0.283 0.278 G316G AGGGAGGGGG G/a CTGAAGATCA 0.114 0.095 I680I ACAACAGCAT C/a CTCTGGTTTA 0.129 0.118 V771 M GCAGGACTAC G/a TGGGCTTCAC 0.029 0.034 V825I CACCACTTCG G/a TCTCCATGAT 0.056 0.060 I883 M AGAAGAGAAT A/g TCAGAAAGTA 0.137 0.126 L1122L GAAGAACCAG C/t TGGGAACAGG 0.023 0.017 E1172D GCGACCATGA G/c AGTGACACGC 0.026 0.027 T1427T GCAGAGACAC G/a CCCTGCCAGG 0.069 0.083 R1587K CTGGACACCA G/a AAATAATGTC 0.216 0.226 *1 subject carried an additional GTTT deletion, leading to an allele of 19 nucleotides.
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ABCA1 p.Arg219Lys 14962947:84:1087
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98 Coding Region By single-locus analysis, the R219K polymorphism was associated with MI, with K219 allele being associated with a decreased risk consistently in the 2 centers (population adjusted ORϭ0.80 [0.68-0.94], Pϭ0.007).
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ABCA1 p.Arg219Lys 14962947:98:44
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104 The "best" model encountered in the systematic exploration was the model with the R219K polymorphism alone, suggesting that apart from the raw effect of the R219K polymorphism, no other polymorphism was associated with the risk of MI.
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ABCA1 p.Arg219Lys 14962947:104:82
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ABCA1 p.Arg219Lys 14962947:104:157
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124 Discussion Much attention has been focused on the association of ABCA1 gene polymorphisms with different phenotypes including lipid variables and clinical endpoints.23,25-29,39 Several studies have consistently reported an association between the R219K polymorphism and coronary artery disease.23,26,27 This polymorphism has been shown to be associated with triglycerides23 but not with HDL-C.26,27 Inconsistent results were also observed for other ABCA1 gene polymorphisms including V825I, I883 M, and E1172D.
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ABCA1 p.Arg219Lys 14962947:124:247
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133 Haplotype Structure Defined by the Polymorphisms of the ABCA1 Gene Coding Region (N‫)6921؍‬ Polymorphisms Estimated Haplotype Frequencies R219K G316G (G/A) I680I (C/A) V771 M V825I I883 M L1122L (C/T) E1172D T1427T (G/A) R1587K Controls (Nϭ639) Cases (Nϭ657) R G C V V I C E G R 0.470 0.522 R G C V V I C E G K 0.089 0.085 R G C V V I C E A R 0.026 0.031 R G C V V I C D G K 0.018 0.019 R G C V V I T E G R 0.016 0.017 R G A V I M C E G R 0.015 0.015 R G A V I M C E G K 0.015 0.015 R G A V I M C E A R 0.028 0.026 K G C V V I C E G R 0.077 0.063 K G C V V I C E G K 0.041 0.037 K G A V V M C E G R 0.026 0.020 K G A V V M C E G K 0.014 0.012 K G A V V M C E A R 0.016 0.019 K A C V V I C E G R 0.042 0.035 K A C V V I C E G K 0.034 0.027 K A C M V I C E G R 0.028 0.027 The haplotype structure of the coding region of the ABCA1 gene can be completely defined by a minimal subset of 8 "tag" polymorphisms indicated in boxes.
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ABCA1 p.Arg219Lys 14962947:133:158
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144 Conversely, the R219K polymorphism was associated with MI but not with ApoA1 levels.
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ABCA1 p.Arg219Lys 14962947:144:16
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149 There are also a number of inconsistencies in the results that we are unable to explain for the moment, especially the fact that R1587K affects plasma ApoA1 but appears unrelated to MI and conversely that R219K is associated with MI but does not affect plasma ApoA1 levels.
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ABCA1 p.Arg219Lys 14962947:149:205
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3 Two polymorphisms were associated with plasma levels of ApoA1, 1 in the promoter (C-564T) and 1 in the coding (R1587K) regions, whereas only 1 polymorphism (R219K) was associated with the risk of MI.
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ABCA1 p.Arg219Lys 14962947:3:157
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75 Strong LD was also present in the coding region for 1 cluster of polymorphisms (R219K, G316G, I680I, V771 M, V825I, I883 M) located in exons 8 to 17.
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ABCA1 p.Arg219Lys 14962947:75:80
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80 Description and Frequency of ABCA1 Gene Polymorphisms in the 2 Centers From the United Kingdom Sequence Allele Frequencyߤ Name 5b18; Flanking Nucleotide Change 3b18; Flanking Belfast (Nafd;888) Glasgow (Nafd;725) A-1814G CAGCCTCCTG A/g GATAACAGGC 0.339 0.366 C-1801T TAACAGGCGC C/t CGCCACCACA 0.443 0.433 A-1652G CACTGCGCCC A/g GCTCAGATCC 0.350 0.364 G-1506C CTCTTCTATG G/c GTCTGTCCTG 0.203 0.205 C-1395T TGAATGTCTG C/t ATGCAGGTGG 0.428 0.425 G-1252A TGCCCTTCAA G/a GTGGCTACAA 0.095 0.088 C-1217T AGGTAGGAGA C/t CTTGTGGCCT 0.120 0.121 afa;1034ins/del ATATTTAGAC afe;AT ATGGTGTGTA 0.210 0.220 T-940G GGCAAACAGA T/g AAGTTGGAGG 0.486 0.483 G-803A AAATTAAAAG G/a GGGCTGGTCC 0.108 0.093 afa;777rpt/23nt* CTGTGTTTTTGTTTGTTTGTTTC 0.527 0.518 afa;777rpt/28nt CTGTGTTTTTGTTTGTTTTGTTTGTTTC 0.267 0.272 afa;777rpt/32nt CTGTGTTTTTGTTTGTTTGTTTTGTTTGTTTC 0.206 0.210 C-564T GAGGACTGTC C/t GCCTTCCCCT 0.456 0.472 G-407C GCGGAAAGCA G/c GATTTAGAGG 0.455 0.459 C-302T CGTCTTAGGC C/t GGCGGGCCCG 0.196 0.189 G-278C GGGGGAAGGG G/c ACGCAGACCG 0.435 0.424 C-14T GGAACTAGTC C/t CGGCAAAAAC 0.335 0.346 R219K GGCCTACCAA G/a GGAGAAACTG 0.283 0.278 G316G AGGGAGGGGG G/a CTGAAGATCA 0.114 0.095 I680I ACAACAGCAT C/a CTCTGGTTTA 0.129 0.118 V771 M GCAGGACTAC G/a TGGGCTTCAC 0.029 0.034 V825I CACCACTTCG G/a TCTCCATGAT 0.056 0.060 I883 M AGAAGAGAAT A/g TCAGAAAGTA 0.137 0.126 L1122L GAAGAACCAG C/t TGGGAACAGG 0.023 0.017 E1172D GCGACCATGA G/c AGTGACACGC 0.026 0.027 T1427T GCAGAGACAC G/a CCCTGCCAGG 0.069 0.083 R1587K CTGGACACCA G/a AAATAATGTC 0.216 0.226 *1 subject carried an additional GTTT deletion, leading to an allele of 19 nucleotides.
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ABCA1 p.Arg219Lys 14962947:80:1110
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94 Coding Region By single-locus analysis, the R219K polymorphism was associated with MI, with K219 allele being associated with a decreased risk consistently in the 2 centers (population adjusted ORafd;0.80 [0.68-0.94], Pafd;0.007).
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ABCA1 p.Arg219Lys 14962947:94:44
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100 The "best" model encountered in the systematic exploration was the model with the R219K polymorphism alone, suggesting that apart from the raw effect of the R219K polymorphism, no other polymorphism was associated with the risk of MI.
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ABCA1 p.Arg219Lys 14962947:100:82
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ABCA1 p.Arg219Lys 14962947:100:157
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120 Discussion Much attention has been focused on the association of ABCA1 gene polymorphisms with different phenotypes including lipid variables and clinical endpoints.23,25-29,39 Several studies have consistently reported an association between the R219K polymorphism and coronary artery disease.23,26,27 This polymorphism has been shown to be associated with triglycerides23 but not with HDL-C.26,27 Inconsistent results were also observed for other ABCA1 gene polymorphisms including V825I, I883 M, and E1172D.
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ABCA1 p.Arg219Lys 14962947:120:247
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129 Haplotype Structure Defined by the Polymorphisms of the ABCA1 Gene Coding Region (Nd1d;1296) Polymorphisms Estimated Haplotype Frequencies R219K G316G (G/A) I680I (C/A) V771 M V825I I883 M L1122L (C/T) E1172D T1427T (G/A) R1587K Controls (Nafd;639) Cases (Nafd;657) R G C V V I C E G R 0.470 0.522 R G C V V I C E G K 0.089 0.085 R G C V V I C E A R 0.026 0.031 R G C V V I C D G K 0.018 0.019 R G C V V I T E G R 0.016 0.017 R G A V I M C E G R 0.015 0.015 R G A V I M C E G K 0.015 0.015 R G A V I M C E A R 0.028 0.026 K G C V V I C E G R 0.077 0.063 K G C V V I C E G K 0.041 0.037 K G A V V M C E G R 0.026 0.020 K G A V V M C E G K 0.014 0.012 K G A V V M C E A R 0.016 0.019 K A C V V I C E G R 0.042 0.035 K A C V V I C E G K 0.034 0.027 K A C M V I C E G R 0.028 0.027 The haplotype structure of the coding region of the ABCA1 gene can be completely defined by a minimal subset of 8 "tag" polymorphisms indicated in boxes.
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ABCA1 p.Arg219Lys 14962947:129:142
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140 Conversely, the R219K polymorphism was associated with MI but not with ApoA1 levels.
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ABCA1 p.Arg219Lys 14962947:140:16
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145 There are also a number of inconsistencies in the results that we are unable to explain for the moment, especially the fact that R1587K affects plasma ApoA1 but appears unrelated to MI and conversely that R219K is associated with MI but does not affect plasma ApoA1 levels.
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ABCA1 p.Arg219Lys 14962947:145:205
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PMID: 15024730 [PubMed] Katzov H et al: "Genetic variants of ABCA1 modify Alzheimer disease risk and quantitative traits related to beta-amyloid metabolism."
No. Sentence Comment
74 Details of ABCA1 SNPs, and Oligos for PCR and DASHn Variant dbSNP rsID Base change Forward primer sequence (50 ^30 ) Reverse primer sequence (30 ^50 ) Probe sequence (50 ^30 ) p.R219K rs2230806 c.658G4A g.10300705G4A b-TTTCTGAGCTTTGTGGCCTACC GCTCTGCTGCAGCCAGTTTCTC GTTTCTCCCTTGGTAGG p.V771M rs2066718 c.2314G4A g.102969093G4A b-TGTGTGTGGCATGGCAGGACTA GCGAAGATCTTGAGTGTGAAGC GAAGCCCACGTAGTCCT p.V825I rs4149312 c.2476G4A g.102967871G4A b-ATGGCTTCAATCTCACCACTTG GGTGTCAAACAGCATCATGGAG CATGGAGACCCAAGTGG p.I883M rs4149313 c.2650A4G g.102966591A4G b-GAGGTCAACAGCACTTACTTTCT AGAAGAGCCACCCTTGTTCCAA AAGAGAATGTCAGAAAG p.R1587K rs2230808 c.4762G4A g.102942642G4A b-ATTTATGACAGGACTGGACACC AGCGGTTTACCTTGACATTATT CATTATTTCTGGTGTCC n Genotyping of SNPs was performed using dynamic allele speci'c hybridization (DASH) [Prince et al., 2001].
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ABCA1 p.Arg219Lys 15024730:74:178
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81 Among these models, significant association for marker rs2230806 (c.658G4A, p.R219K) was observed (P=0.014 for genotypes, P=0.048 for alleles; Table 3).
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ABCA1 p.Arg219Lys 15024730:81:78
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93 Single MarkerAssociations forABCA1and Alzheimer Diseasew p.R219K (rs2230806) G/G G/A A/A P value Set A AD 238 (.62) 125 (.33) 21 (.05) 0.014n Controls 102 (.58) 51 (.29) 22 (.13) Set B AD 58 (.48) 53 (.44) 9 (.08) 0.76 Controls 76 (.53) 59 (.41) 9 (.06) Set C AD 82 (.57) 53 (.37) 8 (.06) 0.66 Controls 183 (.56) 117 (.36) 26 (.08) Set D AD 183 (.56) 122 (.37) 22 (.07) 0.93 Controls 60 (.57) 40 (.38) 6 (.06) p.I883M (rs4149313) C/C C/T T/T Set A AD 2 (.01) 81 (.21) 301 (.78) 0.39 Controls 0 (.00) 31 (.18) 145 (.82) Set B AD 0 (.00) 29 (.24) 91 (.76) 0.27 Controls 3 (.02) 32 (.21) 115 (.77) Set C AD 2 (.01) 27 (.19) 116 (.80) 0.84 Controls 3 (.01) 53 (.17) 256 (.82) Set D AD 3 (.01) 68 (.21) 253 (.78) 0.61 Controls 2 (.02) 19 (.19) 83 (.80) p.R1587K (rs2230808) G/G G/A A/A Set A AD 253 (.66) 114 (.30) 15 (.04) 0.13 Controls 101 (.57) 66 (.38) 9 (.05) Set B AD 56 (.46) 58 (.48) 7 (.06) 0.016n Controls 96 (.64) 48 (.32) 7 (.05) Set C AD 80 (.55) 56 (.39) 9 (.06) 0.70 Controls 189 (.58) 121 (.37) 15 (.05) Det D AD 185 (.57) 118 (.36) 24 (.07) 0.18 Controls 68 (.64) 28 (.26) 10 (.09) p.V771M (rs2066718) G/G G/A A/A Set A AD 365 (.95) 20 (.05) 0 (.00) 0.28 Controls 167 (.95) 7 (.04) 1 (.01) Set B AD 109 (.98) 2 (.02) 0 (.00) 0.029n Controls 126 (.92) 11 (.08) 0 (.00) p.V825I (rs4149312) G/G G/A A/A Set A AD 341 (.93) 20 (.05) 4 (.01) 0.17 Controls 164 (.92) 15 (.08) 0 (.00) w Genotype frequencies for all studied SNPs in ABCA1 are presented.
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ABCA1 p.Arg219Lys 15024730:93:59
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144 Single Marker QuantitativeTrait Associationsn p.R219K (rs2230806) Trait G/G G/A A/A P-value Set A CSF Tau 6407280 (156) 6447280 (78) 7097240 (12) NS CSFAb42 4627167 (149) 4877176 (75) 5067230 (11) NS AAO 72.478.4 (205) 72.377.8 (99) 72.577.0 (18) NS SP-NFT 7.472.0 (43) 6.972.2 (25) 4.771.2 (3) 0.039 Set B AAO 52.077.6 (56) 52.276.2 (52) 55.474.9 (8) NS Set C AAO 76.777.1 (80) 77.276.4 (52) 74.478.1 (8) NS Set D Ab load 4.671.9 (35) 4.372.3 (26) 4.972.7 (7) NS AAO 71.9712.3 (81) 7378.9 (58) 70.176.2 (10) NS p.I883M (rs4149313) Trait C/C C/T T/T Set A CSF Tau 5747318 (2) 6907328 (52) 6337262 (192) NS CSFAb42 354754 (2) 4437137 (48) 4817181 (185) NS AAO 64.978.6 (2) 72.078.8 (68) 72.477.8 (253) NS SP-NFT N/A 6.372.4 (16) 7.371.9 (55) 0.078 Set B AAO N/A 52.075.7 (28) 52.477.2 (88) NS Set C AAO 73.5719.
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ABCA1 p.Arg219Lys 15024730:144:48
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201 The observation of an association with the common rs2230806 (R219K) variant was in indirect agreement with a smaller, recently published study, which suggested an effect upon AAO [Wollmer et al., 2003].
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ABCA1 p.Arg219Lys 15024730:201:61
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PMID: 14986172 [PubMed] Shioji K et al: "A promoter variant of the ATP-binding cassette transporter A1 gene alters the HDL cholesterol level in the general Japanese population."
No. Sentence Comment
28 Well-known common variants, ABCA1 R219K and I823M, were also selected (Wang et al. 2000; Clee et al. 2001; Harada et al. 2003).
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ABCA1 p.Arg219Lys 14986172:28:34
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65 Among the polymorphisms selected from JSNPs, including R219K and I823M, only the IMS-JST071749 polymorphism was associated with the HDL-C level (P=0.0060 adjusted for age, sex, BMI, smoking, and consumption of alcohol; P=0.0093 when also adjusted for the ApoE and ApoA1 (IMS-JST005603) genotypes).
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ABCA1 p.Arg219Lys 14986172:65:55
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66 The R219K and I823M polymorphisms were not associated with the HDL-C level [P=0.3877 (R219K) and P=0.2286 (I823M) adjusted for age, sex, BMI, smoking and consumption of alcohol; P=0.1926 (R219K) and P=0.1209 (I823M) when also adjusted for the ApoE and ApoA1 genotypes].
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ABCA1 p.Arg219Lys 14986172:66:4
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ABCA1 p.Arg219Lys 14986172:66:86
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ABCA1 p.Arg219Lys 14986172:66:188
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PMID: 14681836 [PubMed] Albrecht C et al: "Leukocyte ABCA1 gene expression is associated with fasting glucose concentration in normoglycemic men."
No. Sentence Comment
16 More common variants in the gene encoding ABCA1, such as the R219K variant, which has a carrier frequency of 46% in Europeans, are also associated with altered lipid levels and a modified risk of CHD.9 The association between ABCA1 and CHD is only partly explained by HDL-cholesterol concentrations.
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ABCA1 p.Arg219Lys 14681836:16:61
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PMID: 14644402 [PubMed] Kuivenhoven JA et al: "Heterozygosity for ABCA1 gene mutations: effects on enzymes, apolipoproteins and lipoprotein particle size."
No. Sentence Comment
141 With respect to R219K that we have described to be associated with decreased TG levels [25], this can be explained by the fact that this mutation is thought to enhance ABCA1 function, while the defects studied in the present report concern loss-of-function mutations.
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ABCA1 p.Arg219Lys 14644402:141:16
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PMID: 14576201 [PubMed] Hong SH et al: "Novel polypyrimidine variation (IVS46: del T -39...-46) in ABCA1 causes exon skipping and contributes to HDL cholesterol deficiency in a family with premature coronary disease."
No. Sentence Comment
97 Moreover, several noncoding (eg, C-17G) and coding (eg, R219K) single-nucleotide polymorphisms that do not affect levels of HDL-C have coincided with reduced CHD.23,24 In contrast, most but not all studies evaluating ABCA1 variants have demonstrated an association TABLE 1.
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ABCA1 p.Arg219Lys 14576201:97:56
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92 Moreover, several noncoding (eg, C-17G) and coding (eg, R219K) single-nucleotide polymorphisms that do not affect levels of HDL-C have coincided with reduced CHD.23,24 In contrast, most but not all studies evaluating ABCA1 variants have demonstrated an association TABLE 1.
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ABCA1 p.Arg219Lys 14576201:92:56
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PMID: 12763760 [PubMed] Singaraja RR et al: "Efflux and atherosclerosis: the clinical and biochemical impact of variations in the ABCA1 gene."
No. Sentence Comment
136 Single Nucleotide Polymorphisms in the ABCA1 Gene Nucleotide Amino Acid Exon -1095A/G Promoter ⅐ ⅐ ⅐ -477C/T Promoter ⅐ ⅐ ⅐ -419A/C Promoter ⅐ ⅐ ⅐ -320G/C Promoter ⅐ ⅐ ⅐ -191G/C Promoter ⅐ ⅐ ⅐ C69T 5ЈUTR 1 C117G 5ЈUTR 1 InsG319 5ЈUTR 2 G378C 5ЈUTR 2 G1051A R219K 7 T1591C V399A 11 G2706A V771M 16 A2715C T774P 16 G2723C K776N 16 G2826A V825I 17 A3044G I883M 18 G3911C E1172D 24 G5255A R1587K 35 C5587G S1731C 38 markers, namely, increased arterial wall thickness and ABCA1-mediated cholesterol efflux, was performed.73 The study group consisted of 30 individuals heterozygous for 4 different missense mutations in the ABCA1 gene, C1477R, M1091T, P2150L, and T929I.
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ABCA1 p.Arg219Lys 12763760:136:386
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147 The R219K, V771M, and I883M variants have been recognized as putative antiatherogenic polymorphisms, associated with increased HDL-C and decreased triglyceride levels (K219 and M883) and increased HDL-C and ApoA-I (M771).41,75,82 The E1172D, R1587K cSNPs have been reported to be associated with decreased HDL-C.75 Five promoter SNPs are associated with increased severity of atherosclerosis, including the -191C/-320C/-477T hap- lotype76,78 as well as the G-191C and A-1096G SNPs.
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ABCA1 p.Arg219Lys 12763760:147:4
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148 In TABLE 4. Conservation of Amino Acids Polymorphic in Humans cSNP H. sapiens M. musculus G. gallus D. melanogaster C. elegans R219K R R K ⅐ ⅐ ⅐ L V399A V V V A I V771M V V V L Y T774P T S S S G K776N K K K K R V825I V V A M L I883M I V P R A E1172D E E E ⅐ ⅐ ⅐ ⅐ ⅐ ⅐ R1587K R K K E V S1731C S S S T H Five of 10 (50%) amino acids at which cSNPs occur are conserved with G. gallus, indicating a relatively less crucial functional role of these residues compared with those at which mutations occur (Figure 2).
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ABCA1 p.Arg219Lys 12763760:148:127
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153 The V825I, I883M, and E1172D SNPs have also been associated with increased clinical events and severity of atherosclerosis.75,77 The R219K Variant The R219K SNP has been most studied and highlights many of the difficulties associated with the study of SNPs in general.
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ABCA1 p.Arg219Lys 12763760:153:133
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ABCA1 p.Arg219Lys 12763760:153:151
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160 Clee et al75 reported significant LD between the R219K and the V771M, K776N, I883M, and R1587K cSNPs but found that after carriers of these variants were excluded, R219K remained significantly associated with degree of atherosclerosis and triglyceride levels.
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ABCA1 p.Arg219Lys 12763760:160:49
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ABCA1 p.Arg219Lys 12763760:160:164
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162 Functional Effects of cSNPs and Regulatory SNPs in the ABCA1 Gene Nucleotide Amino Acid/Position Lipids CAD/Atherosclerosis Antiatherogenic SNPs C-17G Promoter No change 2 InsG319 5ЈUTR No change 2 G1051A R219K 2 TG, 1 HDL, 1 ApoA-1, 1 ApoB, 1 LDL 2 A3044G I883M 2 TG, 1 HDL 1 Proatherogenic SNPs -191C/-320C/-477T haplotype Promoter No change 1 G-191C Promoter No change 1 A-1095G Promoter No change 1 C117G 5ЈUTR 1 TG No change G2706A V771M No change 1 G2868A V825I No change 1 G3911C E1172D 2 HDL, 2 ApoB 1 G5155A R1587K 2 HDL No change Associations with lipid levels and CAD are shown by arrows to represent the direction of association.
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ABCA1 p.Arg219Lys 12763760:162:211
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171 The noncoding SNPs G-191C, C-69T, C-17G, and InsG319 and the cSNPs R219K, V771M, and V825I have all been found to be associated with differences in severity of atherosclerosis but not with changes in HDL-C levels in at least 1 study.
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ABCA1 p.Arg219Lys 12763760:171:67
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128 Single Nucleotide Polymorphisms in the ABCA1 Gene Nucleotide Amino Acid Exon afa;1095A/G Promoter ዼ ዼ ዼ afa;477C/T Promoter ዼ ዼ ዼ afa;419A/C Promoter ዼ ዼ ዼ afa;320G/C Promoter ዼ ዼ ዼ afa;191G/C Promoter ዼ ዼ ዼ C69T 5b18;UTR 1 C117G 5b18;UTR 1 InsG319 5b18;UTR 2 G378C 5b18;UTR 2 G1051A R219K 7 T1591C V399A 11 G2706A V771M 16 A2715C T774P 16 G2723C K776N 16 G2826A V825I 17 A3044G I883M 18 G3911C E1172D 24 G5255A R1587K 35 C5587G S1731C 38 Singaraja et al Clinical and Biochemical Impact of ABCA1 Variants markers, namely, increased arterial wall thickness and ABCA1-mediated cholesterol efflux, was performed.73 The study group consisted of 30 individuals heterozygous for 4 different missense mutations in the ABCA1 gene, C1477R, M1091T, P2150L, and T929I.
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ABCA1 p.Arg219Lys 12763760:128:401
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139 The R219K, V771M, and I883M variants have been recognized as putative antiatherogenic polymorphisms, associated with increased HDL-C and decreased triglyceride levels (K219 and M883) and increased HDL-C and ApoA-I (M771).41,75,82 The E1172D, R1587K cSNPs have been reported to be associated with decreased HDL-C.75 Five promoter SNPs are associated with increased severity of atherosclerosis, including the afa;191C/afa;320C/afa;477T hap- lotype76,78 as well as the G-191C and A-1096G SNPs.
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ABCA1 p.Arg219Lys 12763760:139:4
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140 In TABLE 4. Conservation of Amino Acids Polymorphic in Humans cSNP H. sapiens M. musculus G. gallus D. melanogaster C. elegans R219K R R K ዼ ዼ ዼ L V399A V V V A I V771M V V V L Y T774P T S S S G K776N K K K K R V825I V V A M L I883M I V P R A E1172D E E E ዼ ዼ ዼ ዼ ዼ ዼ R1587K R K K E V S1731C S S S T H Five of 10 (50%) amino acids at which cSNPs occur are conserved with G. gallus, indicating a relatively less crucial functional role of these residues compared with those at which mutations occur (Figure 2).
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ABCA1 p.Arg219Lys 12763760:140:127
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145 The V825I, I883M, and E1172D SNPs have also been associated with increased clinical events and severity of atherosclerosis.75,77 The R219K Variant The R219K SNP has been most studied and highlights many of the difficulties associated with the study of SNPs in general.
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ABCA1 p.Arg219Lys 12763760:145:133
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152 Clee et al75 reported significant LD between the R219K and the V771M, K776N, I883M, and R1587K cSNPs but found that after carriers of these variants were excluded, R219K remained significantly associated with degree of atherosclerosis and triglyceride levels.
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ABCA1 p.Arg219Lys 12763760:152:49
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154 Functional Effects of cSNPs and Regulatory SNPs in the ABCA1 Gene Nucleotide Amino Acid/Position Lipids CAD/Atherosclerosis Antiatherogenic SNPs C-17G Promoter No change 2 InsG319 5b18;UTR No change 2 G1051A R219K 2 TG, 1 HDL, 1 ApoA-1, 1 ApoB, 1 LDL 2 A3044G I883M 2 TG, 1 HDL 1 Proatherogenic SNPs afa;191C/afa;320C/afa;477T haplotype Promoter No change 1 G-191C Promoter No change 1 A-1095G Promoter No change 1 C117G 5b18;UTR 1 TG No change G2706A V771M No change 1 G2868A V825I No change 1 G3911C E1172D 2 HDL, 2 ApoB 1 G5155A R1587K 2 HDL No change Associations with lipid levels and CAD are shown by arrows to represent the direction of association.
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ABCA1 p.Arg219Lys 12763760:154:211
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163 The noncoding SNPs G-191C, C-69T, C-17G, and InsG319 and the cSNPs R219K, V771M, and V825I have all been found to be associated with differences in severity of atherosclerosis but not with changes in HDL-C levels in at least 1 study.
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ABCA1 p.Arg219Lys 12763760:163:67
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PMID: 12870173 [PubMed] Srinivasan SR et al: "R219K polymorphism of the ABCA1 gene and its modulation of the variations in serum high-density lipoprotein cholesterol and triglycerides related to age and adiposity in white versus black young adults. The Bogalusa heart study."
No. Sentence Comment
0 R219K Polymorphism of the ABCA1 Gene and Its Modulation of the Variations in Serum High-Density Lipoprotein Cholesterol and Triglycerides Related to Age and Adiposity in White Versus Black Young Adults.
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2 However, information regarding the frequency of common variants, including Arg219Lys (R219K) within the coding region of the ABCA1 gene and their effect on these phenotypes in the general population is limited.
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ABCA1 p.Arg219Lys 12870173:2:75
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3 This study examined the frequency and phenotypic effect of R219K variant in a community-based sample of 887 white and 390 black young adults aged 20 to 38 years.
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10 SERUM HIGH-DENSITY lipoprotein (HDL) cholesterol is inversely related to coronary artery disease (CAD).1 This has been attributed, in part, to the key role HDL plays in the transport of cholesterol from peripheral tissues including the arterial wall to the liver, an antiatherogenic process known as reverse cholesterol transport.2 In addition, HDL is metabolically inversely related to triglyceride-rich lipoproteins,3,4 another strong risk factor for CAD.5 In the general population, factors such as age, race, sex, body fatness, variability in lipoprotein lipase, hepatic triglyceride lipase, and cholesteryl ester transfer protein activities and apolipoprotein (apo) A-I production rate influence HDL cholesterol levels.6-10 It has been known that familial disorders of HDL metabolism contribute to very low levels of HDL cholesterol.11 Mutations in the gene encoding adenosine triphosphate (ATP)- binding cassette transporter 1 (ABCA1) have been identified as the molecular basis of 2 familial HDL disorders, Tangier disease and familial hypoalphalipoproteinemia.12-14 As a cholesterol efflux regulatory protein, ABCA1 participates in the biogenesis of HDL by facilitating both translocation of cholesterol and phospholipid to the plasma membrane and efflux on to lipid poor apo A-I particles.15,16 Because mutations associated with severe functional impairment of ABCA1 are not common among individuals with low HDL cholesterol, research has been focused recently on common single nucleotide polymorphisms in the coding and promotor regions of ABCA1.17-20 The ABCA1 gene, localized on chromosome 9q31, contains 49 exons that range in size from 33 to 249 bp and is over 70 kb in length.21 A G to A transversion at nucleotide position 1051 in exon 7 results in the substitutions of a lysine for arginine at amino acid residue 219 (R219K).
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ABCA1 p.Arg219Lys 12870173:10:1788
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12 As part of the Bogalusa Heart Study, a biracial (black-white) community-based investigation of early natural history of cardiovascular disease, the present study examines the 219K allele frequency and the effect of R219K polymorphism on serum HDL cholesterol and triglycerides in young adults.
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14 Of these, 1,277 individuals (887 whites and 390 blacks) aged 20 to 38 years who had ABCA1 R219K genotype data formed the study sample for this report.
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30 Genotyping of R219K Polymorphism Genotyping of the ABCA1 R219K variant was performed using the TaqMan assay (Applied Biosystems, Foster City, CA).
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ABCA1 p.Arg219Lys 12870173:30:14
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35 Based on the analysis of 67 pairs of blind duplicates, there was 98.5% concordance in R219K genotyping.
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41 Multiple regression model was used to examine the independent effects of R219K polymorphism and the interaction effect between genotype and age, sex, or BMI (or subscapular skinfold) on levels of HDL cholesterol and triglycerides.
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42 RESULTS The R219K genotype and allele frequencies by race are given in Table 1.
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45 Genotype and Allele Frequencies for the R219K Polymorphism of ABCA1 Gene by Race: The Bogalusa Heart Study White (n ϭ 887) Count (%) Black (n ϭ 390) Count (%) Genotype* RR 495 (55.8) 63 (16.2) RK 320 (36.1) 190 (48.7) KK 72 (8.1) 137 (35.1) Allele* R 1,310 (73.8) 316 (40.5) K 464 (26.2) 464 (59.5) *Race difference, P Ͻ .001.
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47 Levels of Serum HDL Cholesterol and Triglycerides in Whites and Blacks by R219K Genotype of ABCA1: The Bogalusa Heart Study K219 Allele PNoncarrier Carrier Whites No.
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66 DISCUSSION The present community-based study demonstrates that (1) the relative allele frequency of the R219K polymorphism of the ABCA1 gene differs markedly between blacks and whites and (2) the R219K variant significantly alters association of HDL cholesterol with age, and triglycerides with adiposity in whites, but not in blacks.
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ABCA1 p.Arg219Lys 12870173:66:104
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70 Heterozygotes for ABCA1 deficiency have decreased HDL cholesterol and increased triglycerides.24,25 In contrast, the phenotypic effects of the common variants, such as R219K and I823M located in the coding region of the ABCA1 gene, are found to be just opposite, suggesting these common variants are associated with an enhanced ABCA1 function.17,18 In the current study, no genotypic effects on HDL cholesterol and triglycerides were apparent in whites or blacks. However, when interaction terms of genotype with age, sex, or adiposity were included in the model, significant interaction effects of genotype and age on HDL cholesterol and genotype and adiposity on triglycerides were noted in whites, but not in blacks.
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ABCA1 p.Arg219Lys 12870173:70:168
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72 Effect of Interaction Between R219K Genotype of ABCA1 and Age, Sex or BMI on Levels of Serum HDL Cholesterol and Triglycerides by Race: The Bogalusa Heart Study Independent Variable White Black HDL Cholesterol Triglycerides* HDL Cholesterol Triglycerides* beta† P beta P beta P beta P Age -0.122 .240 0.010 .045 0.385 .303 0.004 .736 Sex 7.056 Ͻ.001 -0.055 .265 -1.604 .692 -0.264 .052 BMI -0.646 Ͻ.001 0.045 Ͻ.001 -0.899 Ͻ.001 0.016 .081 Genotype -0.449 .697 -0.061 .276 -2.260 .531 0.015 .906 Age* genotype 0.524 Ͻ.001 -0.006 .391 -0.484 .233 0.014 .305 Sex* genotype 0.744 .624 0.041 .576 3.891 .375 0.029 .844 BMI* genotype 0.019 .883 -0.014 .029 0.293 .311 -0.003 .779 NOTE.
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77 Relationship of serum HDL cholesterol to age in whites by R219K genotype of ABCA1.
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81 Based on earlier findings that the expression and activity of P-glycoprotein, another ABC transporter, increases with age,26 it has been suggested that ABCA1 activity may normally increase with age, but this was blunted in ABCA1 heterozygotes.24 With respect to common R219K polymorphism, an earlier study found that the age-related increases in HDL cholesterol and cholesterol efflux in older age groups (median age, 56.7 years) were also blunted in carriers of the K219 allele, although homozygous carriers of this common variant displayed reduced severity of CAD, decreased progression of atherosclerosis, and a trend toward increased HDL cholesterol.17 It is not clear whether differences in age and preexisting CAD among subjects between studies may account for the conflicting finding regarding R219K variant.
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ABCA1 p.Arg219Lys 12870173:81:269
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ABCA1 p.Arg219Lys 12870173:81:801
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85 The observed lack of phenotypic effects of R219K polymorphism and its interaction with age or adiposity in blacks suggests that other factors may play a dominant role in determining levels of HDL cholesterol and triglycerides in this group.
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87 Further, obesity has relatively less impact on these variables in blacks.9,10 Studies, including our own, have shown that blacks versus whites have markedly higher lipoprotein lipase activity and lower hepatic triglyceride lipase activity,30-32 key parameters associated with metabolism and systemic levels of triglyceride-rich lipoproteins and HDL.33 Because these metabolic parameters favor a relatively higher HDL cholesterol and lower triglyceride trait in blacks, the phenotypic effects of the R219K variant per se may not be evident in this group.
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ABCA1 p.Arg219Lys 12870173:87:499
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PMID: 12840658 [PubMed] Miller M et al: "Genetics of HDL regulation in humans."
No. Sentence Comment
64 TD 1051 G/A 7 R219K extracellular [67,68] FHA 1083 C/T 7 R230C extracellular [70] FHA 1158 G/A 8 A255T extracellular [75.]
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ABCA1 p.Arg219Lys 12840658:64:14
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PMID: 12600718 [PubMed] Wollmer MA et al: "ABCA1 modulates CSF cholesterol levels and influences the age at onset of Alzheimer's disease."
No. Sentence Comment
4 Healthy elderly carriers of the A allele of a non-synonymous (R219K) single nucleotide polymorphism (SNP) in the ABCA1 gene (rs2234884) had on average 33% lower total cholesterol in cerebrospinal fluid (CSF) than non-carriers.
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ABCA1 p.Arg219Lys 12600718:4:62
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112 Discussion We found that the A allele of a non-synonymous (R219K) SNP in ABCA1 (rs2234884) is associated with low cholesterol levels in the CSF of cognitively healthy elderly individuals.
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ABCA1 p.Arg219Lys 12600718:112:59
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PMID: 12700893 [PubMed] Evans D et al: "The association of the R219K polymorphism in the ATP-binding cassette transporter 1 ( ABCA1) gene with coronary heart disease and hyperlipidaemia."
No. Sentence Comment
0 Abstract The R219K polymorphism in the ATP-binding cassette transporter 1 gene (ABCA1) has been associated with reduced severity of atherosclerosis, fewer coronary events, decreased triglycerides and a trend to increased HDL in men with coronary heart disease (CHD).
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ABCA1 p.Arg219Lys 12700893:0:13
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7 In conclusion, we provide additional evidence that the R219K polymorphism in the ABCA1 gene either directly or as a result of linkage disequilibrium with additional functional variant(s), has a protective effect against CHD and is associated with lower plasma triglycerides in sub-groups of patients with hyperlipidaemia.
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10 Evans (✉) · F. U. Beil Klinik und Poliklinik für Innere Medizin, Medizinische Klinik I, Universitätsklinikum Hamburg-Eppendorf, Martinistrasse 52, 20246 Hamburg, Germany e-mail: evans@uke.uni-hamburg.de Tel.: +49-40-428036978, Fax: +49-40-428038290 J Mol Med (2003) 81:264-270 DOI 10.1007/s00109-003-0426-y O R I G I N A L A RT I C L E David Evans · F. Ulrich Beil The association of the R219K polymorphism in the ATP-binding cassette transporter 1 (ABCA1) gene with coronary heart disease and hyperlipidaemia Received: 31 October 2002 / Accepted: 16 January 2003 / Published online: 26 March 2003 (c) Springer-Verlag 2003 DAVID EVANS received his Ph.D. in virology in 1979 from the University of Glasgow, UK.
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ABCA1 p.Arg219Lys 12700893:10:415
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22 Clee et al. [15] investigated the phenotypic effects of the R219K polymorphism in 804 Dutch subjects with confirmed coronary artery disease.
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ABCA1 p.Arg219Lys 12700893:22:60
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31 The aim of this study was to investigate the role of the R219K polymorphism in CHD and plasma lipid levels in patients attending a lipid out-patient clinic.
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ABCA1 p.Arg219Lys 12700893:31:57
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44 Genotyping DNA was extracted using standard methods and the frequency of the R219K polymorphism in ABCA1 was determined as described by Clee et al. [15], apoE and lipoprotein lipase LPL polymorphisms were determined as described [19, 20, 21].
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ABCA1 p.Arg219Lys 12700893:44:77
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60 Carriers of the K allele had lower triglycerides and, although not statistically significant, the P value Table 2 R219K polymorphism in the ABCA1 gene and coronary heart disease (CHD) All Men Women* Lp(a)>20 mg/dl n Age (years) n Age (years) n Age (years) All** Men Women CHD present RR 72 56.1±1.5 49 54.7±1.9 23 59.2±2 33 22 11 RK+KK 35+7 54.5±1.8 25+7 53.1±1.9 10+0 59.2±3.9 13+1 9+1 4+0 K frequency 0.21 0.24 0.15 0.16 0.19 0.10 CHD absent RR 337 43.2±0.7 178 42.8±0.8 159 43.7±1.2 78 32 46 RK+KK 245+47 43.7±0.8 128+29 44.2±0.9 117+18 43.1±1.3 66+12 31+8 35+4 K frequency 0.27 0.28 0.26 0.29 0.31 0.24 *P=0.05, difference in allele frequency between the presence and absence of CHD in women (Fisher`s exact test) **P=0.007, combined difference in allele frequency between the presence and absence of CHD (Fisher's exact test) Table 3 R219K polymorphism in the ABCA1 gene and plasma lipids (HDL-c high-density lipoprotein cholesterol, LDL-c low-density lipoprotein cholesterol) Before treatment After diet advice RR (n=279) RK (n=206) KK (n=30) RR (n=338) RK (n=229) KK (n=43) Age (years) 45.8±0.6 45.3±0.7 45.6±2.2 45.9±1 46.2±1 43.7±2 Body mass index 26.4±0.2 26.2±0.3 25.9±0.7 26.5±0.2 26.1±0.3 24.4±1.6 Total cholesterol (mg/dl) 285±4.9 284±6.1 280±10 278±5 284±6 274±8 Triglycerides (mg/dl) 328±30 288±32 236±49 317±26 297±30 216±27 HDL-c (mg/dl) 51±1 52±1 49±12 47±1 48±1 45±2 LDL-c (mg/dl) 188±4 188±5 194±12 190±5 192±5 195±10 ApoB (mg/dl) 135±2 130±3 142±8 - - - ApoAI (mg/dl) 131±2 133±2 127±5 - - - Fig. 1 ABCA1 R219K genotype frequencies and coronary heart disease in patients with elevated (>20 mg/dl) lipoprotein(a) Table 4 R219K polymorphism in the ABCA1 gene and plasma triglycerides before treatment: successive exclusion of factors associated with elevated triglycerides and interaction with apoE genotype (DM2, triglycerides >1000 mg/dl, apoE 2/2, LPL D9N, N291S carriers excluded) Patients excluded RR RK KK Pb apoE genotype None 0.17 n 279 206 30 Triglycerides 328±30 288±32 236±49 DM2, triglycerides >1000 mg/dl 0.13 n 258 191 29 Triglycerides 232±11 207±13 195±27 DM2, triglycerides >1000 mg/dl, apoE 2/2 0.09 ns 255 188 29 Triglycerides 232±12 203±13 195±27 DM2, triglycerides >1000 mg/dl, apoE 2/2, 0.07 LPL D9N, N291S carriers n 194 141 22 Triglycerides 234±14 200±15 158±17 3/3 0.035 n 113 76 11 Triglycerides 200±15 152±14 148±14 */4a 0.24 n 70 53 8 Triglycerides 270±28 249±30 140±28 3/4 0.23 n 59 44 7 Triglycerides 250±28 256±34 125±27 2/3 0.87 n 15 12 3 Triglycerides 321±55 290±54 243±86 was lower (P=0.13 vs. 0.17) despite the lower number of patients.
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ABCA1 p.Arg219Lys 12700893:60:899
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ABCA1 p.Arg219Lys 12700893:60:1797
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76 Discussion In this communication we confirm in patients of both sexes with hyperlipidaemia the findings of Clee et al. [15] in men with CHD that the K allele of the R219K polymorphism in the ABCA1 gene has a protective effect against CHD and is associated with reduced plasma tri- glyceride levels.
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ABCA1 p.Arg219Lys 12700893:76:165
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80 Unlike Clee et al. [15] we did not find an association between the R219K polymorphism and HDL, nor did we find that the age of the patient affected the influence of the polymorphism; however, we did find an association with plasma triglycerides.
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ABCA1 p.Arg219Lys 12700893:80:67
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87 Clee et al. [15] found that the R219K polymorphism was in linkage disequilibrium with two less frequent variants, V771M and K776N; however, excluding patients who were also carriers of these polymorphisms did not alter the results they obtained for the R219K polymorphism.
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ABCA1 p.Arg219Lys 12700893:87:32
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ABCA1 p.Arg219Lys 12700893:87:253
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88 Similarly they observed that the R219K effects were independent of the I883M and R1587K variants.
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ABCA1 p.Arg219Lys 12700893:88:33
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90 Although there is considerable amount of linkage disequilibrium between the polymorphisms, they did not report the extent of disequilibrium with the R219K polymorphism.
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ABCA1 p.Arg219Lys 12700893:90:149
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91 Neither Brousseau et al. [16] nor Wang et al. [13] report on linkage disequilibrium between the R219K and other polymorphisms.
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ABCA1 p.Arg219Lys 12700893:91:96
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92 Lutucuta et al. [17] also reported the effect of polymorphisms in the promoter of the ABCA1 gene on coronary atherosclerosis but did not determine whether this was due to disequilibrium with the R219K polymorphism.
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ABCA1 p.Arg219Lys 12700893:92:195
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93 Therefore given the large number of polymorphisms described to date in the ABCA1 gene we cannot in this communication conclude that the effects which we see of the K allele of the R219K polymorphism are the direct result of the polymorphism, or whether it is a marker for functional variation elsewhere in the gene.
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ABCA1 p.Arg219Lys 12700893:93:180
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95 In conclusion here we provide evidence that the R219K polymorphism in the ABCA1 gene has a protective effect against CHD in patients at high risk due to hyperlipidaemia and especially those with concomitantly elevated Lp(a).
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PMID: 12624133 [PubMed] Cenarro A et al: "A common variant in the ABCA1 gene is associated with a lower risk for premature coronary heart disease in familial hypercholesterolaemia."
No. Sentence Comment
128 In order to know if the presence of the R219K variant in the ABCA1 gene could be a protective factor for premature CHD in FH, we have determined the presence of this genetic variant by amplification by PCR and restriction analysis in a group of 374 FH subjects, with and without premature CHD.
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ABCA1 p.Arg219Lys 12624133:128:40
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129 The K allele of the R219K variant was significantly more frequent in FH subjects without premature CHD (0.32, 95% CI 0.27 to 0.37) than in FH subjects with premature CHD (0.25, 95% CI 0.21 to 0.29) (p<0.05), suggesting that the genetic variant R219K in ABCA1 could influence the development and progression of atherosclerosis in FH subjects.
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ABCA1 p.Arg219Lys 12624133:129:20
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ABCA1 p.Arg219Lys 12624133:129:244
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130 Moreover, the K allele of the R219K polymorphism seems to modify CHD risk without important modification of plasma HDL-C levels, and it appears to be more protective for smokers than non-smokers.
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ABCA1 p.Arg219Lys 12624133:130:30
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137 In order to discover if the presence of the R219K polymorphism in the ABCA1 gene plays a protective role for premature CHD in FH, we have analysed this genetic variant in a group of FH subjects.
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ABCA1 p.Arg219Lys 12624133:137:44
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138 In this work, we report that the common variant R219K in the ABCA1 gene is significantly more frequent in FH subjects without premature CHD than in FH subjects with premature CHD, suggesting that genetic variation in ABCA1 influences the atherosclerosis process in FH subjects.
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195 R219K polymorphism analysis Genomic DNA from peripheral blood was isolated using a previously described method, with minor modifications.27 A 166 bp fragment of exon 7 of the ABCA1 gene involving nucleotide 1051 of the cDNA sequence28 was amplified by polymerase chain reaction (PCR), using the following primers: R219Ks: 5'-GCAAGGCTACCAGTTACATTTGACAAG-3' and R219Kas: 5'- GATTGGCTTCAGGATGTCCATGTTGG-3'.
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ABCA1 p.Arg219Lys 12624133:195:0
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206 Associations between R219K polymorphism and lipid data were analysed by multivariate ANOVA adjusted by age, gender, and BMI.
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ABCA1 p.Arg219Lys 12624133:206:21
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219 The R219K polymorphism is the result of a nucleotide change G→A at position 1051 of the cDNA sequence, and it results in the substitution of lysine for arginine at amino acid 219 of the ABCA1 protein.
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ABCA1 p.Arg219Lys 12624133:219:4
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ABCA1 p.Arg219Lys 12624133:219:147
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222 The R219K polymorphism was in Hardy-Weinberg equilibrium in the control and premature CHD groups.
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ABCA1 p.Arg219Lys 12624133:222:4
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223 The genotype frequency distribution for the R219K polymorphism is shown in table 2.
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ABCA1 p.Arg219Lys 12624133:223:44
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226 The allelic frequencies for the minor K allele of the R219K polymorphism were 0.32 (95% CI 0.27 to 0.37) and 0.25 (95% CI 0.21 to 0.29) for control and premature CHD groups, respectively (p<0.05).
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ABCA1 p.Arg219Lys 12624133:226:54
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227 The presence of the K allele of the R219K polymorphism reduced the coronary event risk in the FH studied population (odds ratio 0.63, 95% CI 0.42 to 0.95).
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ABCA1 p.Arg219Lys 12624133:227:36
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228 The clinical and biochemical characteristics of carriers and non-carriers of the K allele for the R219K variant in the ABCA1 Table 1 Clinical and biochemical characteristics of the FH subjects included in this study Male p Female p Control PCHD Control PCHD No 66 144 92 72 Age (years) 64.3 (6.6) 51.1 (10.4) <0.001 70.5 (5.6) 57.8 (10.5) <0.001 BMI (kg/m2 ) 27.2 (3.0) 27.0 (3.5) NS 27.0 (4.3) 28.2 (4.6) NS TC (mmol/l) 10.7 (1.8) 10.8 (1.9) NS 11.1 (1.9) 11.2 (2.2) NS LDL-C (mmol/l) 8.7 (1.8) 8.9 (1.9) NS 9.0 (1.9) 9.2 (2.4) NS TG (mmol/l) 1.55 (0.71) 1.57 (0.73) NS 1.42 (0.66) 1.39 (0.60) NS HDL-C (mmol/l) 1.24 (0.36) 1.14 (0.30) NS 1.45 (0.36) 1.42 (0.44) NS Lp(a) (µmol/l) 1.50 (1.52) 2.11 (2.01) 0.049 2.11 (2.07) 1.96 (2.16) NS Xanthomas 46.0% 41.1% NS 28.9% 33.8% NS Arcus cornealis 77.8% 55.4% 0.002 63.3% 40.0% 0.003 Hypertension 27.9% 18.0% NS 36.1% 39.3% NS Smoking 61.7% 79.7% 0.008 2.4% 14.8% 0.006 DM-2 11.9% 2.3% 0.006 7.3% 5.2% NS Values are mean (SD) for quantitative variables, and percentages for qualitative variables.
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ABCA1 p.Arg219Lys 12624133:228:98
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231 Male subjects with the RR genotype had higher LDL-C levels than K allele carriers of the R219K polymorphism (p=0.04).
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ABCA1 p.Arg219Lys 12624133:231:89
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233 On the other hand, subjects not carrying the K allele of the R219K polymorphism had more xanthomas than subjects with the RK or KK genotypes (p=0.04).
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ABCA1 p.Arg219Lys 12624133:233:61
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235 The remaining variables, age, BMI, lipid and lipoprotein levels, and presence of arcus cornealis, did not show differences between carriers and non-carriers of the K allele of the R219K polymorphism.
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ABCA1 p.Arg219Lys 12624133:235:180
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236 To assess whether the presence of the K allele of the R219K variant has an effect on the age of onset of the first coronary event in the premature CHD group, we analysed the distribution of carriers and non-carriers of the K allele in subjects who suffered their first coronary event before 40 years old (first quartile) (PCHD<40 group, n=53), in subjects who suffered their first coronary event after 40 years old (PCHD>40 group, n=163), and in the control group.
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ABCA1 p.Arg219Lys 12624133:236:54
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238 A different distribution was observed, with fewer carriers of the K allele of the R219K polymorphism in the PCHD<40 group than in the PCHD>40 and fewer than in the control group.
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ABCA1 p.Arg219Lys 12624133:238:82
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244 The effect of the K allele of the R219K polymorphism on a premature event of CHD (before 40 years) was analysed in smokers and non-smokers separately.
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ABCA1 p.Arg219Lys 12624133:244:34
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247 In subjects with premature CHD before 40 years old, the odds ratio of carrying the K allele in smokers v non-smokers was 0.35 (95% Figure 1 Determination of the R219K genotype by PCR amplification and restriction analysis.
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ABCA1 p.Arg219Lys 12624133:247:161
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252 Table 2 Genotype and allele frequencies distribution for the R219K polymorphism in the control and premature coronary heart disease groups of FH subjects studied Genotype frequencies Allele frequencies RR RK KK p RR RK+KK p R K p Control 45.6% 44.9% 9.5% 0.037 45.6% 54.4% 0.029 0.68 0.32 0.036 PCHD 56.9% 36.1% 6.9% 56.9% 43.1% 0.75 0.25 PCHD, premature coronary heart disease.
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ABCA1 p.Arg219Lys 12624133:252:61
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254 These results would suggest that the protective effect of the K allele of the R219K variant on premature CHD risk is more pronounced in smokers.
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ABCA1 p.Arg219Lys 12624133:254:78
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257 Specifically, the R219K polymorphism has been shown to be associated with decreased TG levels and a decreased severity of CHD, these effects being compatible with a net increase in ABCA1 function and accelerated reverse cholesterol transport.21 This polymorphism could influence the phenotype of FH in such a way that subjects carrying the protective allele have a slower progression of atherosclerosis and a delayed onset of CHD.
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ABCA1 p.Arg219Lys 12624133:257:18
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258 Previous studies have reported a carrier frequency of the R219K polymorphism of 46% in the European population,21 which is similar (47.8%) to that found in our FH patients.
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ABCA1 p.Arg219Lys 12624133:258:58
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260 In the present work, we have found that the frequency of the K allele of the R219K variant is significantly higher in the group of FH subjects without premature CHD than in the group of FH subjects with premature CHD.
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ABCA1 p.Arg219Lys 12624133:260:77
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261 The presence of the K allele of the R219K polymorphism seems to be protective against onset of premature CHD in FH subjects.
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ABCA1 p.Arg219Lys 12624133:261:36
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262 One result of our study is that the K allele of the R219K variant seems to modify CHD risk without important modification of plasma HDL-C concentration.
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ABCA1 p.Arg219Lys 12624133:262:52
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266 It is possible that the R219K variant increases the activity of ABCA1 in a similar way, although the precise mechanism underlying the functional effect of this variant will require further analyses.
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ABCA1 p.Arg219Lys 12624133:266:24
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267 In this series of FH patients studied, we have observed a correlation between the presence of the K allele of the R219K variant and the age of onset of the first coronary event.
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ABCA1 p.Arg219Lys 12624133:267:114
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269 Comparison of the odds ratio of the control v the PCHD<40 group (OR=0.51) with the odds ratio of the control v the premature CHD total group (OR=0.63) suggests that younger subjects lacking the K allele of the R219K variant have a higher coronary risk.
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ABCA1 p.Arg219Lys 12624133:269:210
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270 This observation confirms the protective effect of the K allele, as subjects lacking the K allele of the R219K variant develop CHD at an earlier age than subjects carrying this allele.
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ABCA1 p.Arg219Lys 12624133:270:105
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271 Another observation of our study is that the R219K variant appears to be more protective for smokers and ex-smokers than non-smokers in the PCHD<40 group.
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ABCA1 p.Arg219Lys 12624133:271:45
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274 Similarly, in our series of FH patients, smoking increases the risk of CHD in all subjects, but particularly in those subjects lacking the K allele of the R219K polymorphism in ABCA1.
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ABCA1 p.Arg219Lys 12624133:274:155
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275 Smoking increases the rate of oxidation of lipoprotein particles, and it might be possible that this oxidative stress would be alleviated in part through the ABCA1 pathway, since ABCA1 has been reported to mediate the cellular secretion of α tocopherol, the active form of vitamin E with antioxidant properties.37 Thus, it might be possible that Table 3 Clinical and biochemical characteristics of non-carriers and carriers of the K allele of the R219K polymorphism in FH subjects studied Male Female All RR RK+KK p RR RK+KK p RR RK+KK p No 120 90 75 89 195 179 Age (years) 55.4 (10.8) 55.1 (11.7) NS 63.6 (10.3) 66.1 (10.2) NS 58.5 (11.3) 60.6 (12.3) NS BMI (kg/m2 ) 27.2 (3.4) 26.9 (3.2) NS 27.1 (4.4) 27.9 (4.6) NS 27.2 (3.8) 27.4 (3.9) NS TC (mmol/l) 10.9 (2.0) 10.5 (1.7) NS 11.2 (2.3) 11.1 (1.9) NS 11.1 (2.1) 10.8 (1.8) NS LDL-C (mmol/l) 9.1 (2.0) 8.6 (1.8) 0.04 9.1 (2.4) 9.1 (1.9) NS 9.1 (2.1) 8.8 (1.9) NS TG (mmol/l) 1.53 (0.65) 1.60 (0.81) NS 1.46 (0.64) 1.38 (0.63) NS 1.49 (0.64) 1.49 (0.73) NS HDL-C (mmol/l) 1.17 (0.32) 1.19 (0.33) NS 1.42 (0.38) 1.45 (0.41) NS 1.27 (0.36) 1.32 (0.40) NS Lp(a) (µmol/l) 1.93 (1.70) 1.96 (2.12) NS 2.00 (2.17) 2.07 (2.05) NS 1.96 (1.90) 2.00 (2.08) NS Xanthomas 47.4% 36.4% NS 34.2% 28.4% NS 42.3% 32.4% 0.04 Arcus cornealis 57.9% 68.2% NS 52.8% 53.4% NS 55.9% 60.8% NS Values are mean (SD) for quantitative variables, and percentages for qualitative variables.
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ABCA1 p.Arg219Lys 12624133:275:452
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277 Figure 2 Percentage of non-carriers and carriers of the K allele of the R219K polymorphism in each of the three groups of FH subjects analysed: free of premature coronary heart disease (controls), premature coronary heart disease with first coronary event after 40 years old (PCHD>40), and premature coronary heart disease with first coronary event before 40 years old (PCHD<40); p indicates the difference between the control and PCHD<40 groups.
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ABCA1 p.Arg219Lys 12624133:277:72
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278 subjects carrying the K allele of the R219K variant would be more protected against lipoprotein oxidation and subsequent risk of atherosclerosis.
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ABCA1 p.Arg219Lys 12624133:278:38
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280 In this work we show that the R219K variant of ABCA1 influences premature CHD frequency in subjects with heterozygous familial hypercholesterolaemia.
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ABCA1 p.Arg219Lys 12624133:280:30
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281 FH subjects are a very high cardiovascular risk owing to their high LDL-C levels as a consequence of a mutation in the LDLR gene, but other genetic and/or environmental factors modify the disease expression18 and it is possible that one of them could be the variant R219K in ABCA1.
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ABCA1 p.Arg219Lys 12624133:281:266
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283 Although the ABCA1 locus, and specifically the polymorphism R219K, influences the early onset of CHD in FH, other different loci are also implicated with small and/or large contributions, the disease expression being the result of the interaction of these loci.16 Further studies to that effect will help to identify FH subjects at high risk of premature CHD, which will be helpful for better prevention and management of cardiovascular disease in familial hypercholesterolaemia.
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ABCA1 p.Arg219Lys 12624133:283:60
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PMID: 12573359 [PubMed] Owen JS et al: "ATP-binding cassette A1 protein and HDL homeostasis."
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180 A single nucleotide polymorphism (SNP) in ABCA1, the Arg219Lys variant, which has a carrier frequency of over 40%, slows atherogenesis [85].
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ABCA1 p.Arg219Lys 12573359:180:53
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PMID: 11940086 [PubMed] Zwarts KY et al: "ABCA1 regulatory variants influence coronary artery disease independent of effects on plasma lipid levels."
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22 Interestingly, the R219K cSNP is associated with decreased TG, increased HDL-C and a decreased severity of CAD, which is compatible with a net increase in transporter function (16).
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ABCA1 p.Arg219Lys 11940086:22:19
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PMID: 11352567 [PubMed] Qiu Y et al: "Human and mouse ABCA1 comparative sequencing and transgenesis studies revealing novel regulatory sequences."
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119 These included Arg219Lys, Tyr793Cys, Asp831Asn, Asp1005Lys, Thr1555Ile, Arg1974Lys, and Pro2168Leu.
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ABCA1 p.Arg219Lys 11352567:119:15
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PMID: 11238261 [PubMed] Clee SM et al: "Common genetic variation in ABCA1 is associated with altered lipoprotein levels and a modified risk for coronary artery disease."
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11 The R219K variant has a carrier frequency of 46% in Europeans.
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ABCA1 p.Arg219Lys 11238261:11:4
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13 Atherosclerosis progresses more slowly in carriers of R219K than in noncarriers.
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ABCA1 p.Arg219Lys 11238261:13:54
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29 We report here that a common ABCA1 cSNP, R219K, is associated with decreased TG, increased HDL-C and, importantly, a decreased progression of atherosclerosis and a reduced risk of coronary events, suggesting that common genetic variants in ABCA1 may influence these clinical outcomes in the general population.
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ABCA1 p.Arg219Lys 11238261:29:41
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32 We studied the effects of these cSNPs on the baseline lipid parameters of the cohort of 804 Dutch men with proven CAD who participated in the Regression Growth Evaluation Statin Study (REGRESS); these subjects were described previously.11 For replication studies with the R219K variant, we genotyped 3 smaller cohorts.
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ABCA1 p.Arg219Lys 11238261:32:272
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48 Methods for Restriction Fragment Length Polymorphism Screening of ABCA1 cSNPs Variant pmol of Each Oligo Forward Oligo (5Ј33Ј)* Reverse Oligo (5Ј33Ј)* Annealing Temperature, °C Enzyme Product, bp Wild-type Allele Variant Allele % Agarose Gel for Resolution G1051A 20 GTATTTTTGCAAGGCTACCAGTTACATTTGACAA 60 EcoN I 177 1.5 (R219K) GATTGGCTTCAGGATGTCCATGTTGGAA 107, 70 T1591C 27.5 GCTGCTGTGATGGGGTATCT 57 Hph I 117, 103, 48, 33 1.5 (V399A) ACCTCACTCACACCTGGGAA 220, 48, 33 G2706A 27.5 CAAGTGAGTGCTTGGGATTG 57 BsaA I 98, 252 2 (V771M) TGCTTTTATTCAGGGACTCCA 350 A2715C 27.5 GTGATCCCAGCGTGGTGTTTGTCTT 55 Hph I 56, 69, 95 2 (T774P) GAAAGGCCAGAGGTACTCACAGCGAAGATCTTGAGGG 56, 161 G2723C 12 TCGTTTTATTCAGGGACTCCA 55 Bgl II 269, 80 2 (K776N) CAAGTGAGTGCTTGGGATTG 349 G2868A 27.5 CCCATGCACTGCAGAGATTC 57 Bsa I 149, 237 2 (V825I) GCAAATTCAAATTTCTCCAGG 386 A3044G 27.5 GAGAAGAGCCACCCTGGTTCCAACCAGAAGAGGAT 55 EcoR V 94, 35 2.5 (I883M) AAGGCAGGAGACATCGCTT 129 G3911C 27.5 GAGCAGTTCTGATGCTGGCCTGGGCAGCGACCACGA 55 BssS I 104, 37 2 (E1172D) TCTGCACCTCTCCTCCTCTG 141 G5155A 27.5 CAGCTTGGGAAGATTTATGACAGGACTGGACACGA 55 BssS I 114, 31 2 (R1587K) ATGCCCCTGCCAACTTAC 145 C5587G 20 GTGCAATTACGTTGTCCCTGCCACACT 60 Mnl I 82, 35 3 (S1731C) CCATACAGCAAAAGTAGAAGGGCTAGCACA 117 *Bold indicates mismatch in oligo to create restriction site.
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ABCA1 p.Arg219Lys 11238261:48:350
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61 The population-attributable risk for R219K is calculated from the sum of each genotype frequency multiplied by its risk (relative to KK).
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ABCA1 p.Arg219Lys 11238261:61:37
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68 The R219K Polymorphism Is Associated With a Decreased Severity of CAD The G1051A polymorphism results in the substitution of a lysine for arginine at amino acid 219 of the ABCA1 protein (R219K; Table 2).
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ABCA1 p.Arg219Lys 11238261:68:4
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ABCA1 p.Arg219Lys 11238261:68:127
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71 The K allele of the R219K polymorphism was associated with a decreased severity of CAD (Table 3), as indicated by an increased MSD and MOD.
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ABCA1 p.Arg219Lys 11238261:71:20
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78 For the R219K variant, the population-attributable risk is 5.3%, suggesting that the frequency of CAD events would be 5.3% lower if all individuals carried the KK genotype.
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ABCA1 p.Arg219Lys 11238261:78:8
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79 If the K allele of the R219K variant is protective against CAD, we might expect its frequency to be reduced in this cohort, which was selected for CAD.
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ABCA1 p.Arg219Lys 11238261:79:23
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81 Association of the R219K Polymorphism With Plasma Lipid Levels TG were significantly lower in the carriers of the K allele (Table 4).
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ABCA1 p.Arg219Lys 11238261:81:19
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85 Frequencies of ABCA1 cSNPs Nucleotide Change Amino Acid Change Exon REGRESS Carrier Frequency Allele Frequency n* Nonsynonymous G1051A R219K 7 46.3 0.254 1588 T1591C V399A 11 1.6 0.008 1098 G2706A V771M 16 5.8 0.029 1270 A2715C T774P 16 0.6 0.003 1250 G2723C K776N 16 0.5 0.003 1106 G2868A V825I 17 15.7 0.081 1364 A3044G I883M 18 23.8 0.136 840 G3911C E1172D 24 5.3 0.026 1288 G5155A R1587K 35 44.3 0.259 1566 C5587G† S1731C 38 0 0 558 Synonymous From sequencing G869A None 6 62.5 0.38 32 C1331T None 9 31.3 0.19 32 G1343A None 9 25 0.133 32 T3554G None 22 12.5 0.059 32 G4676A None 30 6.3 0.06 32 C6842T None 49 6.3 0.033 32 *Number of alleles screened.
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ABCA1 p.Arg219Lys 11238261:85:135
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92 In younger individuals, cholesterol efflux and HDL-C were increased in KK compared with RR individuals, which suggests that the R219K variant may be especially protective against premature CAD.
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ABCA1 p.Arg219Lys 11238261:92:128
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93 Age Subgroup Analysis Indicates CAD Progresses More Slowly in R219K Carriers In the noncarriers, MOD and MSD decreased significantly with age, reflecting increased atherosclerosis in the older individuals (1.77Ϯ0.34 versus 1.69Ϯ0.35 mm, PϽ0.0001, and 2.75Ϯ0.36 versus 2.65Ϯ0.38 mm, Pϭ0.006 for MOD and MSD, respectively, in younger versus older noncarriers).
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ABCA1 p.Arg219Lys 11238261:93:62
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94 In contrast, in carriers of the R219K variant, these measurements do not significantly change with age (1.83Ϯ0.36 versus 1.78Ϯ0.34 mm, Pϭ0.30, and 2.79Ϯ0.37 versus 2.75Ϯ0.37 mm, Pϭ0.18, for MOD and MSD, respectively, in younger versus older carriers).
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ABCA1 p.Arg219Lys 11238261:94:32
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95 Thus, vascular disease progresses more slowly with age in carriers of R219K compared with noncarriers (Figure I; can be found Online at www.circulationaha.org).
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ABCA1 p.Arg219Lys 11238261:95:70
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96 Replication Cohorts Show the R219K Variant Is Associated With Decreased TG and Increased HDL-C To confirm and replicate the relationship observed between the R219K variant and plasma lipid levels, we genotyped this variant in 3 small cohorts of European subjects.
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ABCA1 p.Arg219Lys 11238261:96:29
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ABCA1 p.Arg219Lys 11238261:96:158
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103 CAD in R219K Carriers Compared With Controls RR RK KK Carriers (RKϩKK) P RK vs RR KK vs RR RKϩKK vs RR n 424 330 36 366 MSD, mm 2.70Ϯ0.37 2.77Ϯ0.37 2.78Ϯ0.40 2.77Ϯ0.37 0.01 0.22 0.005 MOD, mm 1.73Ϯ0.35 1.81Ϯ0.35 1.85Ϯ0.35 1.81Ϯ0.35 0.002 0.05 0.001 MI before trial, % (n) 48.3 (205) 47.1 (155) 33.3 (12) 45.8 (167) 0.71 0.12 0.48 Events during trial, % (n) 17 (71) 13 (41) 11 (4) 12 (45) 0.10 0.49 0.09 Total events, % (n) 59 (248) 52 (170) 39 (14) 50 (184) 0.06* 0.03† 0.02‡ Values are meanϮSD or % (n).
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ABCA1 p.Arg219Lys 11238261:103:7
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120 Event-free survival curves for R219K carriers (RKϩKK; thin line) and noncarriers (RR; thick line).
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ABCA1 p.Arg219Lys 11238261:120:31
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122 Carriers of R219K had a 29% increased event-free survival compared with noncarriers.
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ABCA1 p.Arg219Lys 11238261:122:12
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ABCA1 p.Arg219Lys 11238261:122:52
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124 Baseline Demographics and Lipid Levels in the REGRESS Cohort by R219K Genotype RR RK KK RKϩKK P RK vs RR KK vs RR RKϩKK vs RR n 424 330 36 366 Age, y 57Ϯ8 55Ϯ8 57Ϯ7 55Ϯ8 0.0007 1 0.03 BMI, kg/m2 25.8Ϯ2.6 26.3Ϯ2.7 25.5Ϯ2.3 26.2Ϯ2.7 0.01 0.50 0.09 Total cholesterol, mmol/L 6.02Ϯ0.86 6.07Ϯ0.89 5.89Ϯ0.85 6.06Ϯ0.89 0.44 0.38 0.60 HDL-C, mmol/L 0.92Ϯ0.22 0.93Ϯ0.23 0.92Ϯ0.20 0.93Ϯ0.23 0.54 1 0.81 LDL-C, mmol/L 4.27Ϯ0.75 4.35Ϯ0.83 4.33Ϯ0.82 4.35Ϯ0.83 0.17 0.65 0.19 TG, mmol/L 1.84Ϯ0.77 1.78Ϯ0.78 1.42Ϯ0.49 1.74Ϯ0.76 0.29 0.001 0.08 Values are meanϮSD.
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ABCA1 p.Arg219Lys 11238261:124:64
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126 Changes in HDL-C and efflux with age by R219K genotype.
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ABCA1 p.Arg219Lys 11238261:126:40
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127 A depicts the relationship between HDL-C and age in R219K carriers (RKϩKK; dashed line) compared with noncarriers (RR; solid line).
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ABCA1 p.Arg219Lys 11238261:127:52
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136 However, all but 2 carriers of V771M were also carriers of R219K.
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ABCA1 p.Arg219Lys 11238261:136:59
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138 No carriers of S1731C were detected in the REGRESS population.
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ABCA1 p.Arg219Lys 11238261:138:26
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140 The presence of this variant in individuals heterozygous for the R2144X ABCA1 mutation was associated with further significantly decreased HDL-C compared with R2144X carriers without this polymorphism (0.16Ϯ0.04 mmol/L, nϭ2, versus 0.64Ϯ0.14 mmol/L, nϭ10; Pϭ0.0009).
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ABCA1 p.Arg219Lys 11238261:140:319
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141 In unaffected family members, although carriers of S1731C (n&#x3ed;6) had slightly lower HDL-C compared with noncarriers (nϭ14, 1.03Ϯ0.22 versus 1.09Ϯ0.23 mmol/L), the difference was not statistically significant.
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ABCA1 p.Arg219Lys 11238261:141:62
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143 The Phenotypic Effects of R219K Are Independent of Other cSNPs There is linkage disequilibrium between cSNPs in the ABCA1 gene.
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ABCA1 p.Arg219Lys 11238261:143:26
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ABCA1 p.Arg219Lys 11238261:143:41
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144 Two rare cSNPs (V771M and K776N) are most commonly found in individuals carrying the R219K K allele.
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ABCA1 p.Arg219Lys 11238261:144:25
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ABCA1 p.Arg219Lys 11238261:144:85
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145 If all V771M and K776N carriers are excluded, the results are unaltered, with increased MOD (1.80Ϯ0.35 versus 1.73Ϯ0.35 mm, Pϭ0.006) and MSD (2.76Ϯ0.36 versus 2.70Ϯ0.37 mm, Pϭ0.02) and lower mean TG levels (1.71Ϯ0.75 versus 1.84Ϯ0.77 mmol/L, Pϭ0.02) in carriers of R219K (nϭ329) compared with noncarriers (nϭ422).
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ABCA1 p.Arg219Lys 11238261:145:319
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146 The I883M and R1587K cSNPs are also often seen in carriers of R219K.
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ABCA1 p.Arg219Lys 11238261:146:62
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147 We identified R219K carriers who do not also carry either the I883M or R1587K genotype (nϭ62) and compared them with the group of individuals who do not carry any of the 3 variants (nϭ116).
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ABCA1 p.Arg219Lys 11238261:147:14
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148 MSD was still significantly increased in R219K carriers compared with noncarriers (2.81Ϯ0.37 versus 2.69Ϯ0.36 mm, Pϭ0.04); MOD was increased in carriers (1.78Ϯ0.39 versus 1.73Ϯ0.38 mm); and TG remained significantly decreased in carriers (1.67Ϯ0.76 versus 1.97Ϯ0.74 mmol/L, Pϭ0.02).
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ABCA1 p.Arg219Lys 11238261:148:41
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149 Thus, the effects of the R219K variant described herein are not due to other cSNPs that are found in linkage disequilibrium with it.
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ABCA1 p.Arg219Lys 11238261:149:25
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161 ABCA cSNPs in REGRESS MOD, mm MSD, mm HDL-C, mmol/L TG, mmol/L Carrier Noncarrier P Carrier Noncarrier P Carrier Noncarrier P Carrier Noncarrier P V825I 1.74Ϯ0.37 (107) 1.77Ϯ0.35 (575) 0.39 2.70Ϯ0.38 2.75Ϯ0.38 0.21 0.91Ϯ0.23 0.93Ϯ0.22 0.42 1.86Ϯ0.84 1.80Ϯ0.76 0.49 I883M 1.74Ϯ0.38 (100) 1.75Ϯ0.36 (320) 0.71 2.69Ϯ0.38 2.73Ϯ0.36 0.41 0.91Ϯ0.22 0.91Ϯ0.21 0.97 1.75Ϯ0.77 1.82Ϯ0.75 0.42 R1587K 1.77Ϯ0.34 (346) 1.76Ϯ0.37 (433) 0.75 2.73Ϯ0.39 2.74Ϯ0.36 0.64 0.90Ϯ0.22 0.94Ϯ0.23 0.03 1.79Ϯ0.76 1.81Ϯ0.78 0.77 V399A 1.92Ϯ0.32 (9) 1.73Ϯ0.35 (540) 0.13 2.73Ϯ0.40 2.71Ϯ0.37 0.89 1.03Ϯ0.28 0.92Ϯ0.23 0.15 1.71Ϯ0.63 1.82Ϯ0.78 0.68 V771M 1.89Ϯ0.38 (37) 1.76Ϯ0.35 (598) 0.045 2.83Ϯ0.49 2.73Ϯ0.37 0.13 0.91Ϯ0.20 0.92Ϯ0.22 0.58 1.98Ϯ0.79 1.78Ϯ0.76 0.11 T774P 1.63Ϯ0.31 (4) 1.76Ϯ0.36 (621) 0.47 2.85Ϯ0.34 2.73Ϯ0.37 0.52 0.85Ϯ0.07 0.93Ϯ0.22 0.50 1.90Ϯ1.04 1.82Ϯ0.77 0.84 K776N 1.92Ϯ0.33 (3) 1.78Ϯ0.34 (546) 0.48 2.95Ϯ0.48 2.76Ϯ0.37 0.36 0.94Ϯ0.28 0.93Ϯ0.22 0.93 2.25Ϯ0.94 1.76Ϯ0.76 0.26 E117SD 1.80Ϯ0.39 (34) 1.77Ϯ0.36 (610) 0.67 2.78Ϯ0.35 2.74Ϯ0.37 0.42 0.93Ϯ0.23 0.94Ϯ0.23 0.89 1.80Ϯ0.90 1.77Ϯ0.76 0.80 Values are meanϮSD (n).
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ABCA1 p.Arg219Lys 11238261:161:78
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164 The R219K variant, with a carrier frequency of 46% in European populations, is associated with a decreased severity of CAD, which manifests as decreased focal and diffuse atherosclerosis, with less progression and decreased coronary events.
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ABCA1 p.Arg219Lys 11238261:164:4
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166 The phenotypic effects of the remaining cSNPs are less striking than those of R219K.
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ABCA1 p.Arg219Lys 11238261:166:73
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168 Both the finding of decreased TG and of increased HDL-C in younger carriers of the R219K K allele is consistent with the decreased CAD observed in carriers of the variant.15,16 TG levels showed similar trends in our replication groups, and increased HDL-C levels in R219K carriers were observed in our independent populations.
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ABCA1 p.Arg219Lys 11238261:168:61
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ABCA1 p.Arg219Lys 11238261:168:83
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ABCA1 p.Arg219Lys 11238261:168:266
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171 The lack of obvious differences in HDL-C in carriers of different cSNPs (R219K, V771M, and I883M), together with clear differences in CAD, suggests that stimulating the RCT pathway can increase the net flux of cholesterol toward the liver without altering steady-state plasma HDL-C levels.
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ABCA1 p.Arg219Lys 11238261:171:73
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173 The mechanism underlying the decreased TG in carriers of the R219K variant is unknown.
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ABCA1 p.Arg219Lys 11238261:173:61
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179 In heterozygotes, the phenotype is more pronounced in older individuals.9 This suggests that ABCA1 activity may normally increase with age but that this is blunted in R219K heterozygotes.
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ABCA1 p.Arg219Lys 11238261:179:167
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180 Age-related increases in the expression and activity of P-glycoprotein, another ATP-binding cassette transporter, have been described.22,23 In the present study, we show that the R219K polymorphism was also associated with an altered relationship between age and HDL-C.
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ABCA1 p.Arg219Lys 11238261:180:179
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192 We showed that common ABCA1 cSNPs are associated with altered plasma lipid levels and severity of atherosclerosis. Specifically, the frequent R219K variant is associated with a decreased severity of atherosclerosis, a decreased risk of coronary events, decreased TG, and increased HDL-C, which is consistent with a gain of function in ABCA1.
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ABCA1 p.Arg219Lys 11238261:192:142
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193 These effects were independent of any other cSNPs found in association with R219K and were seen both in different measures of CAD and in multiple cohorts.
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ABCA1 p.Arg219Lys 11238261:193:76
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5 The R219K variant has a carrier frequency of 46% in Europeans.
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ABCA1 p.Arg219Lys 11238261:5:4
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7 Atherosclerosis progresses more slowly in carriers of R219K than in noncarriers.
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ABCA1 p.Arg219Lys 11238261:7:54
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24 We report here that a common ABCA1 cSNP, R219K, is associated with decreased TG, increased HDL-C and, importantly, a decreased progression of atherosclerosis and a reduced risk of coronary events, suggesting that common genetic variants in ABCA1 may influence these clinical outcomes in the general population.
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ABCA1 p.Arg219Lys 11238261:24:41
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27 We studied the effects of these cSNPs on the baseline lipid parameters of the cohort of 804 Dutch men with proven CAD who participated in the Regression Growth Evaluation Statin Study (REGRESS); these subjects were described previously.11 For replication studies with the R219K variant, we genotyped 3 smaller cohorts.
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ABCA1 p.Arg219Lys 11238261:27:272
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43 Methods for Restriction Fragment Length Polymorphism Screening of ABCA1 cSNPs Variant pmol of Each Oligo Forward Oligo (5b18;33b18;)* Reverse Oligo (5b18;33b18;)* Annealing Temperature, &#b0;C Enzyme Product, bp Wild-type Allele Variant Allele % Agarose Gel for Resolution G1051A 20 GTATTTTTGCAAGGCTACCAGTTACATTTGACAA 60 EcoN I 177 1.5 (R219K) GATTGGCTTCAGGATGTCCATGTTGGAA 107, 70 T1591C 27.5 GCTGCTGTGATGGGGTATCT 57 Hph I 117, 103, 48, 33 1.5 (V399A) ACCTCACTCACACCTGGGAA 220, 48, 33 G2706A 27.5 CAAGTGAGTGCTTGGGATTG 57 BsaA I 98, 252 2 (V771M) TGCTTTTATTCAGGGACTCCA 350 A2715C 27.5 GTGATCCCAGCGTGGTGTTTGTCTT 55 Hph I 56, 69, 95 2 (T774P) GAAAGGCCAGAGGTACTCACAGCGAAGATCTTGAGGG 56, 161 G2723C 12 TCGTTTTATTCAGGGACTCCA 55 Bgl II 269, 80 2 (K776N) CAAGTGAGTGCTTGGGATTG 349 G2868A 27.5 CCCATGCACTGCAGAGATTC 57 Bsa I 149, 237 2 (V825I) GCAAATTCAAATTTCTCCAGG 386 A3044G 27.5 GAGAAGAGCCACCCTGGTTCCAACCAGAAGAGGAT 55 EcoR V 94, 35 2.5 (I883M) AAGGCAGGAGACATCGCTT 129 G3911C 27.5 GAGCAGTTCTGATGCTGGCCTGGGCAGCGACCACGA 55 BssS I 104, 37 2 (E1172D) TCTGCACCTCTCCTCCTCTG 141 G5155A 27.5 CAGCTTGGGAAGATTTATGACAGGACTGGACACGA 55 BssS I 114, 31 2 (R1587K) ATGCCCCTGCCAACTTAC 145 C5587G 20 GTGCAATTACGTTGTCCCTGCCACACT 60 Mnl I 82, 35 3 (S1731C) CCATACAGCAAAAGTAGAAGGGCTAGCACA 117 *Bold indicates mismatch in oligo to create restriction site.
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ABCA1 p.Arg219Lys 11238261:43:349
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56 The population-attributable risk for R219K is calculated from the sum of each genotype frequency multiplied by its risk (relative to KK).
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ABCA1 p.Arg219Lys 11238261:56:37
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63 The R219K Polymorphism Is Associated With a Decreased Severity of CAD The G1051A polymorphism results in the substitution of a lysine for arginine at amino acid 219 of the ABCA1 protein (R219K; Table 2).
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ABCA1 p.Arg219Lys 11238261:63:4
status: NEW
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ABCA1 p.Arg219Lys 11238261:63:127
status: NEW
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ABCA1 p.Arg219Lys 11238261:63:187
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66 The K allele of the R219K polymorphism was associated with a decreased severity of CAD (Table 3), as indicated by an increased MSD and MOD.
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ABCA1 p.Arg219Lys 11238261:66:20
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73 For the R219K variant, the population-attributable risk is 5.3%, suggesting that the frequency of CAD events would be 5.3% lower if all individuals carried the KK genotype.
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ABCA1 p.Arg219Lys 11238261:73:8
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74 If the K allele of the R219K variant is protective against CAD, we might expect its frequency to be reduced in this cohort, which was selected for CAD.
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ABCA1 p.Arg219Lys 11238261:74:23
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76 Association of the R219K Polymorphism With Plasma Lipid Levels TG were significantly lower in the carriers of the K allele (Table 4).
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ABCA1 p.Arg219Lys 11238261:76:19
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80 Frequencies of ABCA1 cSNPs Nucleotide Change Amino Acid Change Exon REGRESS Carrier Frequency Allele Frequency n* Nonsynonymous G1051A R219K 7 46.3 0.254 1588 T1591C V399A 11 1.6 0.008 1098 G2706A V771M 16 5.8 0.029 1270 A2715C T774P 16 0.6 0.003 1250 G2723C K776N 16 0.5 0.003 1106 G2868A V825I 17 15.7 0.081 1364 A3044G I883M 18 23.8 0.136 840 G3911C E1172D 24 5.3 0.026 1288 G5155A R1587K 35 44.3 0.259 1566 C5587Gߤ S1731C 38 0 0 558 Synonymous From sequencing G869A None 6 62.5 0.38 32 C1331T None 9 31.3 0.19 32 G1343A None 9 25 0.133 32 T3554G None 22 12.5 0.059 32 G4676A None 30 6.3 0.06 32 C6842T None 49 6.3 0.033 32 *Number of alleles screened.
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ABCA1 p.Arg219Lys 11238261:80:135
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87 In younger individuals, cholesterol efflux and HDL-C were increased in KK compared with RR individuals, which suggests that the R219K variant may be especially protective against premature CAD.
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ABCA1 p.Arg219Lys 11238261:87:128
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88 Age Subgroup Analysis Indicates CAD Progresses More Slowly in R219K Carriers In the noncarriers, MOD and MSD decreased significantly with age, reflecting increased atherosclerosis in the older individuals (1.77afe;0.34 versus 1.69afe;0.35 mm, Pb0d;0.0001, and 2.75afe;0.36 versus 2.65afe;0.38 mm, Pafd;0.006 for MOD and MSD, respectively, in younger versus older noncarriers).
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ABCA1 p.Arg219Lys 11238261:88:62
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89 In contrast, in carriers of the R219K variant, these measurements do not significantly change with age (1.83afe;0.36 versus 1.78afe;0.34 mm, Pafd;0.30, and 2.79afe;0.37 versus 2.75afe;0.37 mm, Pafd;0.18, for MOD and MSD, respectively, in younger versus older carriers).
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ABCA1 p.Arg219Lys 11238261:89:32
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90 Thus, vascular disease progresses more slowly with age in carriers of R219K compared with noncarriers (Figure I; can be found Online at www.circulationaha.org).
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ABCA1 p.Arg219Lys 11238261:90:70
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91 Replication Cohorts Show the R219K Variant Is Associated With Decreased TG and Increased HDL-C To confirm and replicate the relationship observed between the R219K variant and plasma lipid levels, we genotyped this variant in 3 small cohorts of European subjects.
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ABCA1 p.Arg219Lys 11238261:91:29
status: NEW
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ABCA1 p.Arg219Lys 11238261:91:158
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98 CAD in R219K Carriers Compared With Controls RR RK KK Carriers (RKaf9;KK) P RK vs RR KK vs RR RKaf9;KK vs RR n 424 330 36 366 MSD, mm 2.70afe;0.37 2.77afe;0.37 2.78afe;0.40 2.77afe;0.37 0.01 0.22 0.005 MOD, mm 1.73afe;0.35 1.81afe;0.35 1.85afe;0.35 1.81afe;0.35 0.002 0.05 0.001 MI before trial, % (n) 48.3 (205) 47.1 (155) 33.3 (12) 45.8 (167) 0.71 0.12 0.48 Events during trial, % (n) 17 (71) 13 (41) 11 (4) 12 (45) 0.10 0.49 0.09 Total events, % (n) 59 (248) 52 (170) 39 (14) 50 (184) 0.06* 0.03ߤ 0.02ߥ Values are meanafe;SD or % (n).
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ABCA1 p.Arg219Lys 11238261:98:7
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115 Event-free survival curves for R219K carriers (RKaf9;KK; thin line) and noncarriers (RR; thick line).
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ABCA1 p.Arg219Lys 11238261:115:31
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117 Carriers of R219K had a 29% increased event-free survival compared with noncarriers.
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ABCA1 p.Arg219Lys 11238261:117:12
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119 Baseline Demographics and Lipid Levels in the REGRESS Cohort by R219K Genotype RR RK KK RKaf9;KK P RK vs RR KK vs RR RKaf9;KK vs RR n 424 330 36 366 Age, y 57afe;8 55afe;8 57afe;7 55afe;8 0.0007 1 0.03 BMI, kg/m2 25.8afe;2.6 26.3afe;2.7 25.5afe;2.3 26.2afe;2.7 0.01 0.50 0.09 Total cholesterol, mmol/L 6.02afe;0.86 6.07afe;0.89 5.89afe;0.85 6.06afe;0.89 0.44 0.38 0.60 HDL-C, mmol/L 0.92afe;0.22 0.93afe;0.23 0.92afe;0.20 0.93afe;0.23 0.54 1 0.81 LDL-C, mmol/L 4.27afe;0.75 4.35afe;0.83 4.33afe;0.82 4.35afe;0.83 0.17 0.65 0.19 TG, mmol/L 1.84afe;0.77 1.78afe;0.78 1.42afe;0.49 1.74afe;0.76 0.29 0.001 0.08 Values are meanafe;SD.
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ABCA1 p.Arg219Lys 11238261:119:64
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121 Changes in HDL-C and efflux with age by R219K genotype.
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ABCA1 p.Arg219Lys 11238261:121:40
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131 However, all but 2 carriers of V771M were also carriers of R219K.
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ABCA1 p.Arg219Lys 11238261:131:59
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139 Two rare cSNPs (V771M and K776N) are most commonly found in individuals carrying the R219K K allele.
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ABCA1 p.Arg219Lys 11238261:139:85
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142 We identified R219K carriers who do not also carry either the I883M or R1587K genotype (nafd;62) and compared them with the group of individuals who do not carry any of the 3 variants (nafd;116).
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ABCA1 p.Arg219Lys 11238261:142:14
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159 The R219K variant, with a carrier frequency of 46% in European populations, is associated with a decreased severity of CAD, which manifests as decreased focal and diffuse atherosclerosis, with less progression and decreased coronary events.
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ABCA1 p.Arg219Lys 11238261:159:4
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163 Both the finding of decreased TG and of increased HDL-C in younger carriers of the R219K K allele is consistent with the decreased CAD observed in carriers of the variant.15,16 TG levels showed similar trends in our replication groups, and increased HDL-C levels in R219K carriers were observed in our independent populations.
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ABCA1 p.Arg219Lys 11238261:163:83
status: NEW
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ABCA1 p.Arg219Lys 11238261:163:266
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174 In heterozygotes, the phenotype is more pronounced in older individuals.9 This suggests that ABCA1 activity may normally increase with age but that this is blunted in R219K heterozygotes.
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ABCA1 p.Arg219Lys 11238261:174:167
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175 Age-related increases in the expression and activity of P-glycoprotein, another ATP-binding cassette transporter, have been described.22,23 In the present study, we show that the R219K polymorphism was also associated with an altered relationship between age and HDL-C.
X
ABCA1 p.Arg219Lys 11238261:175:179
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187 We showed that common ABCA1 cSNPs are associated with altered plasma lipid levels and severity of atherosclerosis. Specifically, the frequent R219K variant is associated with a decreased severity of atherosclerosis, a decreased risk of coronary events, decreased TG, and increased HDL-C, which is consistent with a gain of function in ABCA1.
X
ABCA1 p.Arg219Lys 11238261:187:142
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188 These effects were independent of any other cSNPs found in association with R219K and were seen both in different measures of CAD and in multiple cohorts.
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ABCA1 p.Arg219Lys 11238261:188:76
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PMID: 11558901 [PubMed] Iida A et al: "High-density single-nucleotide polymorphism (SNP) map of the 150-kb region corresponding to the human ATP-binding cassette transporter A1 (ABCA1) gene."
No. Sentence Comment
15 Therefore, information concerning naturally occurring genetic variants in human transporter genes such as ABCA1 Fig.1.Single-nucleotidepolymorphism(SNP)mapspanningthe150-kbregioncontainingtheABCA1gene.Exonsarerepresentedbyopenrectanglesandintronsbyhorizontallines.SNPs areindicatedabovethelinesaccordingtonumber(correspondingtothenumbersinthefar-leftcolumnofTable1);thepositionsofeightinsertion-deletionpolymorphismsareindicatedbelow thelines(seeTable2).Microsatellitesequencesarealsoshown Table 1. Characterization of 162 single-nucleotide polymorphisms (SNPs) within the ABCA1 locus Repetitive Identity Number Location Exon SNP (5Ј to 3Ј) Substituion sequence to dbSNP Reference 1 -278 G Ͼ C 5Ј flanking region gggcccgggcgggggaaggg G/C acgcagaccgcggaccctaa rs1800976 2 -99 G Ͼ C 5Ј flanking region acataaacagaggccgggaa G/C ggggcggggaggagggagag 3 159 G Ͼ T intron 1 gcggtgttaaatggggagac G/T atgtcctagtacgagctctg 4 506 G Ͼ C intron 1 gaattggctatatgctcccc G/C ggactggagcggcacagtcc 5 5897 T Ͼ G intron 1 gtacaaaaccctttagcttt T/G gcaaacctcctttaagaccc 6 5929 C Ͼ T intron 1 ttaagacccgatttaaatgc C/T tccctcctcatgaagctctt 7 5962 T Ͼ C intron 1 aagctcttctggatccactc T/C ttcccatcactaagttgaaa 8 5985 A Ͼ C intron 1 cccatcactaagttgaaagt A/C agatccccttctctttactt 9 11416 G Ͼ A intron 1 ttacagtgccctttatagga G/A agaaagaagaaattgtgtct 10 11935 G Ͼ A intron 1 tctctgtggagcaaatagag G/A gctgtctgacacttggttcc 11 12281 T Ͼ A intron 1 gaatgtttgatttgtgaaaa T/A cttaataacagtagtttttt 12 12924 T Ͼ C intron 1 gtgctgacaatcttatactc T/C aggttgaacctccggggaag 13 13002 C Ͼ G intron 1 gagcctcaatcacagattct C/G tctagctcacatgaagttaa 14 17715 C Ͼ T intron 1 ggagcatgactttgtggaag C/T ctctcctcttccacccagag 15 17848 T Ͼ C intron 1 gagggctgactgtcaccctt T/C gataggagcccagcactaaa 16 21384 G Ͼ C intron 1 gtgggtgggaggaattggag G/C aggaagcttgcctaagtgtg 17 22145 C Ͼ G intron 1 gtagcttctaaatcaacgaa C/G tgattcctggagagcagctt rs1340361 18 23063 G Ͼ A intron 1 ggaggcacctgtgacaccca G/A cggagtaggggggcggtgtg 19 23131 G Ͼ A intron 1 agtgtgcatatgtgctgacc G/A tgggagcttgtttgtcggtt 20 156 T Ͼ C intron 2 ggacacaggactgtgtggtc T/C ggatatggcatgtggcttat rs1078143 21 384 A Ͼ G intron 2 gctgtgggtgaagtgagtta A/G tggccccactcttagagatc rs1078144 22 1081 G Ͼ A intron 2 agtgcagccaaaattgcaaa G/A tcataccattcaaattaata rs752187 23 2801 A Ͼ G intron 2 aagaaaagtgatttatttca A/G gttgctgatgcttagattgt 24 2830 C Ͼ G intron 2 tgcttagattgttagagttg C/G aaagatctggcttgcatctt 25 2856 A Ͼ G intron 2 tctggcttgcatcttgtaca A/G ctgacagaactggggctcag 26 3187 A Ͼ G intron 2 tgatagctgttgcctgcagc A/G tacggacgttcattgcgcag 27 3190 C Ͼ T intron 2 tagctgttgcctgcagcata C/T ggacgttcattgcgcagttc 28 3194 C Ͼ T intron 2 tgttgcctgcagcatacgga C/T gttcattgcgcagttcctgt 29 3204 G Ͼ A intron 2 agcatacggacgttcattgc G/A cagttcctgtctcctgagat 30 3401 T Ͼ C intron 2 acataaagcctgtgtgctgc T/C gccaggaagactagaaacgc 31 13927 A Ͼ G intron 2 gtcaccacatacctggcact A/G tgctaaggctgggaatgcag L2 32 4163 G Ͼ A intron 3 ccagcccacttcatcttacc G/A tagttacctccttagagtat 33 4262 T Ͼ C intron 3 tgtcaaagaggaactaagga T/C gccagggactttctgcttag 34 4306 C Ͼ T intron 3 ccctctcatcacttctccaa C/T gctggtatcatgaaccccat 35 240 G Ͼ A intron 5 gacagaagaaaagtccccag G/A gaagaatactacagacttgg rs1107281 36 490 G Ͼ A intron 5 gatgggcatttgaacttgtt G/A tctttaaaaagtgaaatctt 37 583 T Ͼ G intron 5 tatctggggagtgggcattt T/G ctgactgaggcattggctgc 38 1051 C Ͼ T inton 5 ggctacaaaactgtgctttc C/T ttgggcagtaaaagaggcaa 39 3051 G Ͼ A intron 5 tagagaacaagtctaattct G/A ttttccttgaaatagtcgaa 40 3127 A Ͼ G intron 5 aagtccatgattttttaggc A/G aaatggcctcctttcctctt 41 5924 C Ͼ T intron 5 ctttctttcacaaaattgcc C/T cccagagctttctggaaggg 42 6831 T Ͼ C intron 5 ccagtccctcagccttgcca T/C tgcttatgctggtctggaaa 43 12678 G Ͼ C intron 5 gctcaccgctctgctcaccc G/C accctctggccatctcctct 44 14214 G Ͼ A intron 5 cagcttggtcccagaggcct G/A gacctgggtcccagaggtcc 45 14257 C Ͼ T intron 5 gctggttccccggcttggtc C/T cagaggcctggatgtgtggc 46 18078 C Ͼ T intron 5 cctaccacaccatgcacgtg C/T acagccaagggttgttgact 47 18795 G Ͼ A intron 5 ctgggctcttcctggacctg G/A ccagctaaaaggaaatctcc 48 18948 G Ͼ A intron 5 gcattggtggtactaagaac G/A catattccctatcctatagg L2 49 19053 T Ͼ C intron 5 ctcccccaacattaaaagtg T/C aagggatgcttattcaaatg MER5A 50 19148 C Ͼ A intron 5 ggcccaagaaactgcatttt C/A gcatgctccctaaatgaagc MER5A 51 19229 C Ͼ T intron 5 atgctaacagtgtagagtca C/T atgtgatgggaagcatcagg 52 19405 T Ͼ C intron 5 cttgctcaatttattctgtc T/C atataactcaatattactga 53 19534 G Ͼ A intron 5 catgtgaccctcttagctcc G/A cggattaactcctgtcctca 54 474 G Ͼ A coding region 6 gaaaccttctctgggttcct G/A tatcacaacctctctctccc Leu 158 Leu 55 210 A Ͼ C intron 6 gcaacctggcgtcatgggcc A/C gctggttaaaataaaattga 56 334 G Ͼ A intron 6 acagttctgaggcaataacc G/A tggttaagggttattgatct 57 2288 C Ͼ T intron 6 cttctttcaaagcttgtggt C/T cactggaccacgtatgaagt 58 2322 T Ͼ C intron 6 atgaagtagaatagtttagg T/C ccagaaaggcaattaagtaa 59 2820 T Ͼ G intron 6 gtgctttgatacattctgag T/G ttcagtaaagagacctgatg 60 656 G Ͼ A coding region 7 tgagctttgtggcctaccaa G/A ggagaaactggctgcagcag Arg 219 Lys Clee et al. 2001 61 416 G Ͼ A intron 7 catcataaagatgacattgt G/A ggctgtcacagttggaaggc 62 471 C Ͼ T intron 7 agaccacactatttagctta C/T ttagtaataacattgcaaag 63 504 G Ͼ A intron 7 ttgcaaagaaaaattccgac G/A aagttttttcagcctaggaa 64 679 G Ͼ C intron 7 gctctggtgaaattcctctc G/C ctaccccaaacatcatcatt 65 1740 C Ͼ T intron 7 acaaatgctcaccctttcag C/T tggaatgattgaaattttgg 66 2122 A Ͼ G intron 7 tgattaaggtggctactacc A/G ggtgctttctgcatatctcg 67 7753 T Ͼ C intrion 7 taggaattccaagctgtgaa T/C tttttactgaagctctttgg 68 8973 A Ͼ T intron 7 atggaaatttgtttatattg A/T ctacagattgccaatattat 69 8976 A Ͼ G intron 7 gaaatttgtttatattgact A/G cagattgccaatattattag Table 1. Continued Repetitive Identity Number Location Exon SNP (5Ј to 3Ј) Substituion sequence to dbSNP Reference 70 11327 G Ͼ C intron 7 ctaacaatcttatttccatt G/C agtccttataaaagaagtgg 71 11738 C Ͼ T intron 7 ctgacgtttaagggagaccg C/T gtaggtccctttgaggactg 72 12295 T Ͼ A intron 7 agtctgtaaattattgttct T/A ttttttctttagcttatgct 73 387 C Ͼ G intron 8 tagcaaggccaatcatttta C/G caacacacatgcttgctaac 74 697 A Ͼ T intron 8 ggaactgtctggtgtccccc A/T gcataggaagctgagccagg 75 1312 G Ͼ A intron 8 attgctctgcagatcccctc G/A cagccctctgtcccttgttc rs1175929 76 3036 T Ͼ G intron 8 ctttatgtgggaagaaattt T/G tttttttgattggggagtgg 77 3176 C Ͼ A intron 8 aaatggcctggttctctgtc C/A cctttctgtctgtatgcctc 78 3364 A Ͼ T intron 8 ggcagaaggcaaagcttagg A/T cctagagagtgctggaccac 79 3373 G Ͼ A intron 8 caaagcttaggacctagaga G/A tgctggaccacgccactcac 80 3561 C Ͼ A intron 8 cagggatttattaatgattt C/A ttgtgaaatgtttggaaata 81 3654 T Ͼ C intron 8 agtgccggaatacatttgca T/C gtaagacagaacgctgcctg 82 4715 C Ͼ T intron 8 ggcagaggggtctcagaatc C/T gcatttccaacaatgtctcc 83 936 C Ͼ T coding region 9 cgtattgtctgcgggcatcc C/T gagggaggggggctgaagat Pro 312 Pro 84 2309 A Ͼ G intron 9 cccctcaagagtcagtttaa A/G tgttggtcatgttagttgtc 85 2392 T Ͼ C intron 9 atgggagggcttgtgcttca T/C gaaaacatttttccagatca 86 228 A Ͼ G intron 10 tggggatggggaggactggc A/G cagggctgctgtgatggggt 87 319 C Ͼ T intron 10 ttctgcggtccctggctccc C/T acctgactccaggtgaacaa 88 377 A Ͼ C intron 11 gaaagaagtgtgggagcaaa A/C gcatgatgttacatgtagac 89 521 G Ͼ A intron 11 agtgctctagagacaattgg G/A ttcaaatgtggagcaggctg 90 2850 G Ͼ C intron 11 ctctatacaatcattatgct G/C ccattgaaataataaataca 91 2976 A Ͼ G intron 11 ctccaattcggtagaaccag A/G gcttcatcttctctgtcgaa 92 3056 C Ͼ T intron 11 gtttgcagctgctgtttttc C/T ggcagcacatctgtgcaggc 93 340 T Ͼ C intron 12 ggcattatttgtgaaactta T/C ctaaaatcgaattcgggtcc 94 381 A Ͼ G intron 12 aattaaatttttgaaatttt A/G tattaaaaattatattagta 95 1728 C Ͼ T intron 14 caggctcagaggccttggcc C/T atcaccctggctcacgtgtg 96 2040 C Ͼ A coding region 15 atgggcctggacaacagcat C/A ctctggtttagctggttcat Ile 680 Ile 97 1382 G Ͼ A intron 15 cttttagacagaaaagttac G/A tgggatattatctcccacag 98 1453 G Ͼ A intron 15 tatataaggagaaaccagtt G/A aaattacctattgaagaaac 99 1567 G Ͼ A intron 15 ttctgcgtagttttgggtaa G/A tcacttatcttctttaggat MIR 100 1617 T Ͼ A intron 15 cagttgcctcatcagaaaga T/A gaacagcattacgcctctgc MIR 101 95 T Ͼ A intron 16 agttgagaacagaagatgat T/A gtcttttccaatgggacatg 102 452 G Ͼ A intron 16 tggtgttttgcttgagtaat G/A ttttctgaactaagcacaac 103 657 T Ͼ C intron 16 ctgttgcctcagtctgggct T/C cataggcatcagcagcccca 104 2473 G Ͼ A coding region 17 gcttcaatctcaccacttcg G/A tctccatgatgctgtttgac Val 825 Ile Clee et al. 2001 105 2649 A Ͼ G coding region 18 ggttccaaccagaagagaat A/G tcagaaagtaagtgctgttg Ile 883 Met Clee et al. 2001 106 1730 C Ͼ G intron 18 tgaaagttcaagcgcagtgc C/G ctgtgtccttacactccact 107 426 A Ͼ G intron 19 aggaccttacagtgggtagt A/G tcaggaggggtcaggggctg 108 468 A Ͼ G intron 19 aaagcaccagcgttagcctc A/G gtggcttccagcacgattcc 109 876 C Ͼ T intron 20 ccctcctcatctaaagtgaa C/T acatggggctcatgtgcagg 110 118 T Ͼ G intron 22 catgggatactcttctgtta T/G cacagaagagataaagggca 111 560 G Ͼ A intron 22 aaagctttgccattctaggg G/A tcatagccatacagggtgaa 112 102 A Ͼ G intron 23 accccttttgccatgttgaa A/G ccaccatctccctgctctgt 113 287 C Ͼ T intron 23 gtcaaagaaaagagacttgt C/T aagaggtaagagccttggct 114 1063 G Ͼ A intron 23 acctttcaccctcaggaagc G/A aggctgttcacacggcacac 115 321 T Ͼ G intron 25 ctctttacttaagtacagtg T/G gaggaacagcggcatcagga MER5A 116 376 G Ͼ C intron 25 gttagaaattcagcaacttg G/C gcccagctcagacctactga MER5A 117 478 C Ͼ T intron 25 catacataggaaatgacaaa C/T gtttatggatggatagtcta 118 579 G Ͼ T intron 25 tcatttaattctcaaaaaaa G/T atgaaaaaatgaacactcag 119 153 C Ͼ T intron 27 aatggtaaaagccacttgtt C/T tttgcagcatcgtgcatgtg 120 1058 C Ͼ T intron 28 actatcatgggagataatga C/T tatggttgtccatgattgga 121 1317 C Ͼ T intron 28 caggacccagtgttctgagt C/T accctgaatgtgagcactat 122 372 T Ͼ C intron 30 tatatgatttttaggttttg T/C ttatcagcttcttcgctttt 123 506 A Ͼ G intron 30 ccttttaaaaagtaagcagt A/G gataaataaattcagtgaag 124 1033 G Ͼ C intron 30 ctggatttcatggtgccttt G/C attttccacatgaaggttgt 125 4281 G Ͼ A coding region 31 tcttccctttgcagagacac G/A ccctgccaggcaggggagga Thr 1427 Thr 126 626 C Ͼ T intron 33 ggctccttgttactgatttc C/T gtcttttctctctgcctttt 127 719 G Ͼ A intron 33 taatagccctcatgctagaa G/A ggagccggagcctgtgtata 128 726 G Ͼ A intron 33 cctcatgctagaagggagcc G/A gagcctgtgtataaggccag 129 889 A Ͼ G intron 33 ctttcctcaatgtctcagct A/G tctaactgtgtgtgtaatca 130 1097 G Ͼ C intron 33 ctgtgcaccccactgtctgg G/C ttttaatgtcaggctgttct 131 4760 G Ͼ A coding region 35 tatgacaggactggacacca G/A aaataatgtcaaggtaaacc Arg 1587 Lys Clee et al. 2001 132 234 T Ͼ C intron 35 aacctatctaaacctcagtt T/C cctcatctgtgaaatggaga MIR 133 411 C Ͼ T intron 37 aactctgtacattttatcag C/T agcttatccatccattgcaa 134 1224 A Ͼ G intron 37 caggcataggtgattcagag A/G tgaaaggtcaagtccctgaa L2 135 1720 G Ͼ T intron 37 aaattaaaattactctgact G/T ggaatccatcgttcagtaag 136 251 T Ͼ G intron 40 tgaaggtaaggaaaatagtg T/G tatttgcttggatccactgg 137 252 T Ͼ C intron 40 gaaggtaaggaaaatagtgt T/C atttgcttggatccactggc 138 319 A Ͼ G intron 40 agcactggaaaagtcaaacc A/G taactttgagaattaggtga Table 2. Characterization of insertion/deletion polymorphisms at the ABCA1 locus Number Location Variations (5Ј to 3Ј) 1 (-1033)-(-1032) ins AT 5Ј flanking region tgacttaaatatttagacat (AT/ϩ) ggtgtgtaggcctgcattcc 2 6368 del C intron 5 ttctgatggggttgttgctg (C/-) tgagaatcatgactgggtgg 3 9709 del T intron 5 cattttctgtctgaaccccc (T/-) cacccattcaggcagctgct 4 13816 del T intron 5 tccctacttctccttttttt (T/-) catttgcctcctccacccac 5 270-271 ins G intron 10 cttttcagggaggagccaaa (G/ϩ) cgctcattgtctgtgcttct 6 611-612 ins C intron 20 tttagcccatcctctccccc (C/ϩ) gccaccctccttattgaggc 7 391-392 ins T intron 32 gagtgccttgggtactctct (T/ϩ) gatgggggactccatgataa 8 847 del C intron 37 gctgtatattgtgaatgtcc (C/-) gttttcaaaagcaaagccaa Nucleotide numbering is according to the mutation nomenclature (den Dunnen and Antonarakis, 2000) (ϩ), insertion polymorphism; (-), deletion polymorphism Table 1. Continued Repetitive Identity Number Location Exon SNP (5Ј to 3Ј) Substituion sequence to dbSNP Reference 139 957 G Ͼ C intron 40 cttgttactcttttttcctt G/C tcatgggtgatagccatttg 140 146 C Ͼ T intron 41 tgatgtgggcatcccgcagc C/T ccctccctgcccatcctgga 141 239 A Ͼ C intron 42 cattggttttatatgcttac A/C tttatgtgttagttattaaa 142 321 T Ͼ A intron 42 aataaatggttgattttgag T/A ttgagtttcatagtccaaaa 143 322 T Ͼ C intron 42 ataaatggttgattttgagt T/C tgagtttcatagtccaaaaa 144 533 G Ͼ A intron 42 agatgaaaaattatgtagat G/A ataatgaatgatacggttct 145 546 A Ͼ G intron 42 tgtagatgataatgaatgat A/G cggttctaaaaagacaggtt 146 739 T Ͼ A intron 43 tacagccacacttaaaatgg T/A cccattatgaaatacatatt 147 18 T Ͼ C intron 44 taggtgagaaaagaagtggc T/C tgtattttgctgcaaagact 148 264 T Ͼ C intron 44 acaatataatttgcttgttt T/C ttaagagtataatttagtga L1MB8 149 279 T Ͼ C intron 44 tgttttttaagagtataatt T/C agtgatttttggtaaattga L1MB8 150 508 C Ͼ T intron 44 tttacattgctacataaaat C/T cccctatgtacatgtaccta 151 1477 A Ͼ T intron 44 gatctcctctcctgtctctt A/T catttttgcagtagcaatgt 152 1665 G Ͼ A intron 44 tggttgtaagaactgatttg G/A ttggtatagctgtgagggcc 153 1956 T Ͼ G intron 44 gtgttgctcacactcaaaat T/G tctgggccttctcatttggt 154 68 T Ͼ C intron 45 aatatataccttatggcttt T/C ccacacgcattgacttcagg 155 608 G Ͼ C intron 46 ttatactgacttcaatagag G/C tttcagacaaaaagttgttt 156 336 T Ͼ C intron 47 ttcacaattgtaaacaccac T/C acactgaacagcatcatccc L1MD2 157 55 G Ͼ C intron 49 agggtgtggattcctgcccc G/C acactcccgcccataggtcc rs1331924 158 7479 C Ͼ T 3Ј untranslated region 50 aacaaaaatgtgggtgtctc C/T aggcacgggaaacttggttc 159 8226 C Ͼ T 3Ј untranslated region 50 aggagcccactgtaacaata C/T tgggcagccttttttttttt 160 8682 G Ͼ A 3Ј untranslated region 50 aacttcttccactttttcca G/A aatttgaatattaacgctaa rs363717 161 8697 C Ͼ T 3Ј untranslated region 50 ttccagaatttgaatattaa C/T gctaaaggtgtaagacttca 162 9097 A Ͼ G 3Ј untranslated region 50 aactattttgaagaaaacac A/G acattttaatacagattgaa Nucleotide numbering is according to the mutation nomenclature (den Dunnen and Antonarakis, 2000) is an important resource for understanding not only the etiology and risk of some diseases, but also the pharmacokinetics or pharmacodyamics of drugs used to treat them.
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ABCA1 p.Arg219Lys 11558901:15:5334
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39 In fact, it is reported that the R219K substitution is associated with a decreased severity of atherosclerosis, a decreased risk of coronary events, decreased triglycerides, and a higher level of HDL cholesterol (HDL-C) in plasma (Clee et al. 2001).
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ABCA1 p.Arg219Lys 11558901:39:33
status: NEW
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19 Microsatellite sequences are also shown Table 1. Characterization of 162 single-nucleotide polymorphisms (SNPs) within the ABCA1 locus Repetitive Identity Number Location Exon SNP (5b18; to 3b18;) Substituion sequence to dbSNP Reference 1 afa;278 G b0e; C 5b18; flanking region gggcccgggcgggggaaggg G/C acgcagaccgcggaccctaa rs1800976 2 afa;99 G b0e; C 5b18; flanking region acataaacagaggccgggaa G/C ggggcggggaggagggagag 3 159 G b0e; T intron 1 gcggtgttaaatggggagac G/T atgtcctagtacgagctctg 4 506 G b0e; C intron 1 gaattggctatatgctcccc G/C ggactggagcggcacagtcc 5 5897 T b0e; G intron 1 gtacaaaaccctttagcttt T/G gcaaacctcctttaagaccc 6 5929 C b0e; T intron 1 ttaagacccgatttaaatgc C/T tccctcctcatgaagctctt 7 5962 T b0e; C intron 1 aagctcttctggatccactc T/C ttcccatcactaagttgaaa 8 5985 A b0e; C intron 1 cccatcactaagttgaaagt A/C agatccccttctctttactt 9 11416 G b0e; A intron 1 ttacagtgccctttatagga G/A agaaagaagaaattgtgtct 10 11935 G b0e; A intron 1 tctctgtggagcaaatagag G/A gctgtctgacacttggttcc 11 12281 T b0e; A intron 1 gaatgtttgatttgtgaaaa T/A cttaataacagtagtttttt 12 12924 T b0e; C intron 1 gtgctgacaatcttatactc T/C aggttgaacctccggggaag 13 13002 C b0e; G intron 1 gagcctcaatcacagattct C/G tctagctcacatgaagttaa 14 17715 C b0e; T intron 1 ggagcatgactttgtggaag C/T ctctcctcttccacccagag 15 17848 T b0e; C intron 1 gagggctgactgtcaccctt T/C gataggagcccagcactaaa 16 21384 G b0e; C intron 1 gtgggtgggaggaattggag G/C aggaagcttgcctaagtgtg 17 22145 C b0e; G intron 1 gtagcttctaaatcaacgaa C/G tgattcctggagagcagctt rs1340361 18 23063 G b0e; A intron 1 ggaggcacctgtgacaccca G/A cggagtaggggggcggtgtg 19 23131 G b0e; A intron 1 agtgtgcatatgtgctgacc G/A tgggagcttgtttgtcggtt 20 156 T b0e; C intron 2 ggacacaggactgtgtggtc T/C ggatatggcatgtggcttat rs1078143 21 384 A b0e; G intron 2 gctgtgggtgaagtgagtta A/G tggccccactcttagagatc rs1078144 22 1081 G b0e; A intron 2 agtgcagccaaaattgcaaa G/A tcataccattcaaattaata rs752187 23 2801 A b0e; G intron 2 aagaaaagtgatttatttca A/G gttgctgatgcttagattgt 24 2830 C b0e; G intron 2 tgcttagattgttagagttg C/G aaagatctggcttgcatctt 25 2856 A b0e; G intron 2 tctggcttgcatcttgtaca A/G ctgacagaactggggctcag 26 3187 A b0e; G intron 2 tgatagctgttgcctgcagc A/G tacggacgttcattgcgcag 27 3190 C b0e; T intron 2 tagctgttgcctgcagcata C/T ggacgttcattgcgcagttc 28 3194 C b0e; T intron 2 tgttgcctgcagcatacgga C/T gttcattgcgcagttcctgt 29 3204 G b0e; A intron 2 agcatacggacgttcattgc G/A cagttcctgtctcctgagat 30 3401 T b0e; C intron 2 acataaagcctgtgtgctgc T/C gccaggaagactagaaacgc 31 13927 A b0e; G intron 2 gtcaccacatacctggcact A/G tgctaaggctgggaatgcag L2 32 4163 G b0e; A intron 3 ccagcccacttcatcttacc G/A tagttacctccttagagtat 33 4262 T b0e; C intron 3 tgtcaaagaggaactaagga T/C gccagggactttctgcttag 34 4306 C b0e; T intron 3 ccctctcatcacttctccaa C/T gctggtatcatgaaccccat 35 240 G b0e; A intron 5 gacagaagaaaagtccccag G/A gaagaatactacagacttgg rs1107281 36 490 G b0e; A intron 5 gatgggcatttgaacttgtt G/A tctttaaaaagtgaaatctt 37 583 T b0e; G intron 5 tatctggggagtgggcattt T/G ctgactgaggcattggctgc 38 1051 C b0e; T inton 5 ggctacaaaactgtgctttc C/T ttgggcagtaaaagaggcaa 39 3051 G b0e; A intron 5 tagagaacaagtctaattct G/A ttttccttgaaatagtcgaa 40 3127 A b0e; G intron 5 aagtccatgattttttaggc A/G aaatggcctcctttcctctt 41 5924 C b0e; T intron 5 ctttctttcacaaaattgcc C/T cccagagctttctggaaggg 42 6831 T b0e; C intron 5 ccagtccctcagccttgcca T/C tgcttatgctggtctggaaa 43 12678 G b0e; C intron 5 gctcaccgctctgctcaccc G/C accctctggccatctcctct 44 14214 G b0e; A intron 5 cagcttggtcccagaggcct G/A gacctgggtcccagaggtcc 45 14257 C b0e; T intron 5 gctggttccccggcttggtc C/T cagaggcctggatgtgtggc 46 18078 C b0e; T intron 5 cctaccacaccatgcacgtg C/T acagccaagggttgttgact 47 18795 G b0e; A intron 5 ctgggctcttcctggacctg G/A ccagctaaaaggaaatctcc 48 18948 G b0e; A intron 5 gcattggtggtactaagaac G/A catattccctatcctatagg L2 49 19053 T b0e; C intron 5 ctcccccaacattaaaagtg T/C aagggatgcttattcaaatg MER5A 50 19148 C b0e; A intron 5 ggcccaagaaactgcatttt C/A gcatgctccctaaatgaagc MER5A 51 19229 C b0e; T intron 5 atgctaacagtgtagagtca C/T atgtgatgggaagcatcagg 52 19405 T b0e; C intron 5 cttgctcaatttattctgtc T/C atataactcaatattactga 53 19534 G b0e; A intron 5 catgtgaccctcttagctcc G/A cggattaactcctgtcctca 54 474 G b0e; A coding region 6 gaaaccttctctgggttcct G/A tatcacaacctctctctccc Leu 158 Leu 55 210 A b0e; C intron 6 gcaacctggcgtcatgggcc A/C gctggttaaaataaaattga 56 334 G b0e; A intron 6 acagttctgaggcaataacc G/A tggttaagggttattgatct 57 2288 C b0e; T intron 6 cttctttcaaagcttgtggt C/T cactggaccacgtatgaagt 58 2322 T b0e; C intron 6 atgaagtagaatagtttagg T/C ccagaaaggcaattaagtaa 59 2820 T b0e; G intron 6 gtgctttgatacattctgag T/G ttcagtaaagagacctgatg 60 656 G b0e; A coding region 7 tgagctttgtggcctaccaa G/A ggagaaactggctgcagcag Arg 219 Lys Clee et al. 2001 61 416 G b0e; A intron 7 catcataaagatgacattgt G/A ggctgtcacagttggaaggc 62 471 C b0e; T intron 7 agaccacactatttagctta C/T ttagtaataacattgcaaag 63 504 G b0e; A intron 7 ttgcaaagaaaaattccgac G/A aagttttttcagcctaggaa 64 679 G b0e; C intron 7 gctctggtgaaattcctctc G/C ctaccccaaacatcatcatt 65 1740 C b0e; T intron 7 acaaatgctcaccctttcag C/T tggaatgattgaaattttgg 66 2122 A b0e; G intron 7 tgattaaggtggctactacc A/G ggtgctttctgcatatctcg 67 7753 T b0e; C intrion 7 taggaattccaagctgtgaa T/C tttttactgaagctctttgg 68 8973 A b0e; T intron 7 atggaaatttgtttatattg A/T ctacagattgccaatattat 69 8976 A b0e; G intron 7 gaaatttgtttatattgact A/G cagattgccaatattattag Table 1. Continued Repetitive Identity Number Location Exon SNP (5b18; to 3b18;) Substituion sequence to dbSNP Reference 70 11327 G b0e; C intron 7 ctaacaatcttatttccatt G/C agtccttataaaagaagtgg 71 11738 C b0e; T intron 7 ctgacgtttaagggagaccg C/T gtaggtccctttgaggactg 72 12295 T b0e; A intron 7 agtctgtaaattattgttct T/A ttttttctttagcttatgct 73 387 C b0e; G intron 8 tagcaaggccaatcatttta C/G caacacacatgcttgctaac 74 697 A b0e; T intron 8 ggaactgtctggtgtccccc A/T gcataggaagctgagccagg 75 1312 G b0e; A intron 8 attgctctgcagatcccctc G/A cagccctctgtcccttgttc rs1175929 76 3036 T b0e; G intron 8 ctttatgtgggaagaaattt T/G tttttttgattggggagtgg 77 3176 C b0e; A intron 8 aaatggcctggttctctgtc C/A cctttctgtctgtatgcctc 78 3364 A b0e; T intron 8 ggcagaaggcaaagcttagg A/T cctagagagtgctggaccac 79 3373 G b0e; A intron 8 caaagcttaggacctagaga G/A tgctggaccacgccactcac 80 3561 C b0e; A intron 8 cagggatttattaatgattt C/A ttgtgaaatgtttggaaata 81 3654 T b0e; C intron 8 agtgccggaatacatttgca T/C gtaagacagaacgctgcctg 82 4715 C b0e; T intron 8 ggcagaggggtctcagaatc C/T gcatttccaacaatgtctcc 83 936 C b0e; T coding region 9 cgtattgtctgcgggcatcc C/T gagggaggggggctgaagat Pro 312 Pro 84 2309 A b0e; G intron 9 cccctcaagagtcagtttaa A/G tgttggtcatgttagttgtc 85 2392 T b0e; C intron 9 atgggagggcttgtgcttca T/C gaaaacatttttccagatca 86 228 A b0e; G intron 10 tggggatggggaggactggc A/G cagggctgctgtgatggggt 87 319 C b0e; T intron 10 ttctgcggtccctggctccc C/T acctgactccaggtgaacaa 88 377 A b0e; C intron 11 gaaagaagtgtgggagcaaa A/C gcatgatgttacatgtagac 89 521 G b0e; A intron 11 agtgctctagagacaattgg G/A ttcaaatgtggagcaggctg 90 2850 G b0e; C intron 11 ctctatacaatcattatgct G/C ccattgaaataataaataca 91 2976 A b0e; G intron 11 ctccaattcggtagaaccag A/G gcttcatcttctctgtcgaa 92 3056 C b0e; T intron 11 gtttgcagctgctgtttttc C/T ggcagcacatctgtgcaggc 93 340 T b0e; C intron 12 ggcattatttgtgaaactta T/C ctaaaatcgaattcgggtcc 94 381 A b0e; G intron 12 aattaaatttttgaaatttt A/G tattaaaaattatattagta 95 1728 C b0e; T intron 14 caggctcagaggccttggcc C/T atcaccctggctcacgtgtg 96 2040 C b0e; A coding region 15 atgggcctggacaacagcat C/A ctctggtttagctggttcat Ile 680 Ile 97 1382 G b0e; A intron 15 cttttagacagaaaagttac G/A tgggatattatctcccacag 98 1453 G b0e; A intron 15 tatataaggagaaaccagtt G/A aaattacctattgaagaaac 99 1567 G b0e; A intron 15 ttctgcgtagttttgggtaa G/A tcacttatcttctttaggat MIR 100 1617 T b0e; A intron 15 cagttgcctcatcagaaaga T/A gaacagcattacgcctctgc MIR 101 95 T b0e; A intron 16 agttgagaacagaagatgat T/A gtcttttccaatgggacatg 102 452 G b0e; A intron 16 tggtgttttgcttgagtaat G/A ttttctgaactaagcacaac 103 657 T b0e; C intron 16 ctgttgcctcagtctgggct T/C cataggcatcagcagcccca 104 2473 G b0e; A coding region 17 gcttcaatctcaccacttcg G/A tctccatgatgctgtttgac Val 825 Ile Clee et al. 2001 105 2649 A b0e; G coding region 18 ggttccaaccagaagagaat A/G tcagaaagtaagtgctgttg Ile 883 Met Clee et al. 2001 106 1730 C b0e; G intron 18 tgaaagttcaagcgcagtgc C/G ctgtgtccttacactccact 107 426 A b0e; G intron 19 aggaccttacagtgggtagt A/G tcaggaggggtcaggggctg 108 468 A b0e; G intron 19 aaagcaccagcgttagcctc A/G gtggcttccagcacgattcc 109 876 C b0e; T intron 20 ccctcctcatctaaagtgaa C/T acatggggctcatgtgcagg 110 118 T b0e; G intron 22 catgggatactcttctgtta T/G cacagaagagataaagggca 111 560 G b0e; A intron 22 aaagctttgccattctaggg G/A tcatagccatacagggtgaa 112 102 A b0e; G intron 23 accccttttgccatgttgaa A/G ccaccatctccctgctctgt 113 287 C b0e; T intron 23 gtcaaagaaaagagacttgt C/T aagaggtaagagccttggct 114 1063 G b0e; A intron 23 acctttcaccctcaggaagc G/A aggctgttcacacggcacac 115 321 T b0e; G intron 25 ctctttacttaagtacagtg T/G gaggaacagcggcatcagga MER5A 116 376 G b0e; C intron 25 gttagaaattcagcaacttg G/C gcccagctcagacctactga MER5A 117 478 C b0e; T intron 25 catacataggaaatgacaaa C/T gtttatggatggatagtcta 118 579 G b0e; T intron 25 tcatttaattctcaaaaaaa G/T atgaaaaaatgaacactcag 119 153 C b0e; T intron 27 aatggtaaaagccacttgtt C/T tttgcagcatcgtgcatgtg 120 1058 C b0e; T intron 28 actatcatgggagataatga C/T tatggttgtccatgattgga 121 1317 C b0e; T intron 28 caggacccagtgttctgagt C/T accctgaatgtgagcactat 122 372 T b0e; C intron 30 tatatgatttttaggttttg T/C ttatcagcttcttcgctttt 123 506 A b0e; G intron 30 ccttttaaaaagtaagcagt A/G gataaataaattcagtgaag 124 1033 G b0e; C intron 30 ctggatttcatggtgccttt G/C attttccacatgaaggttgt 125 4281 G b0e; A coding region 31 tcttccctttgcagagacac G/A ccctgccaggcaggggagga Thr 1427 Thr 126 626 C b0e; T intron 33 ggctccttgttactgatttc C/T gtcttttctctctgcctttt 127 719 G b0e; A intron 33 taatagccctcatgctagaa G/A ggagccggagcctgtgtata 128 726 G b0e; A intron 33 cctcatgctagaagggagcc G/A gagcctgtgtataaggccag 129 889 A b0e; G intron 33 ctttcctcaatgtctcagct A/G tctaactgtgtgtgtaatca 130 1097 G b0e; C intron 33 ctgtgcaccccactgtctgg G/C ttttaatgtcaggctgttct 131 4760 G b0e; A coding region 35 tatgacaggactggacacca G/A aaataatgtcaaggtaaacc Arg 1587 Lys Clee et al. 2001 132 234 T b0e; C intron 35 aacctatctaaacctcagtt T/C cctcatctgtgaaatggaga MIR 133 411 C b0e; T intron 37 aactctgtacattttatcag C/T agcttatccatccattgcaa 134 1224 A b0e; G intron 37 caggcataggtgattcagag A/G tgaaaggtcaagtccctgaa L2 135 1720 G b0e; T intron 37 aaattaaaattactctgact G/T ggaatccatcgttcagtaag 136 251 T b0e; G intron 40 tgaaggtaaggaaaatagtg T/G tatttgcttggatccactgg 137 252 T b0e; C intron 40 gaaggtaaggaaaatagtgt T/C atttgcttggatccactggc 138 319 A b0e; G intron 40 agcactggaaaagtcaaacc A/G taactttgagaattaggtga Table 2. Characterization of insertion/deletion polymorphisms at the ABCA1 locus Number Location Variations (5b18; to 3b18;) 1 (afa;1033)-(afa;1032) ins AT 5b18; flanking region tgacttaaatatttagacat (AT/af9;) ggtgtgtaggcctgcattcc 2 6368 del C intron 5 ttctgatggggttgttgctg (C/afa;) tgagaatcatgactgggtgg 3 9709 del T intron 5 cattttctgtctgaaccccc (T/afa;) cacccattcaggcagctgct 4 13816 del T intron 5 tccctacttctccttttttt (T/afa;) catttgcctcctccacccac 5 270-271 ins G intron 10 cttttcagggaggagccaaa (G/af9;) cgctcattgtctgtgcttct 6 611-612 ins C intron 20 tttagcccatcctctccccc (C/af9;) gccaccctccttattgaggc 7 391-392 ins T intron 32 gagtgccttgggtactctct (T/af9;) gatgggggactccatgataa 8 847 del C intron 37 gctgtatattgtgaatgtcc (C/afa;) gttttcaaaagcaaagccaa Nucleotide numbering is according to the mutation nomenclature (den Dunnen and Antonarakis, 2000) (af9;), insertion polymorphism; (afa;), deletion polymorphism Table 1. Continued Repetitive Identity Number Location Exon SNP (5b18; to 3b18;) Substituion sequence to dbSNP Reference 139 957 G b0e; C intron 40 cttgttactcttttttcctt G/C tcatgggtgatagccatttg 140 146 C b0e; T intron 41 tgatgtgggcatcccgcagc C/T ccctccctgcccatcctgga 141 239 A b0e; C intron 42 cattggttttatatgcttac A/C tttatgtgttagttattaaa 142 321 T b0e; A intron 42 aataaatggttgattttgag T/A ttgagtttcatagtccaaaa 143 322 T b0e; C intron 42 ataaatggttgattttgagt T/C tgagtttcatagtccaaaaa 144 533 G b0e; A intron 42 agatgaaaaattatgtagat G/A ataatgaatgatacggttct 145 546 A b0e; G intron 42 tgtagatgataatgaatgat A/G cggttctaaaaagacaggtt 146 739 T b0e; A intron 43 tacagccacacttaaaatgg T/A cccattatgaaatacatatt 147 18 T b0e; C intron 44 taggtgagaaaagaagtggc T/C tgtattttgctgcaaagact 148 264 T b0e; C intron 44 acaatataatttgcttgttt T/C ttaagagtataatttagtga L1MB8 149 279 T b0e; C intron 44 tgttttttaagagtataatt T/C agtgatttttggtaaattga L1MB8 150 508 C b0e; T intron 44 tttacattgctacataaaat C/T cccctatgtacatgtaccta 151 1477 A b0e; T intron 44 gatctcctctcctgtctctt A/T catttttgcagtagcaatgt 152 1665 G b0e; A intron 44 tggttgtaagaactgatttg G/A ttggtatagctgtgagggcc 153 1956 T b0e; G intron 44 gtgttgctcacactcaaaat T/G tctgggccttctcatttggt 154 68 T b0e; C intron 45 aatatataccttatggcttt T/C ccacacgcattgacttcagg 155 608 G b0e; C intron 46 ttatactgacttcaatagag G/C tttcagacaaaaagttgttt 156 336 T b0e; C intron 47 ttcacaattgtaaacaccac T/C acactgaacagcatcatccc L1MD2 157 55 G b0e; C intron 49 agggtgtggattcctgcccc G/C acactcccgcccataggtcc rs1331924 158 7479 C b0e; T 3b18; untranslated region 50 aacaaaaatgtgggtgtctc C/T aggcacgggaaacttggttc 159 8226 C b0e; T 3b18; untranslated region 50 aggagcccactgtaacaata C/T tgggcagccttttttttttt 160 8682 G b0e; A 3b18; untranslated region 50 aacttcttccactttttcca G/A aatttgaatattaacgctaa rs363717 161 8697 C b0e; T 3b18; untranslated region 50 ttccagaatttgaatattaa C/T gctaaaggtgtaagacttca 162 9097 A b0e; G 3b18; untranslated region 50 aactattttgaagaaaacac A/G acattttaatacagattgaa Nucleotide numbering is according to the mutation nomenclature (den Dunnen and Antonarakis, 2000) is an important resource for understanding not only the etiology and risk of some diseases, but also the pharmacokinetics or pharmacodyamics of drugs used to treat them.
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ABCA1 p.Arg219Lys 11558901:19:4893
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43 In fact, it is reported that the R219K substitution is associated with a decreased severity of atherosclerosis, a decreased risk of coronary events, decreased triglycerides, and a higher level of HDL cholesterol (HDL-C) in plasma (Clee et al. 2001).
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ABCA1 p.Arg219Lys 11558901:43:33
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PMID: 18537706 [PubMed] Koehn J et al: "Multiple drug resistance associated with function of ABC-transporters in diabetes mellitus: molecular mechanism and clinical relevance."
No. Sentence Comment
130 In humans various studies link variations in ABCA1 to T2D [62, 63, 64, 65, 66] and the ABCA1 variant R219K has been associated with reduced responsiveness to the thiazolidinedione drug rosiglitazone used as insulin sensitizer in T2D [67].
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ABCA1 p.Arg219Lys 18537706:130:101
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PMID: 18508037 [PubMed] Uehara Y et al: "ATP-binding cassette transporter G4 is highly expressed in microglia in Alzheimer's brain."
No. Sentence Comment
123 The genetic variant R219K of ABCA1 was found to be associated with increased HDL cholesterol, and it delayed the age of onset of AD (Wollmer et al., 2003).
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ABCA1 p.Arg219Lys 18508037:123:20
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PMID: 16596262 [PubMed] Kolsch H et al: "Polymorphism in ABCA1 influences CSF 24S-hydroxycholesterol levels but is not a major risk factor of Alzheimer's disease."
No. Sentence Comment
2 Since altered cholesterol metabolism is also involved in Alzheimer's disease (AD), the effects of two ABCA1 polymorphisms (G-395C promoter polymorphism (rs 2246293) and exonic R219K) on the risk of AD in 241 AD patients and 294 non-demented controls, and on CSF cholesterol and 24S-hydroxycholesterol in 74 AD patients and 42 non-demented controls were investigated.
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ABCA1 p.Arg219Lys 16596262:2:176
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4 However, the ABCA1 G-395C polymorphism influenced CSF levels of 24S-hydroxycholesterol, but not of cholesterol, whereas the R219K influenced neither CSF levels of 24S-hydroxycholesterol nor cholesterol.
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ABCA1 p.Arg219Lys 16596262:4:124
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18 Furthermore, an exonic non-synonymous (R219K) polymorphism influenced CSF cholesterol levels and risk of premature coronary heart disease in patients with hypercholesterolemia (17).
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ABCA1 p.Arg219Lys 16596262:18:39
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21 To further explore the effect of ABCA1 G-395C and R219K polymorphisms on AD risk and on the CSF levels of cholesterol and 24S-hydroxycholesterol, we investigated genotype distribution in a homogeneous age matched sample of German origin.
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ABCA1 p.Arg219Lys 16596262:21:50
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32 The G-395C promoter polymorphism [rs 2246293 (13)] and the R219K polymorphism in ABCA1 were determined by RFLP.
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ABCA1 p.Arg219Lys 16596262:32:59
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33 In brief, for the G-395C polymorphism the whole product was amplified using the following primers: 5'-TGAGGGAGAT TCAGCCTAGATC-3' (forward) and 5'-AGTGGAATTTGC TTCCTCTAGATC-3' (reverse), the forward primer contained a nucleotide change (underlined), to generate a control restriction site specific for BstY I. The amplification products of the Gand the C-alleles were 72, 24 and 18 bp or 96 and 18 bp. The R219K polymorphism was investigated by using the following primers: 5'- TCAGAAGAGATGATTCAACT TGG -3' (forward) and 5'-TTTCTACAAAACAAAGTCAT CCTG-3' (reverse), the reverse primer contained a nucleotide change (underlined), to generate a control restriction site specific for EcoN I. The amplification products of the Ror the K-alleles were 190 and 27 bp or 135, 55 and 27 bp. The APOE genotype was studied as described (24).
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ABCA1 p.Arg219Lys 16596262:33:405
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45 The power to detect a relative risk of 2.0 with &#b7;=0.05 was 98% for the R219K polymorphism and 92% for the G-395C polymorphism.
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ABCA1 p.Arg219Lys 16596262:45:75
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50 Genotype distribution and allele frequencies of both polymorphisms in AD patients and controls are given in Table I. Logistic regression analysis revealed that the two investigated ABCA1 polymorphisms did not influence the risk of AD (G-395C, presence of C-allele: c7;2 =0.31, d.f.=1, p=0.59; R219K, presence of K-allele: c7;2 =0.65, d.f.=1, p=0.42).
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ABCA1 p.Arg219Lys 16596262:50:296
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51 There was also no interaction between both ABCA1 polymorphisms on the risk of AD (c7;2 =0.81, d.f.=1, p=0.37), and no interaction between ABCA1 polymorphisms and the APOE4 allele (G-395C, presence of C-allele vs. presence of APOE4: c7;2 =1.61, d.f.=1, p=0.21; R219K, presence of K-allele vs. presence of APOE4: c7;2 =0.01, d.f.=1, p=0.95).
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ABCA1 p.Arg219Lys 16596262:51:266
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55 ----------------------------------------------------------------------------------------------------- ABCA1 G-395C Allele frequency Genotype &#af;2 test -------------- -------------- ----------------------------- --------------- n G C G/G (%) G/C (%) C/C (%) &#af; df p ----------------------------------------------------------------------------------------------------- AD patients 241 0.55 0.45 74 (30.7) 115 (47.7) 52 (21.6) 0.82 2 0.67 Controls 294 0.53 0.47 80 (27.2 149 (50.7) 65 (22.1) ----------------------------------------------------------------------------------------------------- ABCA1 R219K Allele frequency Genotype &#af;2 test ------------- -------------- ----------------------------- --------------- n R K R/R (%) R/K (%) K/K (%) &#af; df p ----------------------------------------------------------------------------------------------------- AD patients 241 0.72 0.28 130 (53.9) 88 (36.5) 23 (9.5) 1.89 2 0.39 Controls 294 0.72 0.28 149 (50.7) 123 (41.8) 22 (7.5) ----------------------------------------------------------------------------------------------------- 24S-hydroxycholesterol concentrations were lower in probands who were carriers of at least one C-allele of the ABCA1 G-395C polymorphism than in carriers of the GG-genotype (F=5.74, d.f.=1, p=0.018; Fig. 1); however, levels of cholesterol were not influenced by this polymorphism (F=0.87, d.f.=1, p=0.35).
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ABCA1 p.Arg219Lys 16596262:55:602
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56 We did not find any effect of the ABCA1 R219K polymorphism on the CSF levels of cholesterol (F=0.68, d.f.=1, p=0.41) or of 24S-hydroxycholesterol (F=0.01, d.f.=1, p=0.91) in our whole proband sample.
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ABCA1 p.Arg219Lys 16596262:56:40
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61 Since a previous publication (19) reported altered levels of cholesterol depending on ABCA1 polymorphisms only in non-demented probands, statistical analysis assessed the interaction between ABCA1 polymorphisms and diagnosis: we did not find any significant interaction of ABCA1 polymorphisms and diagnosis either on cholesterol levels (G-395C, presence of C-allele vs. diagnosis: c7;2 =0.56, d.f.=1, p=0.45; R219K, presence of K-allele vs. diagnosis: c7;2 =0.07, d.f.=1, p=0.94) or on levels of 24S-hydroxycholesterol (G-395C, presence of C-allele vs. diagnosis: c7;2 =3.2, d.f.=1, p=0.08; R219K, presence of K-allele vs. diagnosis: c7;2 =0.27, d.f.=1, p=0.61).
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ABCA1 p.Arg219Lys 16596262:61:412
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ABCA1 p.Arg219Lys 16596262:61:600
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62 Discussion We investigated the ABCA1 G-395C and R219K polymorphisms for their influence on the risk of AD and on CSF levels of cholesterol and 24S-hydroxycholesterol.
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ABCA1 p.Arg219Lys 16596262:62:48
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65 The exonic R219K polymorphism in ABCA1 has been shown to influence CSF cholesterol levels in healthy probands (19), while our study did not detect any effect.
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ABCA1 p.Arg219Lys 16596262:65:11
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67 We also did not find the exonic R219K or the promoter G-395C polymorphisms to influence the risk of AD; thus, we cannot support the suggestion that polymorphisms in ABCA1 might act as risk factors of AD.
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ABCA1 p.Arg219Lys 16596262:67:32
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PMID: 18219093 [PubMed] Balcerzyk A et al: "Protective effect of R allele of PON1 gene on the coronary artery disease in the presence of specific genetic background."
No. Sentence Comment
64 ABCA1 R219K polymorphism was genotyped using a method described by Clee et al. [8], with some modifications.
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ABCA1 p.Arg219Lys 18219093:64:6
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PMID: 22403555 [PubMed] Piehler AP et al: "A-Subclass ATP-Binding Cassette Proteins in Brain Lipid Homeostasis and Neurodegeneration."
No. Sentence Comment
97 Among the allelic variants identified in the ABCA1 gene, the SNPs rs2230806 (R219K), rs4149313 (I883M), and rs2230808 (R1587K) have been most extensively studied.
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ABCA1 p.Arg219Lys 22403555:97:77
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96 Among the allelic variants identified in the ABCA1 gene, the SNPs rs2230806 (R219K), rs4149313 (I883M), and rs2230808 (R1587K) have been most extensively studied.
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ABCA1 p.Arg219Lys 22403555:96:77
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PMID: 22419126 [PubMed] Guay SP et al: "ABCA1 gene promoter DNA methylation is associated with HDL particle profile and coronary artery disease in familial hypercholesterolemia."
No. Sentence Comment
211 Associations of the ATP-binding cassette transporter A1 R219K polymorphism with HDL-C level and coronary artery disease risk: a meta-analysis.
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ABCA1 p.Arg219Lys 22419126:211:56
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PMID: 23053993 [PubMed] Li YY et al: "ATP-binding cassette transporter A1 R219K polymorphism and coronary artery disease in Chinese population: a meta-analysis of 5,388 participants."
No. Sentence Comment
0 ATP-binding cassette transporter A1 R219K polymorphism and coronary artery disease in Chinese population: a meta-analysis of 5,388 participants Yan-yan Li ߦ Hui Zhang ߦ Xiao-yi Qin ߦ Xin-zheng Lu ߦ Bing Yang ߦ Ming-long Chen Received: 16 January 2012 / Accepted: 1 October 2012 / Published online: 9 October 2012 &#d3; Springer Science+Business Media Dordrecht 2012 Abstract The ATP-binding cassette transporter A1 (ABCA1) R219K gene polymorphism has been suggested to lower the risk of coronary artery disease (CAD).
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ABCA1 p.Arg219Lys 23053993:0:36
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ABCA1 p.Arg219Lys 23053993:0:453
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2 Meta-analysis involving 2,730 CAD patients and 2,658 controls was performed to investigate the relationship between ABCA1 R219K gene polymorphism and CAD in Chinese population.
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ABCA1 p.Arg219Lys 23053993:2:122
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5 A significant association between ABCA1 R219K gene polymorphism and CAD was found in the Chinese population under the following genetic models: an allelic genetic model (OR 0.70, 95 % CI 0.62-0.78, P \ 0.00001), a recessive genetic model (OR 0.51, 95 % CI 0.41-0.64, P \ 0.00001), an additive genetic model (OR 0.816, 95 % CI 0780-0.855, P = 0), a dominant genetic model (OR 1.326, 95 % CI 1.232-1.427, P = 0), a homozygote genetic model (OR 0.640, 95 % CI 0.575-0.712, P = 0), and a heterozygote genetic model (OR 0.640, 95 % CI 0.575-0.712, P = 0).
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ABCA1 p.Arg219Lys 23053993:5:40
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6 The K allele of the ABCA1 R219K gene has a protective role for CAD risk in Chinese population and is possibly associated with decreased CAD susceptibility.
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ABCA1 p.Arg219Lys 23053993:6:26
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7 Keywords ATP-binding cassette transporter A1  R219K  Gene polymorphism  Coronary artery disease  Chinese Introduction Coronary artery disease (CAD) is one of the leading causes of death.
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ABCA1 p.Arg219Lys 23053993:7:47
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20 R219K is a common variation in the ABCA1 gene-coding region.
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ABCA1 p.Arg219Lys 23053993:20:0
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24 [7] found that ABCA1 R219K polymorphism was associated with a higher HDL-C level in Asians and performed a protective role for CAD in both Asians and Caucasians.
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ABCA1 p.Arg219Lys 23053993:24:21
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26 They reported that the K allele of ABCA1 R219K polymorphism was a protective factor associated with decreased CAD susceptibility worldwide [8].
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ABCA1 p.Arg219Lys 23053993:26:41
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29 Domestically, results of the widely researched topics of ABCA1 R219K gene polymorphism and CAD are still debatable [10, 11].
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ABCA1 p.Arg219Lys 23053993:29:63
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30 Hence, the current meta-analysis on 2,730 CAD patients and 2,658 subjects was conducted to arrive at a decisive conclusion on the associations between ABCA1 R219K gene polymorphism and CAD in the Chinese population.
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ABCA1 p.Arg219Lys 23053993:30:157
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33 The studies had to comply with the following major criteria: (a) Evaluation of the ABCA1 R219K gene polymorphism and CAD in Chinese population; (b) CAD was diagnosed by coronary arteriography and clinical symptoms combined with electrocardiogram, echocardiography, treadmill exercise test, and myocardial perfusion imaging in emission computed tomography (ECT); (c) The individual study should be a case-control or cohort study published in an official journal; and (d) The individual study should agree with the Hardy-Weinberg equilibrium (HWE).
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ABCA1 p.Arg219Lys 23053993:33:89
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45 The odds ratios (ORs) corresponding to 95 % confidence intervals (CIs) were used to examine the association between ABCA1 R219K gene polymorphism and CAD.
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ABCA1 p.Arg219Lys 23053993:45:122
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59 Out of the 17 excluded studies, two were repeated publications, seven were of review character, and six were not associated with ABCA1 R219K gene polymorphism.
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ABCA1 p.Arg219Lys 23053993:59:137
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63 Pooled analyses A significant association between ABCA1 R219K gene polymorphism and CAD was found in the Chinese population under the following genetic models: an allelic genetic model (OR 0.70, 95 % CI 0.62-0.78, P \ 0.00001), a recessive genetic model (OR 0.51, 95 % CI 0.41-0.64, P \ 0.00001), an additive genetic model (OR 0.816, 95 % CI 0780-0.855, P = 0), a dominant genetic model (OR 1.326, 95 % CI 1.232-1.427, P = 0), a homozygote genetic model (OR 0.640, 95 % CI 0.575-0.712, P = 0) and a heterozygote genetic model (OR 0.640, 95 % CI 0.575-0.712, P = 0).
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ABCA1 p.Arg219Lys 23053993:63:56
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66 The CAD group sample size (allelic genetic model, P = 0.015), KK genotype sample size of CAD group (KK1) (recessive genetic Fig. 1 Flow diagram of articles selection process for ABCA1 R219K gene polymorphism and CAD risk meta-analysis model, P = 0.014; homozygote genetic model, P = 0.014), RR genotype sample size of CAD group (RR1) (dominant genetic model, P = 0.004), and RK genotype sample size of CAD group (RK1) (heterozygote genetic model, P = 0.004) (additive genetic model, P = 0.013) possibly explained the heterogeneity.
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ABCA1 p.Arg219Lys 23053993:66:184
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70 No significant association was detected between ABCA1 R219K gene polymorphism and CAD in subgroup 1 (OR 0.85, 95 % CI 0.70-1.03, Pheterogeneity = 0.09, I2 = 58.4 %, P = 0.10.
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ABCA1 p.Arg219Lys 23053993:70:54
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76 No positive association was detected between ABCA1 R219K gene polymorphism and CAD in subgroup 1 (recessive genetic model, OR 0.78, 95 % CI 0.56-1.10, Pheterogeneity = 0.12, I2 = 53.4 %, P = 0.16) (homozygote genetic model, OR 0.812, 95 % CI 0.696-0.948, Pheterogeneity = 0.126, I2 = 51.7 %, P = 0.008).
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ABCA1 p.Arg219Lys 23053993:76:51
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81 A significant association was found between ABCA1 R219K gene polymorphism and CAD in the three subgroups (subgroup 1, OR 1.337, 95 % CI 1.199-1.491, Pheterogeneity = 0.005, I2 = 76.9 %, P = 0) (subgroup 2, OR 1.257, 95 % CI 1.081-1.462, Pheterogeneity = 0.760, I2 = 0 %, P = 0.003) (subgroup 3, OR 1.369, 95 % CI 1.198-1.564, Pheterogeneity = 0.215, I2 = 27.9 %, P = 0).
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ABCA1 p.Arg219Lys 23053993:81:50
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86 A significant association was found between ABCA1 R219K gene polymorphism Table 1 Characteristics of the investigated studies of the association between ABCA1 R291K gene polymorphism and coronary artery disease Author Year Region Ethnicity CAD Control Matching criteria Sample size (CAD/ control) P value of HWE RR RK KK RR RK KK Zhaoa 2004 Hunan Han 96 111 29 80 123 48 Age, sex, ethnicity, BMI 236/251 0.95 Lib 2005 Sichuan Han 158 174 64 124 198 95 Age, sex, ethnicity 396/417 0.35 Sunc 2005 Jiangsu Han 105 85 34 62 129 57 Ethnicity, BMI 224/248 0.52 Wangd 2006 Hebei Han 108 105 21 67 101 30 Age, sex, ethnicity, BMI 234/198 0.42 Zhae 2006 Guangdong Han 47 53 12 34 52 22 Age, sex, ethnicity 112/108 0.80 Lif 2008 Heilongjiang Han 140 170 55 92 116 38 Age, sex, ethnicity 365/246 0.89 Liug 2008 Gansu Han 29 39 3 57 60 28 Ethnicity 71/145 0.10 Wangh 2008 Zhejiang Han 85 161 75 67 155 72 Ethnicity 321/294 0.35 Yui 2008 Shanghai Han 29 18 2 24 35 13 Sex, ethnicity 49/72 0.97 Zhangj 2008 Zhejiang Han 71 65 26 49 93 44 Sex, ethnicity 162/186 0.99 Shik 2009 Hunan Han 49 60 23 53 66 38 Age, sex, ethnicity, BMI 132/157 0.54 Xial 2011 Guangxi Han 96 107 24 51 78 33 Age, sex, ethnicity, BMI 227/162 0.75 Xum 2011 Beijing Han 63 63 15 31 53 25 Ethnicity 141/109 0.80 Yuann 2011 Neimenggu Mongolian 22 28 10 16 21 18 Age, ethnicity 60/55 0.08 The polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) geno-typing method and case-control study design were adopted in all of the above studies BMI body mass index a Ref. [10], b Ref. [16], c Ref. [17], d Ref. [18], e Ref. [19], f Ref. [20], g Ref. [21], h Ref. [11], i Ref. [22], j Ref. [23], k Ref. [24], l Ref. [25], m Ref. [26], n Ref. [27] and CAD in the three subgroups (heterozygote genetic model, subgroup 1, OR 0.916, 95 % CI 0.846-0.992, Pheterogeneity = 0.365, I2 = 0.8 %, P = 0.032; subgroup 2, OR 0.804, 95 % CI 0.734-0.881, Pheterogeneity = 0.105, I2 = 51.2 %, P = 0; subgroup 3, OR 0.863, 95 % CI 0.781-0.953, Pheterogeneity = 0.119, I2 = 40.8 %, P = 0.004) (additive genetic model, subgroup 1, OR 0.906, 95 % CI 0.844-0.971, Pheterogeneity = 0.085, I2 = 59.4 %, P = 0.006; subgroup 2, OR 0.762, 95 % CI 0.702-0.829, Pheterogeneity = 0.545, I2 = 0 %, P = 0; subgroup 3, OR 0.759, 95 % CI 0.695-0.829, Pheterogeneity = 0.398, I2 = 3.7 %, P = 0) (Table 2; Figs.
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ABCA1 p.Arg219Lys 23053993:86:50
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91 Discussion In the current meta-analysis of 2,730 CAD patients and 2,658 control subjects in Chinese population, the K allele of ABCA1 R219K was significantly associated with decreased CAD risk under allelic (OR 0.70), recessive (OR 0.51), additive (OR 0.816), dominant (OR 1.326), homozygote (OR 0.640), and heterozygote genetic model (OR 0.863).
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94 The association of ABCA1 R219K gene polymorphism and Table 2 Summary of meta-analysis of association of ABCA1 R219K polymorphism and CAD risk Genetic model Group analysis Pooled OR (95 % CI) P value Literature number CAD size Control size Pheterogeneity Allelic genetic model Whole population 0.70 (0.62-0.78) \0.00001* 14 2,730 2,658 0.030* Subgroup1: T1 [ 300 0.85 (0.70-1.03) 0.100 3 1,082 957 0.090 Subgroup2: 300 [ T1 [ 200 0.65 (0.57-0.75) \0.00001* 4 921 859 0.400 Subgroup3: T1 \ 200 0.63 (0.54-0.73) \0.00001* 7 727 842 0.470 Recessive genetic model Whole population 0.51 (0.41-0.64) \0.00001* 14 2,730 2,658 0.020* Subgroup1: KK1 [ 40 0.78 (0.56-1.10) 0.160 3 1,082 957 0.120 Subgroup2: 20 \ KK1 \ 40 0.50 (0.40-0.63) \0.00001* 6 1,215 1,202 0.970 Subgroup3: KK1 \ 20 0.29 (0.19-0.43) \0.00001* 5 433 489 0.630 Dominant genetic model Whole population 1.326 (1.232-1.427) 0.000* 14 2,730 2,658 0.049* Subgroup1: RR1 [ 100 1.337 (1.199-1.491) 0.000* 4 784 707 0.005* Subgroup2: 80 \ RR1 \ 100 1.257 (1.081-1.462) 0.003* 3 1,219 1,109 0.760 Subgroup3: RR1 \ 80 1.369 (1.198-1.564) 0.000* 7 727 842 0.215 Homo genetic model Whole population 0.640 (0.575-0.712) 0.000* 14 2,730 2,658 0.016* Subgroup1: KK1 [ 40 0.812 (0.696-0.948) 0.008* 3 1,082 957 0.126 Subgroup2: 20 \ KK1 \ 40 0.575 (0.487-0.678) 0.000* 6 1,215 1,202 0.728 Subgroup3: KK1 \ 20 0.426 (0.310-0.587) 0.000* 5 433 489 0.495 Hetero genetic model Whole population 0.863 (0.819-0.908) 0.000* 14 2,730 2,658 0.046* Subgroup1: RK1 [ 150 0.916 (0.846-0.992) 0.032* 3 1,082 957 0.365 Subgroup2: 150 [ RK1 [ 70 0.804 (0.734-0.881) 0.000* 4 921 859 0.105 Subgroup3: RK1 \ 70 0.863 (0.781-0.953) 0.004* 7 727 842 0.119* Additive genetic model Whole population 0.816 (0.780-0.855) 0.000* 14 2,730 2,658 0.013* Subgroup1: RK1 [ 150 0.906 (0.844-0.971) 0.006* 3 1,082 957 0.085 Subgroup2: 150 [ RK1 [ 70 0.762 (0.702-0.829) 0.000* 4 921 859 0.545 Subgroup3: RK1 \ 70 0.759 (0.695-0.829) 0.000* 7 727 842 0.398 CI confidence interval; OR odds ratio; MI size the total number of MI cases; control size the total number of control group; homo genetic model homozygote genetic model; hetero genetic model heterozygote genetic model; T1 total CAD group sample size; KK1 KK1 genotype sample size of CAD group; RR1 RR1 genotype sample size of CAD group; RK1 RK1genotype sample size of CAD group *P \ 0.05 CAD distinctly weakened in the three studies with T1 [ 300.
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ABCA1 p.Arg219Lys 23053993:94:25
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97 The association of ABCA1 R219K gene polymorphism with CAD was also distinctly impaired in the three studies with KK1 [ 40.
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100 Results of the current meta-analysis indicated that the K allele of ABCA1 R219K gene has a protective effect on CAD risk in the Chinese population.
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112 Recent studies have Fig. 2 Forest plot of coronary artery disease associated with ATP-binding cassette transporter A1 (ABCA1) R219K polymorphism under an allelic genetic model (distribution of K allelic frequency of ABCA1 R219K gene) stratified by CAD sample size (T1) Fig. 3 Forest plot of coronary artery disease associated with ATP-binding cassette transporter A1 (ABCA1) R219K polymorphism under a recessive genetic model (KK vs. RK ?
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113 RR) stratified by KK1 genotype sample size Fig. 4 Funnel plot for studies of the association of coronary artery disease and ATP-binding cassette transporter A1 (ABCA1) R219K polymorphism under the allelic genetic model (distribution of K allelic frequency of ABCA1 R219K gene).
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118 R219K is the familiar variation of ABCA1 gene.
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119 Studies on the gene polymorphism of R219K focused on the association between atherosclerosis and lipid metabolism.
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120 The R219K mutation correlated with increased HDL-C, alleviated atherosclerosis, and decreased CAD risk [30, 31].
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122 The association of the K allele of the ABCA1 R219K gene with decreased CAD susceptibility was further verified in the current meta-analysis.
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123 In addition, the study suggests that the distribution of K allele of the ABCA1 R219K gene indicated a protective factor for CAD risk.
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127 The R219K genotype distribution, K allele frequency, and carriers were confirmed to be different among different ethnicities [32].
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133 Thus, the relationship between ABCA1 R219K gene polymorphism and CAD in the Chinese population cannot be elucidated clearly as that in the current meta-analysis even if they obtained a positive conclusion.
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135 Large-scale research on arteriosclerosis protection of R219K remains inadequate.
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137 Finally, the current meta-analysis suggested that the distribution of the K allele frequency of the ABCA1 R219K gene may protect the Chinese population from CAD risks.
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PMID: 23181436 [PubMed] Xiao Z et al: "Association studies of several cholesterol-related genes (ABCA1, CETP and LIPC) with serum lipids and risk of Alzheimer's disease."
No. Sentence Comment
35 One of the most studied ABCA1 variants is R219K (rs2230806) in exon region.
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36 Previous researches indicated the common R219K variant was associated with CSF cholesterol levels [38].
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74 The ABCA1 R219K polymorphism was investigated by using the following primers: 5'-GTA TTT TTG CAA GGC TAC CAG TTA CAT TTG ACAA-3'(forward) and 5'-GAT TGG CTT CAG GAT GTCC-3'(reverse), according to previous literure [65].
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114 For ABCA1 R219K polymorphism, there were significantly higher levels of HDL-C and apoA-I in the carriers of KK genotype and K allele (P < 0.05).
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126 There existed evident combined genotype effect of the ABCA1 R219K and the LIPC-250 G/A polymorphisms on HDL-C levels in total subjects: the carriers of the KK/AA genotype showed the highest levels of HDL-C (2.07 +/- 0.11 mmol/L), whereas those carrying the RR/GG genotype showed the lowest (1.07+/- 0.22 mmol/L) (Table 4).
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162 performed in 281 AD patients indicated that serum TC and LDL levels were clearly positively correlated with densities of neuritic plaques in both neocortex and hippocampal Table 4 Combination of ABCA1 R219K and LIPC -250 G/A variants and serum HDL-C levels(mmol/L) LIPC-250 G/A genotypes GG GA AA ABCA1 R219 K genotypes RR 1.07&#b1;0.22 1.33&#b1;0.82 1.19&#b1;0.26 RK 1.40&#b1;0.26 1.36&#b1;0.24 1.52&#b1;0.19 KK 2.02&#b1;0.66 1.70&#b1;0.40 2.07&#b1;0.11 F = 3.930 P = 0.004 Table 5 Logistic regression analysis:risk factors for AD Variable B P OR 95%CI age 0.963 0.003 2.620 1.381-4.972 education -1.052 0.004 0.349 0.172-0.710 219K allele -0.903 0.005 0.405 0.217-0.758 -250A allele -0.905 0.018 0.405 0.191-0.858 regions [77].
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ABCA1 p.Arg219Lys 23181436:162:201
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164 In this pilot study we determined an apparent association between the polymorphism of ABCA1 R219K and AD.
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169 The minor allele frequency of R219K was reported 25% in Caucasian populations [79], 46% in Europeans [65].
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181 Many conflicting results from previous studies have evaluated the associations of R219K polymorphism with level of HDL-C and risk of developing CAD [82,84,85].
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ABCA1 p.Arg219Lys 23181436:181:82
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183 In this pilot study, we first reported the association of R219K gene variants with lipids in AD patients, suggesting the possible involvement of cholesterol with AD.
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188 However, other studies failed to find any significant influence of R219K variation on HDL-C or other lipid parameters levels [85,89-91].
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220 We found a significant interaction of ABCA1 R219K and LIPC-250 G/A polymorphisms on HDL-C levels in the total subjects (F = 3.930, P = 0.004).
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267 Conclusion In summary, for the first time we reported a significant association of the ABCA1 R219K and LIPC-250A polymorphisms with sporadic AD risk and cognitive and memorial scores in Southern Chinese Han population, but no pronounced effect in CETP TaqIB SNP.
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514 Ma XY, Liu JP, Song ZY: Associations of the ATP-binding cassette transporter A1 R219K polymorphism with HDL-C level and coronary artery disease risk: a meta-analysis.
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ABCA1 p.Arg219Lys 23181436:514:80
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549 Zhao SP, Xiao ZJ, Li QZ, et al: Relationship between ATP-binding cassette transporter 1 R219K genetic variation and blood lipids.
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560 Huang Y, Wu Y, Liu R, et al: Differential effect of ATP binding cassette transporter A1 R219K and cholesteryl ester transfer protein TaqIB genotypes on HDL-C levels in overweight/obese and non-obese Chinese subjects.
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566 Li J, Wang LF, Li ZQ, et al: Effect of R219K polymorphism of the ABCA1 gene on the lipid-lowering effect of pravastatin in Chinese patients with coronary heart disease.
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PMID: 23372063 [PubMed] Villard EF et al: "Genetic determination of plasma cholesterol efflux capacity is gender-specific and independent of HDL-cholesterol levels."
No. Sentence Comment
4 The rs2230806 (ABCA1 p.R219K) SNP has been reported to be associated with HDL-C and the severity of atherosclerosis.12 The K219 allele is associated with higher plasma HDL-C and small HDL particle levels, and is proposed to be an antiatherogenic allele.13 The functional rs5082 (APOAII c.-265 T>C) SNP has been shown to be associated with coronary artery disease risk.14 Moreover, the rs1378577 (ABCG1 c.-134 T>G) SNP has been shown to modulate transcriptional activity of the human ABCG1 gene and was reported to be associated with plasma HDL-C levels in some studies, but not in others.15 The rs708272 (CETP TaqIB) SNP identified in the first intron of the CETP gene is associated with plasma CETP concentration, Received on: October 8, 2012; final version accepted on: January 10, 2013.
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10 We demonstrated that rs17231506 (CETP c.- 1337 C>T), rs2230806 (ABCA1 p.R219K), rs1799837 (APOA1 c.-75 G>A), rs5086 (APOAII c.-265 T>C), and rs1800588 (LIPC c.-514 C>T) single nucleotide polymorphisms (SNPs) significantly modulate the capacity of whole-plasma to mediate cholesterol efflux from human macrophages in a sex-dependent manner.
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12 In women, we identified the APOA1 c.-75 G>A and the LIPC c.-514 C>T variants as major contributors of interindividual variability of plasma efflux capacity, whereas the ABCA1 p.R219K and the APOAII c.-265 T>C SNPs mostly contribute to total variance of plasma efflux capacity in men.
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44 Table 2.ߓ Impact of Genetic Variants on Overall Capacity of Plasma to Mediate Cholesterol Efflux From Human THP-1 Macrophages Additive Model Recessive or Dominant Model Model 1 Model 2 Model 1 Model 2 Mean Difference r2 P Valueߤ Mean Difference r2 P Valueߤ Mean Difference r2 P Valueߤ Mean Difference r2 P Valueߤ CETP TaqIB Women 1.2 ns 1.3 ns 0.7 ns 0.8 ns Men -0.9 ns -0.9 ns -2.9 ns -3.0 ns CETP c. -1337 C>T Women -0.9 ns -0.8 ns 0.8 ns 0.8 ns Men -2.6 ns -2.6 ns -8.9 1.01 0.03 -9.8 0.90 0.03 LIPC c. -514 C>T Women 4.0 1.50 0.02 4.1 1.47 0.03 9.9 2.08 0.004ߤ 10.4 2.06 0.003ߤ Men 0.8 ns 0.6 ns 3.4 ns 3.1 ns APOA1 c. -75 G>A Women 6.0 1.77 0.003ߤ 5.8 2.22 0.004ߤ 15.1 1.67 0.005ߤ 15.3 1.91 0.004ߤ Men -4.1 ns -4.0 ns -0.5 ns -0.8 ns ABCA1 p.R219K Women -0.9 ns -0.9 ns -2.5 ns -2.7 ns Men 4.3 1.22 0.002ߤ 4.5 1.18 0.002ߤ 13.2 2.39 0.001ߤ 13.6 2.38 0.001ߤ ABCG1 c. -134 T>G Women -2.6 ns -2.7 ns -6.0 ns -6.6 ns Men 2.2 ns 2.0 ns 3.4 ns 3.6 ns APOAII c. -265 T>C Women -0.4 ns -0.4 ns -0.1# ns -0.6# ns Men 4.8 1.41 0.01 4.6* 1.37 0.03 7.4# 1.93 0.005ߤ 7.4# 1.92 0.005ߤ For each SNP, 1 indicates the most frequent allele and 2 indicates the less frequent allele.
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82 Multiple linear regression analyses including rs708272 (CETP TaqIB), rs17231506 (CETP c. -1337 C>T), rs1800588 (LIPC c. -514 C>T), rs1799837 (APOAI c. -75 G>A), rs2230806 (ABCA1 p.R219K), rs1378577 (ABCG1 c. -134 T>G), and rs5082 (APOAII c. -265 T>C) SNPs as predictive variables were performed to explain variance of plasma efflux capacity in men (left) and women (right).
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PMID: 23555974 [PubMed] Song C et al: "Genetic variants from lipid-related pathways and risk for incident myocardial infarction."
No. Sentence Comment
225 Andrikovics H, Pongracz E, Kalina E, Szilvasi A, Aslanidis C, et al. (2006) Decreased frequencies of ABCA1 polymorphisms R219K and V771M in Hungarian patients with cerebrovascular and cardiovascular diseases.
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PMID: 24084154 [PubMed] Coban N et al: "Gender specific association of ABCA1 gene R219K variant in coronary disease risk through interactions with serum triglyceride elevation in Turkish adults."
No. Sentence Comment
0 Gender specific association of ABCA1 gene R219K variant in coronary disease risk through interactions with serum triglyceride elevation in Turkish adults AddressforCorrespondence:Dr.NihanErginel-&#dc;naltuna,‚stanbul&#dc;niversitesiDeneyselTƒpAraf;tƒrmaEnstit&#fc;s&#fc;,GenetikB&#f6;l&#fc;m&#fc;, VakƒfGurebaCad.e;ehremini,‚stanbul-T&#fc;rkiye Phone:+902124142200-33324 Fax:+902125324171 E-mail:nihanerginel@yahoo.com Accepted Date: 16.07.2013 Available Online Date: 26.09.2013 (c)Copyright 2014 by AVES - Available online at www.anakarder.com doi:10.5152/akd.2013.234 Neslihan &#c7;oban, Altan Onat1, Evrim K&#f6;m&#fc;rc&#fc;-Bayrak, &#c7;a f;rƒ G&#fc;le&#e7;, G&#fc;nay Can2, Nihan Erginel-&#dc;naltuna Department of Genetics, Institute for Experimental Medical Research, ‚stanbul University; ‚stanbul-Turkey Departments of 1Cardiology and 2Public Health, Cerrahpaf;a Medical Faculty, ‚stanbul University; ‚stanbul-Turkey ABSTRACT Objective: ATP binding cassette transporter A1 (ABCA1) controls the reverse cholesterol transport.
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3 Methods: Selected 627 individuals of the Turkish Adult Risk Factor Study were genotyped for ABCA1 R219K polymorphism using PCR-RFLP (polymerase chain reaction-restriction fragment length polymorphism) method.
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5 Results: We demonstrated a gender-specific effect of the R219K polymorphism on plasma lipids and CHD.
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8 R219K heterozygosity in women independently doubled (95% CI 1.00; 3.80) the odds ratio for CHD risk in regression models, after adjustment for several variables.
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18 The K allele of the R219K polymorphism (Arg219Lys, rs2230806) has been associated with decreased triglyceride (TG) concentrations (11, 13) and increased HDL-C concentrations (9, 11, 12), consistent with a net increase in transporter function; the rare allele of the R219K, on the other hand, was found to be associated with increased risk of CHD (14).
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19 Because findings on the relationship between ABCA1 R219K polymorphism and CHD have been inconclusive, a meta-analysis was recently conducted comprising over 9400 cases and over 16.000 controls (12, 15).
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21 Among other ABCA1 polymorphisms, R219K variant`s association with HDL-C was examined by Hodo f;lugil et al. (10) on a large sample of Turkish adults, and an association was lacking in men.
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22 The KK genotype of R219K polymorphism alone showed no association with elevated HDL-C but an association was observed in combination with TT genotype of C-14T polymorphism.
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26 We, therefore, explored the role of ABCA1 gene in predisposing Turkish adults to CHD in a nested case-control study comprising 627 genotyped individuals for the R219K polymorphism.
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28 The specific aim of this study was to examine the relation of the R219K polymorphism with both the lipid concentrations and CHD in a randomly selected sample of the Turkish Adult Risk Factor Study (TARF) cohort, representative of Turkish adults (20).
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54 Genetics analysis The detection of R219K polymorphism using RFLP (restriction fragment length polymorphism) DNA was extracted from peripheral blood leukocytes using a QIAmpR DNA Maxi KIT (Qiagen, Hilden, Germany).
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55 A 243-bp fragment of exon 7 of the ABCA1 gene involving nucleotide 1051 of the DNA sequence was amplified by polymerase chain reac- tion (PCR), using the following primers: R219K Forward: 5`-tca taa tcc tct tct gct ag-3` and R219K Reverse: 5`-cag tta gca agt cta cgc a-3`.
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81 Allele and genotype distributions of ABCA1 R219K polymorphism The genotype frequencies of the ABCA1 R219K polymorphism, determined for 627 participants, disclosed the following distribution: 36.4% (n=228), 50.4% (n=316) and 13.2% (n=83) for the RR, RK and KK genotypes, respectively.
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83 Genotype distribution of the ABCA1 R219K polymorphism was in Hardy-Weinberg equilibrium for our study population.
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84 Association of the ABCA1 R219K variant with biochemical variables We examined the relationship between concentrations of biochemical variables and the R219K polymorphism of the ABCA1 gene in a total of 627 individuals (men=282, women=345).
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ABCA1 p.Arg219Lys 24084154:84:25
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87 Determination of the R219K genotype by PCR amplification and restriction analysis.
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95 In relation to TG concentration, but not to LDL-C and total cholesterol, the ABCA1 R219K polymorphism had significant gender-by-genotype interaction (p=0.049).
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102 Associations of ABCA1 R219K polymorphism with CHD risk We investigated the distribution of the clinical and biochemical characteristics of genotypes of R219K polymorphism in the CHD and there were no significant associations (data not shown).
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103 The allele and genotype frequencies of R219K polymorphism were examined in 220 cases of CHD and 407 without CHD.
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106 Frequencies of ABCA1 R219K genotypes (RR, RK and KK) were 25.5% (n=27), 64.1% (n=68) and 10.4% (n=11) in women with CHD (p=0.012) and 40.4% (n=46), 44.7% (n=51) and 14.9% (n=17) in men with CHD (p=0.53), respectively.
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107 In relation to CHD, the ABCA1 R219K polymorphism had significant gender-by-genotype interaction (p=0.009).
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108 The R219K polymorphism was found to be associated with CHD only in women using the chi-square test.
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110 Further analyses adjusted by genetic models of R219K polymor- Variables Males (n) Females (n) **P Age, years 58.9&#b1;12.8 (282) 56.7&#b1;12.3 (345) 0.03 Body mass index, kg/m2 27.7&#b1;4.4 (213) 30.6&#b1;5.9 (361) <0.001 Waist circumference, cm 96.3&#b1;11.9 (267) 94&#b1;13.7 (330) 0.037 Total cholesterol, mg/dL 184&#b1;43.8 (272) 194.5&#b1;42.5 (335) 0.003 HDL-C, mg/dL 43.3&#b1;12.7 (272) 49.7&#b1;12 (337) <0.001 LDL-C, mg/dL 107.2&#b1;34.5 (259) 111.6&#b1;34.2 (307) 0.132 Fasting triglycerides, mg/dL* 136.1&#b1;1.75 (270) 135.8&#b1;1.71 (332) 0.966 Fasting glucose, mg/dL 109.6&#b1;44.4 (259) 105.2&#b1;40.8 (330) 0.218 Apolipoprotein A-I, mg/dL 133.8&#b1;24.1 (156) 145.4&#b1;27.4 (200) <0.001 Apolipoprotein B, mg/dL 97.1&#b1;27.5 (157) 101.7&#b1;26 (204) 0.105 Systolic blood pressure, mmHg 121.0&#b1;21.9 (267) 128.2&#b1;23.6 (332) 0.01 Diastolic blood pressure, mmHg 76.6&#b1;11.7 (267) 78.8&#b1;11.9 (332) 0.026 Diabetes mellitus, %(n) 19.9 (56) 17.7 (61) 0.486 Obesity, %(n) 27.2 (58) 52.1 (136) <0.001 Coronary heart disease, %(n) 40.4 (114) 30.7 (106) 0.011 Cigarette smoking, %(n) 28.9 (77) 14.2 (47) <0.001 Alcohol usage, %(n) 10.2 (27) 1.2 (4) <0.001 Lipid-lowering medication, %(n) 9.9 (28) 10.7 (37) 0.745 Antihypertensive medication, %(n) 30.1 (85) 38.3 (132) 0.034 Medication for diabetes, %(n) 13.1 (37) 12.8 (44) 0.892 Continuous variables are presented as mean&#b1;SD and dichotomous variables as percentages.
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114 In logistic regression analysis, after adjusting for age, current smoking, alcohol usage, waist circumference, TG, systolic blood pressure and diabetes, the overdominant genetic model (RK genotype vs the RR+KK genotypes) of R219K polymorphism showed significantly higher odd ratios for CHD in women [OR 1.95 (95%CI 1.003.80, p=0.059)] (Table 4, model 1).
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117 The analysis after adjustment for the same covariates by a recessive genetic model for R219K polymorphism showed no association with CHD in women (OR=0.57, 95%CI; 0.21-1.55, p= 0.27).
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118 Discussion The ABCA1 gene R219K polymorphism, shown to be related to serum lipids, displayed a sex interaction in a nested case-control sample of Turkish adults with respect to both lipid levels and the CHD risk.
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121 Female R219K heterozygosity constituted a significant independent factor doubling the CHD risk which could be demonstrated to an interaction of the R219 allele with triglyceride elevation induced by the 219K allele.
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123 Among other ABCA1 polymorphisms, R219K variant`s association with HDL-C was examined by Hodoglugil at el. (10) on a large sample of Turkish adults, and an association was lacking in men (as well as in women in whom this was confirmed herein).
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126 p values obtained by ANCOVA for comparisons p* among R219K genotypes, p** RR genotype versus K allele carriers (RK+KK genotypes).
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127 In relation to TG (not to LDL-C and total cholesterol) concentrations; the ABCA1 R219K polymorphism had gender-by-genotype interaction (p=0.049).
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135 Interaction between ABCA1 R219K, elevated TG and sex The finding of 219K allele carriage being independently associated with higher TG concentration in women can be accounted for by serum TG being strong independent covariate of total phospholipids (30) and the knowledge that dietary long-chain polyunsaturated fatty acids arachidonic acid and docosahexaenoic acid contribute to plasma phospholipids more in women than men, and mainly in populations with low dietary n-3 fatty acid intake (30, 31) to which Turks belong.
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142 On the other hand, Villard et al. (35) reported that R219K polymorphism significantly modulates the capacity of whole-plasma to mediate cholesterol efflux from human macrophages in a sex-dependent manner.
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143 Furthermore, Villard et al. (35) demonstrated impact of the R219K on plasma total cholesterol, LDL-C and Apo A-I concentrations but not HDL-C and TG concentrations in men or women subjects.
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146 A recent meta-analysis demonstrated ethnic differences in the protective and risk conferring alleles of the ABCA1 R219K polymorphism for CHD (12).
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151 In relation to CHD, the ABCA1 R219K polymorphism had significant gender-by-genotype interaction (p=0.009).
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155 Multiple logistic regression analysis for the adjusted association of ABCA1 R219K variant with CHD in men and women According to a proposed a novel hypothesis on systemic inflammation, oxidized phospholipids and fatty acids metabolized from arachidonic acid affect endothelial and small intestinal cells to induce cytokines that influence macrophages or hepatocytes (37).
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158 Thus, inflammation and oxidized phospholipids are closely linked to ABCA1 R219K polymorphism, gender and CHD risk.
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160 Focusing on the effect of ABCA1 R219K polymorphism, without assessing the combined effect of other interacting genetic factors on analyses might limit the interpretation of our study.
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167 Genotyping for the ABCA1 R219K polymorphism might yield practical benefit in prevention.
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168 Conclusion In conclusion, R219K polymorphism as a common ABCA1 variant influences lipid concentrations and the CHD risk gender-specifically among Turkish adults.
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PMID: 24157307 [PubMed] Hou R et al: "ATP-binding cassette transporter A1 R219K polymorphism and ischemic stroke risk in the Chinese population: a meta-analysis."
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0 ATP-binding cassette transporter A1 R219K polymorphism and ischemic stroke risk in the Chinese population: A meta-analysis Rongyao Hou a,1,2 , Xiaoyan Zhu b,1,2 , Xudong Pan c, Ìe;,2 , Ruiyou Guo a , Teng Ma a , Xiang Xu c a Department of Neurology, The Affiliated Hiser Hospital of Qingdao University, Qingdao, China b Department of Critical Care Medicine, The Affiliated Hiser Hospital of Qingdao University, Qingdao, China c Department of Neurology, The Affiliated Hospital of Qingdao University, Qingdao, China a b s t r a c t a r t i c l e i n f o Article history: Received 16 July 2013 Received in revised form 13 September 2013 Accepted 3 October 2013 Available online 12 October 2013 Keywords: ATP-binding cassette transporter A1 (ABCA1) Gene polymorphism The Chinese population Ischemic stroke Meta analysis R219K Recently, many studies have been focused on the association between the ATP-binding cassette transporter A1 (ABCA1) gene R219K polymorphism and ischemic stroke (IS).
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4 Odds ratios with 95% confidence intervals were applied to evaluate the strength of the association between ABCA1 gene R219K polymorphism and IS.
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ABCA1 p.Arg219Lys 24157307:4:118
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7 For R219K in IS, there were significant associations with these genetic models, but not with the recessive genetic model.
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8 Our meta-analysis indicated that the ABCA1 gene R219K polymorphism might be associated with IS and the K allele might be a protective factor in the Chinese population.
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30 R219K is a common variation in the ABCA1 gene-coding region.
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38 One study found that the ABCA1 R219K polymorphism cloud modulate the association between HDL-C and age in whites [17].
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39 Another study also found that the ABCA1 R219K polymorphism was associated with a higher HDL-C level in Caucasians and Asians [14].
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40 Domestically, results of the widely researched studies of ABCA1 R219K gene polymorphism and IS are still debatable.
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43 To illustrate inconsistencies, we collected the data from the relevant published literature to quantify the ABCA1 R219K polymorphism effect on the risk of IS in the Chinese population.
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47 The following medical subject heading (MeSH) terms were used: "cerebrovascular accident," "cerebrovascular disease," "stroke," "cerebral infarct," "polymorphism,""ABCA1,""R219K"and "the Chinese population".
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50 Selection criteria The included studies were all selected according to the following criteria: (1) studies that related the R219K polymorphism to susceptibility to IS; (2) studies restricted to the Chinese population; (3) a clear diagnosis for IS; (4) applied case-control studies and (5) full-text articles.
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77 Meta-regression testing can explain Records identified through database searching (n = 38) Articles excluded: Obvious irrelevance (n = 12) Articles screened ( n = 26) Articles excluded: Without Chinese population included (n = 3) Without SNP R219K (n = 6) No case-control studies (n = 2) Duplicated publications (n = 2) No genotype frequency (n = 1) Other not according with standards of research (n = 3) Full-text articles assessed for eligibility (n = 9) No full-text articles excluded Studies included in the meta-analysis (n=9) Fig. 1.
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90 Discussion The association remains controversial between the R219K polymorphism of ABCA1 and IS in many studies, especially in the Chinese population. Therefore, this meta-analysis was very necessary to evaluate the association.
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94 It showed that the dominant genetic model (OR = 0.92, 95% CI: 0.88-0.96, P = 0.000), the homozygote genetic model (OR = 0.64, 95% CI: 0.44-0.94, P = 0.02), the heterozygote genetic model (OR = 0.81, 95% CI: 0.69-0.95, P = 0.009) and the allelic genetic model (OR = 0.83,95% CI:0.69-0.99, P = 0.036) indicated a significant association between R219K polymorphism and IS.
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102 Results of the current meta-analysis indicated the R219K polymorphism of ABCA1 gene might be associated with IS and that the K allele might be a protective factor for IS in the Chinese populations.
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107 Studies on the polymorphism of R219K have focused on the association between AS and lipid metabolism.
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108 Many of those studies focused on the association about R219K gene polymorphism in AS, coronary heart disease (CHD) and IS [14,15,24].
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109 The R219K gene polymorphism correlated with increasing HDL-C, alleviating atherosclerosis and decreasing CHD risk, and described the protective effect against AS and CHD [31,32].
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111 Other studies also showed that R219K polymorphism of the ABCA1 gene had a protective effect against IS [18,24].
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ABCA1 p.Arg219Lys 24157307:111:31
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115 Another study didn't support the ABCA1 R219K polymorphism played a major role among the risk factors of IS [35].
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117 In our meta-analysis, the ABCA1 R219K polymorphism might be associated with IS and the K allele maybe a protective factor against IS in the Chinese population.
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119 Table 2 Summary of meta-analysis of association of ABCA1 R219K polymorphism and IS risk.
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131 [25] 2012 Ningxia Chinese (Hui) Age, sex, ethnicity PCR-RFLP 105/257 30 63 12 63 125 69 0.669 The reasons for the ABCA1 R219K polymorphism reducing the risk of IS might be the reduction in the incidence of AS.
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ABCA1 p.Arg219Lys 24157307:131:122
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133 The studies of R219K gene polymorphism associated with CHD also found that the R219K polymorphism and CHD were closely related, and that the K allele might be a genetic protective factor [31,32].
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ABCA1 p.Arg219Lys 24157307:133:79
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134 The R219K polymorphism was significantly associated with HDL-C metabolism and CHD risk [36].
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ABCA1 p.Arg219Lys 24157307:134:4
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136 R219K polymorphism of the ABCA1 gene is associated with susceptibility to IS.
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ABCA1 p.Arg219Lys 24157307:136:0
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137 The above literature was not consistent regarding the risk of the ABCA1 gene R219K polymorphism in the development of IS.
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ABCA1 p.Arg219Lys 24157307:137:77
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154 In conclusion, our meta-analysis indicated that the ABCA1 gene R219K polymorphism might be associated with IS and that the K allele might be a protective factor for IS in the Chinese population.
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ABCA1 p.Arg219Lys 24157307:154:63
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156 In the future, more well-designed research is needed to evaluate the association between the ABCA1 R219K polymorphism and IS.
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PMID: 24466114 [PubMed] Yin YW et al: "Influence of ATP-binding cassette transporter 1 R219K and M883I polymorphisms on development of atherosclerosis: a meta-analysis of 58 studies."
No. Sentence Comment
1 , Dong Gao1 , Yan-Xiu Chen2 , Bing-Hu Li1 , Jing-Zhou Wang1 , Yun Liu1 , Shao-Qiong Liao1 , Ming-Jie Zhang1 , Chang-Yue Gao1 , Li-Li Zhang1 * 1 Department of Neurology, Institute of Surgery Research, Daping Hospital, Third Military Medical University, Yuzhong District, Chongqing, PR China, 2 Department of Neurology, The brain hospital of Liaocheng Hospital, Liaocheng, Shandong, PR China Abstract Background: Numerous epidemiological studies have evaluated the associations between ATP-binding cassette transporter 1 (ABCA1) R219K (rs2230806) and M883I (rs4149313) polymorphisms and atherosclerosis (AS), but results remain controversial.
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6 For the ABCA1 R219K polymorphism, 42 studies involving 12,551 AS cases and 19,548 controls were combined showing significant association between this variant and AS risk (for K allele vs. R allele: OR = 0.77, 95% CI = 0.71-0.84, P,0.01; for K/K vs. R/R: OR = 0.60, 95% CI = 0.51-0.71, P,0.01; for K/K vs. R/K+R/R: OR = 0.69, 95% CI = 0.60-0.80, P,0.01; for K/K+R/K vs. R/R: OR = 0.74, 95% CI = 0.66-0.83, P,0.01).
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9 Conclusions: The present meta-analysis suggested that the ABCA1 R219K and M883I polymorphisms were associated with the susceptibility to AS.
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11 Citation: Yin Y-W, Li J-C, Gao D, Chen Y-X, Li B-H, et al. (2014) Influence of ATP-Binding Cassette Transporter 1 R219K and M883I Polymorphisms on Development of Atherosclerosis: A Meta-Analysis of 58 Studies.
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28 Recently, a number of molecular epidemiological studies have been done to evaluate the associations between the ABCA1 gene polymorphisms (such as R219K, M883I, C69T, V825I, R1587K, V771M and 2565C/T) and the risk of atherosclerotic diseases [248].
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30 In 2011, Ma et al. performed a meta-analysis to evaluate the association between the ABCA1 R219K polymorphism and coronary artery disease (CAD), and demonstrated that the ABCA1 R219K polymorphism was a protective role for CAD both in Asians and Caucasians [53].
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32 However, they just found the ABCA1 R219K polymorphism was a protective factor in Asians, but not in Caucasians.
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33 Considering the above two meta-analyses only focused on the association of ABCA1 R219K polymorphism with the single atherosclerotic disease, we therefore performed this meta-analysis of all the studies available now to derive a more precise estimation of the associations between the ABCA1 R219K and M883I polymorphisms and overall AS risk.
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41 Inclusion and Exclusion Criteria To be included in the present meta-analysis, the studies had to comply with the following major criteria: (1) case-control or cohort studies evaluating the associations between the ABCA1 R219K and M883I polymorphisms and AS risk; (2) published studies with full text articles; (3) Diagnosises of atherosclerotic diseases were made according to the internationally recognized diagnostic criterion.
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54 The strength of associations between the ABCA1 R219K and M883I polymorphisms and AS risk were assessed by ORs with 95% CIs.
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55 The pooled ORs were performed for allelic model (K allele vs. R allele for R219K; I allele vs. M allele for M883I), additive model (K/K vs. R/R for R219K; I/I vs. M/M for M883I), recessive model (K/K vs. R/K+R/R for R219K; I/I vs. M/I+M/M for M883I), and dominant model (K/K+R/K vs. R/R for R219K; I/I+M/I vs. M/M for M883I).
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66 After careful review, 47 articles involving 58 studies (42 studies for R219K polymorphism and 16 studies for M883I polymorphism) met the inclusion criteria and were selected in this meta-analysis [2-48].
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67 For the ABCA1 R219K polymorphism, 12551 AS cases and 19548 controls were included to assess the association between the variant and AS risk [2-41].
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76 Quantitative Synthesis For the ABCA1 R219K polymorphism, 42 studies were combined.
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77 The overall results showed evidence of significant association between the ABCA1 R219K polymorphism and the susceptibility to AS, suggesting that the ABCA1 R219K polymorphism was a protective role for AS (for K allele vs. R allele: OR = 0.77, 95% CI = 0.71-0.84, P,0.01; for K/K vs. R/R: OR = 0.60, 95% CI = 0.51-0.71, P,0.01; for K/K vs. R/K+R/ R: OR = 0.69, 95% CI = 0.60-0.80, P,0.01; for K/K+R/K vs. R/R: OR = 0.74, 95% CI = 0.66-0.83, P,0.01).
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88 Overall, the corresponding pooled ORs were not materially altered, either for the ABCA1 R219K polymorphism or for M883I polymorphism.
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91 Heterogeneity Analysis For the ABCA1 R219K polymorphism, significant heterogeneity existed in the overall comparisons (for allelic model: PQ,0.01, I2 = 77.4%; for additive model: PQ,0.01, I2 = 67.9%; for recessive model: PQ,0.01, I2 = 64.2%; for dominant model: PQ,0.01, I2 = 69.7%).
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95 For the ABCA1 R219K polymorphism, heterogeneity can be explained by the subtype of atherosclerotic diseases (allelic model: PT2 = 0.013, additive model: PT2 = 0.034, and recessive model: PT2 = 0.017) and study type (dominant model: PT4 = 0.037).
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101 For the ABCA1 R219K polymorphism, visual inspection of the funnel plot (Fig. 4: K allele vs. R allele) displays asymmetrical distribution of OR estimations, suggesting significant publication bias.
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ABCA1 p.Arg219Lys 24466114:101:14
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105 In addition to the above analyses, we also calculated the Nfs (for the ABCA1 R219K polymorphism, Nfs = 133 for allelic model, Nfs = 146 for additive model, Nfs = 75 for recessive model, and Nfs = 49 for dominant model; for the ABCA1 M883I polymorphism, Nfs = 50 for allelic model), which reflected the minimum number of non-significant studies that would lead to the P-value to non-significant (P.0.05).
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106 Discussion To the best of our knowledge, this is the first comprehensive meta-analysis to date investigating the associations between the ABCA1 R219K and M883I polymorphisms and AS risk.
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107 Forty-two studies investigating the association between the ABCA1 R219K polymorphism and AS risk were combined [241], and 16 studies investigating the association between the ABCA1 M883I polymorphism and AS risk were combined Figure 1.
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111 Study Source of Sample size HWE Position First author Year Country Ethnicity type Disease controls (case/ control) Genotypes distribution (case/control) Y/N(P) Score R219K R/R R/K K/K R K Clee 2001 Canada Caucasians CS CAD HB 432/358 248/176 170/160 14/22 666/512 198/204 Y(0.067) 6 Brousseau 2001 USA Caucasians CCS CAD PB 1014/1013 454/543 484/402 76/68 1392/1488 636/538 Y(0.580) 7 Cenarro 2003 Spain Caucasians CCS CAD HB 216/158 123/72 78/71 15/15 324/215 108/101 Y(0.676) 6 Evans 2003 Germany Caucasians CCS CAD HB 114/629 72/337 35/245 7/47 179/919 49/339 Y(0.789) 7 Harada 2003 Japan Asian CCS CAD HB 273/137 73/31 139/73 61/33 285/135 261/139 Y(0.440) 6 Wang 2004 China Asian CCS CAD PB 222/278 79/76 94/125 49/77 252/277 192/279 Y(0.093) 7 Zhao 2004 China Asian CCS CAD PB 236/251 96/80 111/123 29/48 303/283 169/219 Y(0.953) 8 Wang-a 2004 China Asian CCS IS PB 58/60 23/21 27/34 8/5 73/76 43/44 Y(0.088) 7 Wang-b 2004 China Asian CCS IS PB 58/60 19/14 35/36 4/10 73/64 43/56 Y(0.112) 7 Xiao 2004 China Asian CCS IS PB 379/351 149/112 172/172 58/67 470/396 288/306 Y(0.947) 8 Woll 2005 USA Caucasians CCS CAD PB 838/257 450/115 327/112 61/30 1227/342 449/172 Y(0.732) 6 Cui 2005 China Asian CCS IS PB 96/90 15/21 35/45 46/24 65/87 127/93 Y(0.992) 7 Whiting 2005 USA Mixed CS CAD HB 2468/834 1298/449 975/318 195/67 3571/1216 1365/452 Y(0.313) 6 Sun 2005 China Asian CCS CAD PB 224/248 105/62 85/129 34/57 295/253 153/243 Y(0.521) 8 Li 2005 China Asian CCS CAD PB 264/278 104/83 116/132 44/63 324/298 204/258 Y(0.449) 7 Chang 2005 China Asian CCS CAD PB 178/83 66/17 75/22 37/44 207/56 149/110 N(0.000) 7 Wang 2006 China Asian CCS CAD PB 396/417 158/124 174/198 64/95 490/446 302/388 Y(0.350) Wang 2006 China Asian CCS CAD HB 150/139 61/47 69/53 20/39 191/147 109/131 N(0.006) 6 Wang 2006 China Asian CCS CAD PB 234/198 108/67 105/101 21/30 321/235 147/161 Y(0.422) 8 Cha 2006 China Asian CCS CAD PB 112/108 47/34 53/52 12/22 147/120 77/96 Y(0.795) 7 Wu 2006 China Asian CCS CAD PB 67/20 26/2 30/7 11/11 82/11 52/29 Y(0.585) 6 Martƒ &#b4;n 2006 Spain Caucasians CS MI HB 100/100 48/49 42/40 10/11 138/138 62/62 Y(0.516) 6 Andrikovics -a 2006 Hungary Caucasians CCS IS PB 244/193 131/97 84/73 29/23 346/267 142/119 Y(0.116) 7 Andrikovics -b 2006 Hungary Caucasians CCS CAD PB 150/193 84/97 55/73 11/23 223/267 77/119 Y(0.116) 7 Yu 2008 China Asian CCS MI PB 49/72 29/24 18/35 2/13 76/83 22/61 Y(0.969) 7 Zhang 2008 China Asian CCS IS PB 177/234 43/40 87/129 47/65 173/209 181/259 Y(0.078) 7 Wang 2008 China Asian CCS CAD HB 111/75 30/17 54/41 27/17 114/75 108/75 Y(0.419) 6 Zhang 2008 China Asian CCS MI PB 162/186 71/49 65/93 26/44 207/191 117/181 Y(0.992) 8 Balcerzyk 2008 Poland Caucasians CCS CAD PB 178/180 90/91 68/78 20/11 248/260 108/100 Y(0.283) 6 Frikke-Schmidt 2008 Denmark Caucasians CS CAD PB 1107/7858 603/4260 429/3032 75/566 1635/ 11552 579/4164 Y(0.405) 7 Porchay-Balde &#b4;relli 2009 France Caucasians CS CAD HB 223/2906 106/1491 102/1183 15/232 314/4165 132/1647 Y(0.901) 6 Li 2009 China Asian CCS CAD PB 365/246 140/92 170/116 55/38 450/300 280/192 Y(0.886) 8 Shi 2009 China Asian CCS CAD HB 132/157 49/53 60/66 23/38 158/172 106/142 Y(0.058) 7 Doosti 2009 Iran Asian CCS CAD HB 207/94 71/17 77/38 59/39 219/72 195/116 Y(0.161) 6 Guo 2010 China Asian CCS CAD PB 71/83 30/29 37/38 4/16 97/96 45/70 Y(0.576) 7 Xu 2011 China Asian CCS CAD PB 246/109 95/31 128/53 23/25 318/115 174/103 Y(0.798) 8 Yuan 2011 China Asian CCS CAD PB 60/55 22/16 28/21 10/18 72/53 48/57 Y(0.081) 7 Yi 2011 China Asian CCS IS PB 240/240 36/45 97/109 107/86 169/199 311/281 Y(0.319) 7 Xue 2012 China Asian CCS CAA, IS PB 182/229 70/62 91/118 21/49 231/242 133/216 Y(0.608) 8 Wang 2012 China Asian CCS CAD PB 141/109 63/31 63/53 15/25 189/115 93/103 Y(0.798) 7 Li 2012 China Asian CCS MI PB 150/100 52/30 74/48 24/22 178/108 122/92 Y(0.735) 7 Xia 2012 China Asian CCS CAD HB 227/162 96/51 107/78 24/33 299/180 155/144 Y(0.750) 6 [14,15,22,23,29,30,42-48].
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112 According to the GRADE approach, the quality of the evidence was very low in the ABCA1 R219K polymorphism.
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114 The overall findings showed that the ABCA1 R219K and M883I polymorphisms may exert an reduced risk effect on AS.
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115 For the ABCA1 R219K polymorphism, the risk of developing AS in R allele carriers was 1.30-fold higher than those without R allele.
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118 Therefore, it is reasonable to assume that the ABCA1 R219K K allele and M883I I allele are the protective factors for the development of AS.
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120 For the ABCA1 R219K polymorphism, significant associations were found between this variant and the susceptibility to AS in the Asians group, CAD group, population-based group, hospital-based group and the subgroup of case-control study, respectively.
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121 These results further strengthened the conclusion that the ABCA1 R219K K allele was a protective factor for AS.
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137 For Caucasians, we did not find significant association between the ABCA1 R219K and M883I polymorphisms and AS risk.
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138 In fact, the minor allele frequencies (MAF) of ABCA1 R219K and M883I are low among utah residents with Northern and Western European ancestry (CEU) (MAF = 0.210 and 0.133 in HapMap CEU) [64].
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139 However, the ABCA1 R219K and M883I polymorphisms are common among Han Chinese in Beijing, China (CHB) and Japanese in Tokyo, Japan (JPT) (MAF = 0.453/0.434 and 0.255/0.438, respectively) [64].
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145 As for the ABCA1 R219K polymorphism, the corresponding pooled ORs were not materially altered in all comparisons.
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147 Meta-analyses of ABCA1 R219K and M883I polymorphisms and risk of AS in each subgroup.
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148 Allelic model Additive model Recessive model Dominant model Position SS (case/control) OR (95% CI) P value OR (95% CI) P value OR (95% CI) P value OR (95%CI) P value Overall analysis R219K 12551/19548 0.77[0.71,0.84] ,0.01 0.60[0.51,0.71] ,0.01 0.69[0.60,0.80] ,0.01 0.74[0.66,0.83] ,0.01 M883I 4224/13462 0.85[0.77,0.95] ,0.01 0.79 [0.61,1.01] 0.06 0.92[0.74,1.13] 0.42 0.86[0.72,1.02] 0.08 Subgroup analysis based on ethnicity R219K (C) 4616/13845 0.91[0.80,1.04] 0.16 0.83[0.65,1.06] 0.14 0.87[0.72,1.05] 0.14 0.90[0.76,1.07] 0.23 R219K (A) 7935/5703 0.71[0.64,0.79] ,0.01 0.52[0.42,0.63] ,0.01 0.62[0.52,0.75] ,0.01 0.66[0.59,0.74] ,0.01 M883I (C) 2067/11556 0.94[0.78,1.12] 0.48 1.24[0.67,2.29] 0.50 1.29[0.70,2.38] 0.41 1.05[0.86,1.28] 0.66 M883I (A) 2157/1906 0.82[0.72,0.93] ,0.01 0.72[0.54,0.95] 0.02 0.88[0.70,1.09] 0.25 0.75[0.61,0.91] ,0.01 Subgroup analysis based on type of diseases R219K (CAD) 11117/18091 0.74[0.67,0.82] ,0.01 0.56[0.47,0.67] ,0.01 0.64[0.55,0.74] ,0.01 0.72[0.64,0.82] ,0.01 R219K (IS) 1434/1457 0.94[0.75,1.17] 0.58 0.86[0.55,1.35] 0.51 1.00[0.69,1.45] 1.00 0.82[0.65,1.02] 0.08 M883I (CAD) 3890/13257 0.82[0.74,0.90] ,0.01 0.73[0.57,0.94] 0.01 0.88[0.71,1.09] 0.24 0.81[0.68,0.97] 0.02 M883I (IS) 334/205 1.43[1.02,2.02] 0.04 2.79[0.95,8.21] 0.06 2.51[0.86,7.29] 0.09 1.40[0.94,2.07] 0.10 Subgroup analysis based on source of controls R219K (PB) 7898/13799 0.76[0.67,0.85] ,0.01 0.58[0.47,0.72] ,0.01 0.68[0.56,0.82] ,0.01 0.72[0.62,0.83] ,0.01 R219K (HB) 4653/5749 0.81[0.71,0.92] ,0.01 0.65[0.51,0.82] ,0.01 0.72[0.59,0.87] ,0.01 0.80[0.68,0.94] ,0.01 M883I (PB) 3612/10285 0.87[0.78,0.97] 0.01 0.77[0.58,1.04] 0.09 0.91[0.73,1.13] 0.39 0.86[0.72,1.04] 0.11 M883I (HB) 612/3177 0.75[0.52,1.08]a 0.13 0.93[0.45,1.90] 0.84 1.02[0.50,2.09] 0.95 0.88[0.51,1.55] 0.67 Subgroup analysis based on study type R219K (CS) 4330/12056 0.97[0.88,1.07] 0.55 0.91[0.75,1.10] 0.32 0.91[0.76,1.07] 0.25 0.99[0.87,1.12] 0.84 R219K (CCS) 8221/7492 0.74[0.67,0.82] ,0.01 0.57[0.47,0.68] ,0.01 0.67[0.57,0.78] ,0.01 0.70[0.62,0.79] ,0.01 M883I (CS) 1673/11346 0.87[0.71,1.08] 0.21 1.05[0.54,2.04] 0.89 1.10[0.56,2.14] 0.78 1.04[0.80,1.36] 0.77 M883I (CCS) 2551/2116 0.85[0.75,0.97] 0.01 0.75[0.56,1.02] 0.06 0.90[0.72,1.12] 0.34 0.79[0.65,0.95] 0.01 Sensitivity analysis R219K (BS) 7061/14128 0.76[0.68,0.85] ,0.01 0.60[0.49,0.73] ,0.01 0.69[0.58,0.82] ,0.01 0.72[0.62,0.83] ,0.01 R219K (BH) 12223/19326 0.79[0.72,0.86] ,0.01 0.62[0.53,0.74] ,0.01 0.73[0.64,0.83] ,0.01 0.75[0.67,0.84] ,0.01 R219K (BT) 11647/18669 0.78[0.71,0.85] ,0.01 0.60[0.51,0.71] ,0.01 0.70[0.61,0.80] ,0.01 0.74[0.66,0.83] ,0.01 M883I (BS) 3255/10125 0.87[0.77,0.99] 0.03 0.77[0.54,1.10] 0.16 0.90[0.71,1.16] 0.42 0.87[0.71,1.05] 0.15 M883I (BH) 3571/13041 0.88[0.79,0.98] 0.02 0.80[0.58,1.10] 0.17 0.92[0.73,1.15] 0.44 0.84[0.71,0.98] 0.03 M883I (BT) 3870/13084 0.84[0.76,0.92] ,0.01 0.75[0.58,0.95] 0.02 0.89[0.72,1.10] 0.29 0.85[0.71,1.01] 0.07 A: Asians, C: Caucasians, PB: population-based, HB: hospital-based.
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156 Significant heterogeneity existed in the present meta-analysis, either for the ABCA1 R219K polymorphism or for the ABCA1 M883I polymorphism.
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ABCA1 p.Arg219Lys 24466114:156:85
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158 For the ABCA1 R219K polymorphism, the heterogeneity can be explained by the subtype of atherosclerotic diseases (CAD and IS) and study type (case-control and cohort study).
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168 Forest plot for ABCA1 R219K polymorphism and AS risk in the allelic model (K allele vs. R allele).
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172 Funnel plots for ABCA1 R219K and M883I polymorphisms and AS risk.
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173 K allele vs. R allele for ABCA1 R219K polymorphism.
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ABCA1 p.Arg219Lys 24466114:173:32
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179 In conclusion, the present meta-analysis suggested that the ABCA1 R219K and M883I polymorphisms were associated with the susceptibility to AS, especially in Asians.
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ABCA1 p.Arg219Lys 24466114:179:66
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182 Supporting Information Figure S1 Forest plot for ABCA1 R219K polymorphism and AS risk in the additive model (K/K vs. R/R).
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ABCA1 p.Arg219Lys 24466114:182:55
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183 (TIF) Figure S2 Forest plot for ABCA1 R219K polymorphism and AS risk in the rssive model (K/K vs. R/K+R/R).
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ABCA1 p.Arg219Lys 24466114:183:38
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184 (TIF) Figure S3 Forest plot for ABCA1 R219K polymorphism and AS risk in the dominant model (K/K+R/K vs. R/R).
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ABCA1 p.Arg219Lys 24466114:184:38
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190 (DOC) Table S3 The meta-regression results for the association of the ABCA1 R219K polymorphism and AS.
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PMID: 24649047 [PubMed] Zargar S et al: "Involvement of ATP-binding cassette, subfamily A polymorphism with susceptibility to coronary artery disease."
No. Sentence Comment
39 The presence of SNP rs2230806 (R219K variant) in exon 7 of the ABCA1 gene (c.969A࢐G) was determined for each sample.
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40 The presence of the missense mutation at nucleotide 969 (AGG to AAG), which leads to the replacement of arginine with lysine at codon 219, was evaluated in genomic DNA by polymerase chain reaction (PCR)ߛRFLP analysis, according to methods described by Cook et al (17).
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75 There was no significant difference in the correlation between age and HDL and triglyceride levels in individuals carrying different rs2230806 (R219K) genotypes (data not shown).
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ABCA1 p.Arg219Lys 24649047:75:144
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108 In a subset of the samples, sequencing was used to validate the GG, AA and GA genotypes of the R219K polymorphism that were identified by RFLP (Fig. 1).
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ABCA1 p.Arg219Lys 24649047:108:95
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112 We also observed an association between triglyceride levels and the R219K polymorphism, but no significant associations were observed for other lipid parameters.
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ABCA1 p.Arg219Lys 24649047:112:68
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113 The most common missense polymorphism in the coding region of the ABCA1 gene is R219K, with an allelic frequency of 25ߛ46% in the Caucasian population.
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114 Two large studies including 2,028 and 794 individuals resulted in contradictory conclusions regarding the possible role of rs2230806 (R219K) in arteriosclerosis.
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ABCA1 p.Arg219Lys 24649047:114:134
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115 One study reported an elevated R219K allelic frequency in patients with CHD and a low HDL level compared to diseaseߛfree individuals, suggesting that the mutant allele is likely associated with decreased HDL levels, the promotion of arteriosclerosis and the subsequent development of CHD (11).
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116 The other study reported a decreased R219K allelic frequency in patients with CHD in conjunction with high observed levels of HDL, suggesting that the mutant allele conferred a protective effect (22).
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122 In this study, we observed a correlation between the R219K allele and lipid parameters, although the observed associations were not very significant, except for the associations with HDLߛC levels (P=0.02).
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PMID: 24844148 [PubMed] Koldamova R et al: "ATP-binding cassette transporter A1: from metabolism to neurodegeneration."
No. Sentence Comment
978 R219K (rs2230806), I883M (rs4149313), and R1587K (rs2230808) are the non-synonymous variants most extensively investigated since they translate into amino acid changes and have been shown to associate with the risk for CAD.
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ABCA1 p.Arg219Lys 24844148:978:0
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PMID: 24854628 [PubMed] Akao H et al: "ABCA1 gene variation and heart disease risk reduction in the elderly during pravastatin treatment."
No. Sentence Comment
0 ABCA1 gene variation and heart disease risk reduction in the elderly during pravastatin treatmentq Hironobu Akao a,b,1 , Eliana Polisecki a,c,1 , Ernst J. Schaefer a,c , Stella Trompet d,e , Michele Robertson f , Ian Ford f , J. Wouter Jukema d,e , Anton J.M. de Craen d,e , Christopher Packard g , Brendan M. Buckley h , Kouji Kajinami b,*, on behalf of the PROspective Study of Pravastatin in the Elderly at Risk (PROSPER) Investigator a Lipid Metabolism Laboratory, Jean Mayer USDA Human Nutrition Research Center on Aging at Tufts University and Tufts University School of Medicine, Boston, MA, USA b Department of Cardiology, Kanazawa Medical University, Uchinada, Japan c Boston Heart Diagnostics, Framingham, MA, USA d Department of Cardiology, Leiden University Medical Centre, Leiden, The Netherlands e Department of Gerontology, and Geriatrics, Leiden University Medical Centre, Leiden, The Netherlands f Robertson Centre of Biostatistics, University of Glasgow, Glasgow, Scotland, UK g Department of Vascular Biochemistry, University of Glasgow, Glasgow, Scotland, UK h Department of Pharmacology and Therapeutics, University College Cork, Cork, Ireland a r t i c l e i n f o Article history: Received 17 January 2014 Received in revised form 17 April 2014 Accepted 25 April 2014 Available online 8 May 2014 Keywords: ABCA1 gene Statins Low-density lipoprotein cholesterol lowering response Heart disease risk reduction a b s t r a c t Aims: Our goals were to examine the relationships of a specific ATP-binding cassette transporter A1 (ABCA1) variant, rs2230806 (R219K), on baseline lipids, low-density lipoprotein cholesterol (LDL-C) lowering due to pravastatin, baseline heart disease, and cardiac endpoints on trial.
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1 Methods and results: The ABCA1 R219K variant was assessed in 5414 participants in PROSPER (PROspective Study of Pravastatin in the Elderly at Risk) (mean age 75.3 years), who had been randomized to pravastatin 40 mg/day or placebo and followed for a mean of 3.2 years.
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6 Conclusion: Our data indicate that subjects with the ABCA1 R219K variant may get significantly less heart disease risk reduction from pravastatin treatment than those without the variant.
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29 The most studied variant at the ABCA1 gene locus is the R219K variant which causes an amino substitution in which an arginine is replaced by a lysine at amino acid position 219 in the ABCA1 protein [11].
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30 It has been previously reported that individuals carrying the R219K variant (found in 46% of a population of 790 subjects) had significantly lower triglyceride levels, slightly higher HDL-C levels, and significantly reduced severity of CHD as compared to non-carriers [12].
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32 Subsequently it was reported that the presence of the R219K ABCA1 variant in patients with familial hypercholesterolemia (n &#bc; 374) was associated with a markedly reduced risk of CHD (hazards ratio 0.32, p < 0.001) as compared to non-carriers [13].
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33 A recent meta-analysis based on an examination of 6597 CHD cases and 15,369 controls concluded that the presence of the R219K ABCA1 variant was associated with a lower risk of CHD (hazards ratio 0.76, p < 0.0001), and modestly higher HDL-C levels [14].
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ABCA1 p.Arg219Lys 24854628:33:120
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34 However, there are no studies to our knowledge that have assessed whether the R219K ABCA1 genetic variant affects responses to statin treatment in terms of lipid modification or CHD risk reduction.
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35 Our goals in this study were to determine whether the ABCA1 variant rs2230806 or R219K in PROSPER participants would affect baseline lipids, CHD prevalence at baseline, pravastatin induced LDL-C lowering, and pravastatin mediated CHD risk reduction.
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48 For DNA analysis the single nucleotide polymorphism (SNP), R219K (rs2230806) of the ABCA1 gene was genotyped using Taq Man&#d2; SNPs genotyping assays (Applied Biosystems, Foster City, CA).
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63 There was no interaction between R219K and apoE phenotype.
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78 Associations with lipid response to treatment To determine whether the R219K variant affected lipid responses to pravastatin, the association between the R219K variant under study and 6 month and 12 month changes in TC, LDL-C, HDL-C, and triglyceride levels in individuals treated with pravastatin or placebo were examined.
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ABCA1 p.Arg219Lys 24854628:78:71
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81 Associations with history and within trial incidence of cardiovascular disease There were no significant associations between the prevalence of various forms of vascular disease at baseline and the presence of the R219K variant (data not shown).
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85 For all subjects, there was a significantly increased risk of new cardiovascular disease (fatal CHD, non-fatal myocardial infarction, or fatal or non-fatal stroke) on trial for those who carried the ABCA1 R219K variant as compared to those who did not.
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ABCA1 p.Arg219Lys 24854628:85:205
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89 ABCA1 SNP rs2230806 R219K pa GG GA AA All (n) 2834 2167 413 TC (mmol/L) 5.69  0.91 5.68  0.89 5.75  0.93 0.463 LDL-C (mmol/L) 3.81  0.80 3.79  0.80 3.80  0.80 0.655 HDL-C (mmol/L) 1.27  0.34 1.28  0.35 1.30  0.34 0.024 TG (mmol/L) 1.56  0.72 1.53  0.69 1.52  0.64 0.140 apoA-I (g/L) 1.32  0.24 1.33  0.25 1.35  0.23 0.066 apoB (g/L) 1.15  0.23 1.15  0.23 1.15  0.22 0.222 Men (n) 1395 1040 184 TC (mmol/L) 5.36  0.80 5.36  0.80 5.31  0.71 0.819 LDL-C (mmol/L) 3.59  0.72 3.58  0.73 3.54  0.62 0.820 HDL-C (mmol/L) 1.17  0.31 1.18  0.33 1.21  0.30 0.133 TG (mmol/L) 1.50  0.74 1.50  0.74 1.44  0.59 0.568 apoA-I (g/L) 1.24  0.21 1.25  0.24 1.26  0.22 0.166 apoB (g/L) 1.11  0.22 1.10  0.21 1.09  0.19 0.227 Women (n) 1439 1127 229 TC (mmol/L) 6.00  0.89 5.97  0.88 6.11  0.93 0.110 LDL-C (mmol/L) 4.01  0.81 3.99  0.81 4.07  0.82 0.281 HDL-C (mmol/L) 1.36  0.35 1.38  0.35 1.40  0.34 0.091 TG (mmol/L) 1.61  0.69 1.55  0.64 1.60  0.68 0.127 apoA-I (g/L) 1.39  0.25 1.40  0.24 1.42  0.21 0.221 apoB (g/L) 1.20  0.23 1.18  0.22 1.20  0.23 0.577 a p values using the three genotypes, men and women combined; adjusted for gender, body mass index, age, alcohol, smoking, diabetes, apoE phenotype, and country. As for Bonferroni correction of multiple testing, p-value threshold divided by independent tests would be 0.05/12 &#bc; 0.004.
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ABCA1 p.Arg219Lys 24854628:89:20
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98 Discussion We examined the association of a prevalent genetic polymorphism, R219K, at the ABCA1 gene locus with baseline lipids and vascular disease, pravastatin induced LDL-C lowering response, and cardiovascular endpoints on trial in PROSPER, in which participants who had been randomized to pravastatin 40 mg/day or placebo and were followed for a mean of 3.2 years [8].
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104 To date, the association between ABCA1 R219K variant and increased HDL-C level remains controversial.
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105 To our knowledge, only one small study examined potential effects of the R219K variant on statin induced lipid responses [28].
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ABCA1 p.Arg219Lys 24854628:105:73
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108 Our study did not provide direct evidence for the mechanism by which the R219K variant affect the statin effects in cardiovascular event reduction.
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111 Another possible mechanism is that R219K variant plays a novel role in lipid metabolism.
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112 Supporting this is a recent study suggesting that the R219K variant not only affects apoA-I and HDL metabolism, but may also significant influence postprandial lipid metabolism [29].
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115 As for R219K variant, a meta-analysis including 5388 participants reported opposite genotype effects, K-variant as a protective allele, in Chinese population [30].
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ABCA1 p.Arg219Lys 24854628:115:7
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117 Another meta-analysis including 42 studies for R219K variant reported a potential protective role of K-allele, but again suggested limited interpretation of results because of significant heterogeneity among enrolled studies [31].
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119 This pharmacogenetic study enrolled 1686 patients with familial hypercholesterolemia without history of coronary heart disease and analyzed statin-ABCA1 C69T, not R219K, polymorphism interaction by comparing treated and untreated patients.
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130 In conclusion, ABCA1 R219K variant might be a novel genetic determinant for pravastatin treatment response in heart disease risk reduction in the elderly.
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PMID: 25027185 [PubMed] Liu H et al: "Effects of R219K polymorphism of ATP-binding cassette transporter 1 gene on serum lipids ratios induced by a high-carbohydrate and low-fat diet in healthy youth."
No. Sentence Comment
1 And the R219K polymorphism at the gene of ATP-binding cassette transporter 1(ABCA1) was reported to be associated with the profiles.
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ABCA1 p.Arg219Lys 25027185:1:8
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3 This study was to evaluate the effects of ABCA1 R219K polymorphism on serum lipid and apolipoprotein (apo) ratios induced by a high-carbohydrate/low-fat (high-CHO) diet.
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ABCA1 p.Arg219Lys 25027185:3:48
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7 ABCA1 R219K was analyzed by a PCR-RFLP method.
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12 Conclusions: These results suggest that ABCA1 R219K polymorphism is associated differently in males and females with elevated log(TG/HDL-C) and decreased LDL-C/HDL-C induced by the high-CHO diet.
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ABCA1 p.Arg219Lys 25027185:12:46
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30 One of the most common missense polymorphisms in the coding region of the ABCA1 is R219K polymorphism with an allele frequency of the K allele of 46% in the European population [24].
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32 It is believed that the K allele of R219K polymorphism alone is an independent protective factor against CVD.
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33 However, little is known about the interactions between the R219K polymorphism of ABCA1 and the high-CHO diet and their effects on serum lipids and apolipoproteins in health youth.
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34 In this study, we investigated the effects of R219K polymorphism of ABCA1 on the anthropometric parameters and plasma lipid and apolipoprotein ratios after the high-CHO diet in healthy young Chinese, a population well characterized with diets containing high carbohydrate and low incidence of CVD.
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ABCA1 p.Arg219Lys 25027185:34:46
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36 Results The frequencies of genotypes and alleles of R219K polymorphism of ABCA1 The fragment contained R219K polymorphism site of ABCA1 was 177 bp.
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ABCA1 p.Arg219Lys 25027185:36:103
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38 The genotype and allele frequencies of R219K polymorphism of ABCA1 in this study population are shown in Table 1.
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41 The characteristics of the subjects on the 1st day of this study according to R219K genotypes of ABCA1 Due to the small number of the subjects with the KK genotype, the subjects with the RK genotype and the subjects with the KK genotype were combined and defined as the K allele carriers.
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55 R219K polymorphism is located on the first intracellular region of ABCA1 protein, where glycosylation sites can be found.
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64 However, the males with the K allele might be more susceptible than the female counterparts to the favorable effect of R219K polymorphism on serum TG (Table 3), which may be induced by the steroids or other sex hormones [28].
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70 To our knowledge, this is the first attempt to investigate the effects of the high-CHO diet on serum lipid ratios and apoA-1/apoB-100 in young subjects with different genotypes of R219K polymorphisms of ABCA1 in a Chinese young population well characterized with a diet of higher carbohydrate and lower fat and a lower incidence of CVD.
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77 Moreover, unchanged levels of these lipids, or even decreased TG and increased HDL-C and LDL-C, Table 1 Frequencies of the genotype and allele of ABCA1 R219K polymorphism Genotype Allele frequency N RR [case (%)] RK [case (%)] KK [case (%)] R allele K allele Total 56 20 (35.7) 22 (39.3) 14 (25.0) 0.55 0.45 Male 27 8 (14.3) 11 (19.6) 8 (14.3) 0.50 0.50 Female 29 12 (21.4) 11 (19.6) 6 (10.7) 0.60 0.40 were reported after the high-CHO diet [34].
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89 Once confirmed by bigger population and multi-center trials, the findings could provide a new point of view for personalized dietary intervention for the subjects with different genotypes of the R219K polymorphism of ABCA1 to reduce the risks of CVD, especially in a country with a quarter of the world's population.
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110 The primers for the amplification of the DNA fragments containing the R219K polymorphism of ABCA1 by polymerase chain reactions (PCR) were designed according to Clee [24].
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113 The genotype of R219K polymorphism of ABCA1 was analyzed by XagI enzyme digestion.
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189 Li YY, Zhang H, Qin XY, Lu XZ, Yang B, Chen ML: ATP-binding cassette transporter A1 R219K polymorphism and coronary artery disease in Chinese population: a meta-analysis of 5,388 participants.
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207 Evans D, Beil FU: The association of the R219K polymorphism in the ATP-binding cassette transporter 1 (ABCA1) gene with coronary heart disease and hyperlipidaemia.
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238 Biosci Trends 2011, 5:198-204. doi:10.1186/0717-6287-47-4 Cite this article as: Liu et al.: Effects of R219K polymorphism of ATP-binding cassette transporter 1 gene on serum lipids ratios induced by a high-carbohydrate and low-fat diet in healthy youth.
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PMID: 25104170 [PubMed] Liu N et al: "The R219K polymorphism on ATP-binding cassette transporter A1 gene is associated with coronary heart disease risk in Asia population: evidence from a meta-analysis."
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0 ORIGINAL PAPER The R219K Polymorphism on ATP-Binding Cassette Transporter A1 Gene is Associated with Coronary Heart Disease Risk in Asia Population: Evidence from a Meta-Analysis Nannan Liu ߦ Mingxiao Hou ߦ Weidong Ren ߦ Junying Cao ߦ Hongli Wu ߦ Weiwei Zhou Published online: 8 August 2014 &#d3; Springer Science+Business Media New York 2014 Abstract A number of case-control studies have been conducted to investigate the relationship between the ATP-binding cassette transporter A1 (ABCA1) gene polymorphisms and risk of coronary heart disease (CHD).
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6 Statistically significant association between ABCA1 gene R219K polymorphism and increased CHD risk was found in total population analyses in all four genetic comparison models (ORC vs. T 1.19, 95 % CI 1.07-1.31; P = 0.001; ORHomozygote model 1.28, 95 % CI 1.07-1.52; P = 0.007; ORRecessive genetic model 1.22, 95 % CI 1.04-1.44, P = 0.015; ORDominant model 1.21, 95 % CI 1.07-1.35; P = 0.001).
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8 ABCA1 R219K polymorphism is associated with CHD susceptibility, and individuals with ABCA1 have a significantly higher risk of cancer particularly in Asians.
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9 Keywords ABCA1 R219K  CHD  Asians Introduction Coronary heart disease (CHD) is one of the major causes of mortality, being responsible for approximately 30 % of deaths worldwide [34].
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23 lysine substitution at exon 7 (R219K, rs2230806) and isoleucine ?
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25 To date, many case-control studies have been carried out to investigate the relationship between ABCA1 R219K polymorphism and the risk of developing CHD, but the results were conflicting or inconclusive.
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27 Therefore, there is a role for meta-analysis in pooling these studies, particularly to clarify the effect of R219K polymorphism on ABCA1 gene with the risk of CHD.
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32 The inclusion criteria were (1) case-control studies which evaluated the association of R219K polymorphism on ABCA1 with CHD risk; (2) based on unrelated cancer individuals; (3) sufficient published genotype data for estimating an odds ratio (OR) with 95 % confidence interval (CI); and (4) genotype distribution of the control population reported was in Hardy-Weinberg equilibrium (HWE).
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53 Subgroup analyses based on cancer type showed ABCA1-R219K variant was significantly associated with increased risk of CHD and cardiovascular disease (Table 3).
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55 Table 1 Characteristics of studies included in this meta-analysis References Ethnicity (country) Characteristics of cases Characteristics of controls HWE&#e0; Qi et al. [24] Asians 109 histologically confirmed malignant mesothelioma cases 252 population controls Yes Shi et al. [25] Asians 995 histologically confirmed breast cancer cases 1,004 cancer-free controls Yes Sun et al. [27] Asians 234 bladder cancer patients 253 cancer-free controls Yes Tsai et al. [30] Asians 43 histologically confirmed breast cancer cases 31 healthy volunteers Yes Harada et al. [14] Asians 456 histologically confirmed gastric cancer patients 507 healthy controls Yes Tan et al. [28] Asians 294 histologically confirmed lung cancer cases 288 cancer-free controls Yes Zhang et al. [35] Asians 350 histologically confirmed lung cancer cases 350 cancer-free controls Yes Martƒ &#b4;n et al. [19] Caucasians 109 histologically confirmed lung cancer cases 110 cancer-free controls Yes Andrikovics et al. [1] Caucasians 530 bladder cancer patients 556 healthy controls Yes Jensen et al. [15] Caucasians 247 breast cancer cases 380 healthy controls Yes Nebel et al. [20] Caucasians 1,024 histologically confirmed lung cancer cases 1,118 cancer-free controls Yes Evans and Beil [11] Caucasians 710 lung cancer patients 710 cancer-free controls Yes Frikke-Schmidt et al. [12] Caucasians 405 histologically confirmed ESCC cases 478 cancer-free controls Yes ESCC esophageal squamous cell carcinoma; &#e0; HWE Hardy-Weinberg equilibrium Table 2 Distribution of ABCA1 and R219K genotypes and alleles among cancer cases and controls in the meta-analysis References Genotype Allele PHWE T/T (n) T/C (n) C/C (n) T (n) C (n) Case Control Case Control Case Control Case Control Case Control Martƒ &#b4;n et al. [19] 75 104 99 144 27 47 249 352 153 238 0.81 Qi et al. [24] 766 817 210 179 19 8 1,742 1,813 248 195 0.60 Frikke-Schmidt et al. [12] 174 178 56 73 4 2 404 429 64 77 0.06 Andrikovics et al. [1] 20 15 19 13 4 3 59 43 27 19 0.94 Shi et al. [25] 155 188 219 238 82 81 529 614 383 400 0.70 Tsai et al. [30] 251 250 40 37 3 1 542 537 46 39 0.76 Sun et al. [27] 264 291 75 55 11 4 603 637 97 63 0.45 Jensen et al. [15] 37 40 53 52 19 18 127 132 91 88 0.87 Zak and co-authors [2] 174 187 266 275 90 94 614 649 446 463 0.68 Nebel et al. [20] 90 134 107 187 50 59 287 455 207 305 0.64 Harada et al. [14] 783 924 223 182 18 12 1,789 2,030 259 206 0.37 Tan et al. [28] 500 558 198 148 12 4 1,198 1,264 222 156 0.08 Zhang et al. [35] 305 384 94 89 6 5 704 857 106 99 0.95 Caucasians 551 668 763 909 272 302 1,865 2,245 1,307 1,513 0.81 Asians 3,043 3,402 896 763 73 36 6,982 7,567 1,042 835 0.34 Total 3,594 4,070 1,659 1,672 345 338 8,847 9,812 2,349 2,348 \0.01 PHWE P values for Hardy-Weinberg equilibrium The between-study heterogeneity was not obvious in most comparisons except the Allele gene model (R vs. K) comparison analysis based on total studies (I2 = 50.4 %).
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63 The present meta-analysis of 13 case-control studies, involving a total of 5,898 cancer cases and 6,080 controls, provides the most comprehensive assessment so far of the association between ABCA1-R219K polymorphism and cancer risk.
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64 The findings of this meta-analysis indicate that variant homozygote CC of ABCA1-R219K is significantly associated with increased cancer risk (OR = 1.28, 95 % CI 1.07-1.52; P = 0.007).
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71 Therefore, we first stratified studies Fig. 1 Flow chart of selection of studies for inclusion in the meta-analysis Fig. 2 Forest plots of pooled OR with 95 % CI for associations between ABCA1 and R219K polymorphism and CHD risk (The size of the data markers is inversely proportional to the variance of the log ORs; horizontal lines represent the 95 % CIs.
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74 One explanation about how ABCA1 R219K polymorphism modifies the risk of CHD is that ABCA1 may influence the plasma lipid levels.
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76 Only the R219K was significantly associated with HDL-C concentration and CAD risk.
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79 It is probable that the protective function of R219K polymorphism is not only explained by increased plasma HDL-C level, but also by ABCA1 polymorphism.
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82 Another probable mechanism is that R219K polymorphism induces the activity of ABCA1 protein, which mediates cholesterol efflux from peripheral cells back to liver independent of plasma HDL-C levels.
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91 In additional, Cenaro et al. reported that R219K variant appeared to be more protective for smokers and exsmokers than non-smokers in the premature CHD group.
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96 Our meta-analysis supports an association of ABCA1 R219K polymorphism with CHD in Asians.
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99 In subgroup analyses, evidence was obtained to suggest different risk effects of R219K between populations of Caucasians and Asians.
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PMID: 25110219 [PubMed] Abd El-Aziz TA et al: "Increased risk of premature coronary artery disease in Egyptians with ABCA1 (R219K), CETP (TaqIB), and LCAT (4886C/T) genes polymorphism."
No. Sentence Comment
0 Increased risk of premature coronary artery disease in Egyptians with ABCA1 (R219K), CETP (TaqIB), and LCAT (4886C/T) genes polymorphism Tarek A. Abd El-Aziz, MD, Rasha H. Mohamed, PhD*, Hoda A. Hagrass, MD Department of Cardiology, Faculty of Medicine, Zagazig University, Zagazig, Egypt (Dr Abd El-Aziz); Department of Biochemistry, Faculty of Pharmacy, Zagazig University, Zagazig, Egypt (Dr Mohamed); and Department of Clinical Pathology, Faculty of Medicine, Zagazig University, Zagazig, Egypt (Dr Hagrass) KEYWORDS: PCAD; HDLc; ABCA1; CETP; LCAT BACKGROUND: Epidemiological studies have shown a strong inverse relationship between high-density lipoprotein (HDL) cholesterol (HDLc) levels and coronary artery disease (CAD), and a low concentration of plasma HDLc is considered an independent risk factor for premature atherosclerosis.
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20 The common polymorphism in the coding region is R219K (rs2230806), which lead to an arginine/lysine substitution at exon 7.6 CETP facilitates the uptake of cholesterol from peripheral tissues to the liver in an antiatherogenic process known as reverse cholesterol transport.
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34 Amplification of ABCA1 gene R219K (rs2230806) polymorphism The ABCA1 gene polymorphism R219K was detected using polymerase chain reaction (PCR) and restricted fragment length polymorphism analysis (RFLP) as previously described.21 The oligonucleotide primers used were 50 -AAA GAC TTC AAG GACCCAGCTT-30 and 50 - CCTCACATTCCGAAAGCATTA-30 .22 PCR was subjected to 95 C for 5 minutes, 30 cycles of 95 C for 30 seconds, 55 C for 30 seconds, 72 C for 30 seconds, and final extension to 72 C for 7 minutes, producing a fragment of 309 bp.
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36 Amplification of CETP gene TaqIB (rs708272) polymorphism The ABCA1 gene polymorphism R219K was detected using PCR and RFLP as previously described.23 Briefly, a 535-bp fragment in intron 1 of the CETP gene was amplified by PCR, with use of the following oligonucleotide primers: F-50 -CAC TAG CCC AGA GAGAGAGGAGTGCC-30 and R-50 -CTG AGC CCA GCC GCA CAC TAAC-30 at 95 C for 3 minutes followed by 30 cycles of 95 C for 30 seconds, 60 C for 30 seconds, 72 C for 45 seconds, and, last, by 1 cycle at 72 C for 5 minutes.
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58 For R219K polymorphism, we observed a higher frequency of the R allele (46.6% vs 37.8%, OR 1.43; 95% CI 0.99-2.07; P 5 .03) in PCAD patients compared with control group.
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67 Table 2 Genotype and allele frequencies in the study population Polymorphism Case (n 5 116) Control (n 5 119) OR 95% CI P ABCA1 (R219K) KK n (%) 36 (31.1) 50 (42.0) KR n (%) 52 (44.8) 48 (40.3) 1.50 0.84-2.69 .11 RR n (%) 28 (24.1) 21 (17.6) 1.85 0.91-3.76 .06 R allele n (%) 108 (46.6) 90 (37.8) 1.43 0.99-2.07 .03 CETP (Taq1B) B2B2 n (%) 18 (15.5) 32 (26.9) B1B2 n (%) 60 (51.7) 57 (47.9) 1.87 0.95-3.70 .05 B1B1 n (%) 38 (32.8) 30 (25.2) 2.25 1.06-4.77 .02 B1allele n (%) 136 (58.6) 117 (49.16) 1.46 1.01-2.11 .02 LCAT (4886C/T) CC n (%) 26 (22.4) 49 (41.2) CT n (%) 56 (48.3) 55 (46.2) 1.92 1.05-3.51 .02 TT n (%) 34 (29.3) 15 (12.6) 4.27 1.97-9.24 .000 T allele n (%) 124 (53.5) 85 (35.7) 2.07 1.43-2.99 .000 ABCA1, ATP-binding cassette A1 transporter; CETP, cholesteryl ester transfer protein; LCAT, lecithin: cholesterol acyltransferase.
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72 The frequency of the B1 allele was also significantly increased in the combined hyperlipidemic group compared with the control group (61.1% vs Table 3 Genotypes distribution and correlation with HDLc levels Polymorphism PCAD with low HDLc (n 5 70) PCAD with normal HDLc (n 5 46) OR 95% CI P ABCA1 (R219K) K allele n (%) 46 (32.9) 78 (84.8) R allele n (%) 94 (67.1) 14 (15.2) 11.38 5.83-22.23 .000 CETP (Taq1B) B2 allele n (%) 36 (25.7) 60 (65.2) B1allele n (%) 104 (74.3) 32 (34.8) 5.41 3.05-9.60 .000 LCAT (4886C/T) C allele n (%) 42 (30.0) 66 (71.7) T allele n (%) 98 (70.0) 26 (28.3) 5.92 3.31-10.58 .000 ABCA1, ATP-binding cassette A1 transporter; CETP, cholesteryl ester transfer protein; HDLc, high-density lipoprotein cholesterol; LCAT, lecithin: cholesterol acyltransferase; PCAD, premature coronary artery disease.
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73 Table 4 Genotypes distribution across different phenotypes Polymorphism Control (n 5 119) PCAD with high TGs (phenotype I, IV) (n 5 24) OR 95% CI P ABCA1 (R219K) K allele n (%) 148 (62.2) 24 (50.0) R allele n (%) 90 (37.8) 24 (50.0) 3.64 1.22-10.85 .009 CETP (Taq1B) B2 allele n (%) 121 (50.8) 16 (33.3) B1allele n (%) 117 (49.2) 32 (66.7) 2.06 1.07-3.96 .019 LCAT (4886C/T) C allele n (%) 153 (64.3) 24 (50.0) T allele n (%) 85 (35.7) 24 (50.0) 3.33 1.11-9.92 .016 Polymorphism Control (n 5 119) PCAD with high LDL (phenotype IIa) (n 5 2) OR 95% Cl P ABCA1 (R219K) K allele n (%) 148 (62.2) 3 (75.0) R allele n (%) 90 (37.8) 1 (25.0) 0.54 0.05-5.35 .52 CETP (Taq1B) B2 allele n (%) 121 (50.8) 2 (50.0) B1 allele n (%) 117 (49.2) 2 (50.0) 0.96 0.13-6.97 .67 LCAT (4886C/T) C allele n (%) 153 (64.3) 3 (75.0) T allele n (%) 85 (35.7) 1 (25.0) 0.60 0.06-5.85 .55 Polymorphism Control (n 5 119) PCAD with high TG 1 LDL (phenotype IIb) (n 5 72) OR 95% CI P ABCA1 (R219K) K allele n (%) 148 (62.2) 72 (50.0) R allele n (%) 90 (37.8) 72 (50.0) 1.64 1.08-2.50 .013 CETP (Taq1B) B2 allele n (%) 121 (50.8) 56 (38.9) B1 allele n (%) 117 (49.2) 88 (61.1) 1.62 1.06-2.47 .015 LCAT (4886C/T) C allele n (%) 153 (64.3) 60 (41.7) T allele n (%) 85 (35.7) 84 (58.3) 2.52 1.64-3.85 .000 ABCA1, ATP-binding cassette A1 transporter; CETP, cholesteryl ester transfer protein; HDLc, high-density lipoprotein cholesterol; LDLc, low-density lipoprotein cholesterol; LCAT, lecithin: cholesterol acyltransferase; PCAD, premature coronary artery disease; TC, total cholesterol; TG, triglyceride.
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ABCA1 p.Arg219Lys 25110219:73:155
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84 These factors may vary depending on race and ethnic group.25 HDL Table 5 Lipid profile distribution across genotypes TC (mg/dL) TG (mg/dL) LDLc (mg/dL) HDLc (mg/dL) ABCA1 (R219K) KK 196.96 6 65.86 187.39 6 65.19 104.19 6 59.94 55.12 6 7.55 RK 215.14 6 67.66* 217.91 6 49.10** 130.88 6 70.27** 40.72 6 7.94# RR 242.14 6 55.68# 223.48 6 72.15** 168.05 6 60.54# 29.28 6 2.66# CETP (Taq1B) B2B2 197.68 6 66.84 184.22 6 74.77 110.19 6 70.34 58.90 6 7.52 B2B1 224.62 6 64.66 215.67 6 54.72** 128.87 6 57.02 44.20 6 8.18# B1B1 234.69 6 60.53* 211.95 6 61.13* 160.98 6 61.58** 31.32 6 4.19# LCAT (4886C/T) CC 200.15 6 72.52 205.07 6 62.86 104.52 6 66.62 54.43 6 8.55 CT 216.37 6 67.38 201.41 6 58.20 133.86 6 72.16** 42.23 6 9.46# TT 230.40 6 49.52* 226.95 6 67.67* 154.80 6 49.31# 30.14 6 3.45# HDLc, high-density lipoprotein cholesterol; LDLc, low-density lipoprotein cholesterol; TC, total cholesterol; TG, triglyceride.
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92 R219K is the most common polymorphism of ABCA1 and the allele frequency of the K allele is 26-46% in the Caucasian population.29,30 To date, several studies have reported controversial results about the possible role of R219K in arteriosclerosis.
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94 This is in line with recent meta-analysis31 involving 2730 CAD patients and 2658 controls and found that the K allele of the ABCA1 R219K gene has a protective role for CAD risk in Chinese population and is possibly associated with decreased CAD susceptibility.
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96 Also, Takagi et al. concluded that the polymorphism does not seem to influence coronary atherosclerosis.35 HDLc is a major independent factor involved in the development of premature CAD The antiatherogenic function of HDL has been attributed to its role in reverse cholesterol transport, and the protein ABCA1 plays a crucial role in its initial step.36 Several studies have showed that the R allele in the R219K ABCA1gene polymorphism causes low HDLc levels, increased triglycerides, depressed levels of cholesterol efflux, and an increased risk of CAD.37,38 In agreement of this finding, we found that the frequency of the R allele of ABCA1 was significantly increased in PCAD with low HDLc levels compared with PCAD with normal HDLc levels (67.1% vs 15.2%).
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PMID: 25279016 [PubMed] Marvaki A et al: "Impact of 3 Common ABCA1 Gene Polymorphisms on Optimal vs Non-Optimal Lipid Profile in Greek Young Nurses."
No. Sentence Comment
1 They evaluated the influence of ATP-binding cassette transporter A1 (ABCA1) gene polymorphisms [such as rs2230806 (R219K), rs2230808 (R1587K) and rs4149313 (I883M)] on the human lipid profile (defined as Optimal and Non-Optimal).
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3 All subjects were genotyped and the ABCA1 polymorphisms (R219K, R1587K and I883M) were recorded.
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5 Results: No statistical differences were observed in the distribution of R219K, R1587K and I883M polymorphisms according to the lipid profile (p>0.05 in all cases).
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6 No statistical differences were observed in the distribution of R219K, R1587K and I883M polymorphisms according to sex (p>0.05 in all cases).
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15 Several ABCA1 gene polymorphisms have been identified, such as rs2230806 (R219K) in the chromosomal position 107620867, rs2230808 (R1587K) in the chromosomal position 106602625 and rs4149313 (I883M) in the chromosomal position 106626574.
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17 The aim of the study, in line with our previous work [57], was to evaluate the R219K, R1587K and I883M of ABCA1 gene polymorphisms according to lipid profile.
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26 According to Genotypes We evaluated single nucleotide polymorphisms (SNPs) in chromosome 9 such as rs2230806 (R219K) in the position 107620867, rs2230808 (R1587K) in the position 106602625 and rs4149313 (I883M) in the position 106626574 according to lipid profile by using polymerase chain reaction (PCR) and restricted fragment length polymorphism analysis (RFLP`s) (see below).
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29 DNA Analysis and Determination of Blood Lipids The ABCA1 gene polymorphisms (R219K, R1587K and I883M) were detected using PCR and RFLP`s.
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31 For R219K polymorphism the oligonucleotide primers which were used were AAAGACTTCAAGGACCCAGCTT and CCTCACATTCCGAAAGCATTA [9].
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45 There was no difference in R219K, R1587K and I883M polymorphisms frequency according to Optimal and Non-Optimal lipid profile (p = 0.49, 0.29 and 0.42, respectively).
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48 DISCUSSION We examined the impact of the R219K, R1587K and I883M of ABCA1 polymorphisms as a genetic influence on the lipid profile in Greek subjects.
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49 In this context, the possible effects of the ABCA1 polymorphisms on lipids or cardiovascular disease were recently evaluated in various populations such as Japanese [11] in which correlation with HDL-C concentrations was found, Saudi [12] in which the ABCA1 C69T gene frequency was higher in healthy subjects compared with diabetic patients, Chinese [13], in which ABCA1 gene R219K polymorphism was associated with ischemic stroke, Greek [5-7] in which a gender-specific effect of the R219K polymorphism on plasma lipids was demonstrated, Turkish [14] in which a gender-specific effect of the R219K polymorphism on plasma lipids and CHD was shown and Mexican [15] in which several European loci as well as a novel one for high TG and low HDL-C levels were identified.
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ABCA1 p.Arg219Lys 25279016:49:376
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52 The relationship between ABCA1 R219K, R1587K and I883M and Alzheimer disease has been reported in various ethnic groups with contradictory results.
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54 With regard to subgroups with low HDL-C, Hodo f;lugil et al. [17] reported that R219K and I883M polymorphisms were related to higher HDL-C levels, Slatter et al. [18] found that R1587K was overexpressed in low HDL-C individuals, whereas Frikke-Schmidt et al. [19] did not observe any association with R219K but reported that R1587K polymorphism was overexpressed in individuals with low HDL-C concentrations.
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55 In subgroups with high HDL-C, Kakko et al. [20] found a minor association between ABCA1 polymorphisms and HDL-C levels in women, whereas Clee et al. [4] reported a non-significant trend towards higher HDL-C levels in carriers of R219K.
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58 R219K R1587K I883M n (%) n (%) n (%) RR 225 (50.2) RR 211 (47.1) II 309 (69.0) RK 191 (42.6) RK 193 (43.1) IM 131 (29.2) KK 32 (7.1) KK 44 (9.8) MM 8 (1.8) R 71.5 R 68.6 I 83.6 K 28.5 K 31.4 M 16.4 Table 1.
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63 For example, Clee et al. [4] reported that carriers of K allele of R219K polymorphism had significantly lower TG levels in relation to carriers of the R allele, whereas others did not find any associations.
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65 Delgado-Lista et al. [21] reported a trend for lower fasting TG and large TG-rich lipoproteins in minor allele carriers compared with major allele homozygotes of R219K polymorphism.
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66 In our study with young Greek nurses (living and working in similar conditions) we did not observe any association of R219K polymorphism with HDL-C or other lipid levels, although we found that individuals with RK genotype of R1587K polymorphism had significantly higher TC, LDL-C and TG levels compared with the RR genotype [7].
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68 Sandhofer et al. [22] found that K allele of R219K gene displayed a lower intima media thickness and a reduced risk of advanced plaque extent compared with non-carriers only in non-smokers and concluded that smoking abrogates the protective effect of the R219K.
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69 Cenarro et al. [23] reported that the K allele of the R219K gene was significantly more frequent in familial hypercholesterolemia subjects without premature CHD than in familial hypercholesterolemia subjects with premature CHD and it appears to be more protective for smokers than non-smokers.
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PMID: 25286446 [PubMed] Kelishadi R et al: "Genetic association with low concentrations of high density lipoprotein-cholesterol in a pediatric population of the Middle East and North Africa: the CASPIAN-III study."
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121 A study in Iranian adults showed that R219K SNP could affect HDL-C levels and could influence the risk of atherosclerosis in Iranian population [46].
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123 In a meta-analysis with 6597 cases and 15,369 controls for investigation of the association between the ABCA1 R219K polymorphism and ACVD risk; the R219K SNP was associated with a higher HDL-C level in Asians and protective for ACVD risk both in Asians and Caucasians.
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124 A recent meta-analysis involving 2730 ACVD patients and 2658 controls showed that K allele of the ABCA1 R219K gene has a protective role for ACVD risk in the Chinese population [48].
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PMID: 25527331 [PubMed] Yin YW et al: "ATP-binding cassette transporter 1 C69T and V825I polymorphisms in the development of atherosclerosis: a meta-analysis of 18,320 subjects."
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36 Previously, we performed a meta-analysis to evaluate the associations between the ABCA1 R219K and I883M polymorphisms and AS risk, and demonstrated the above variants were the protective roles for AS [17].
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122 So far, at least seven single-nucleotide polymorphisms at the ABCA1 gene promoter have been studied to investigate the associations between these variants and the susceptibility of atherosclerotic diseases, such as R219K, M883I, C69T, V825I, R1587K, V771M and -565C/T.
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123 In our previous study, we have demonstrated that the ABCA1 R219K and M883I polymorphisms are the protective factors for AS [17].
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PMID: 25785043 [PubMed] He Y et al: "Up-regulated miR-93 contributes to coronary atherosclerosis pathogenesis through targeting ABCA1."
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128 [4] Abd ET, Mohamed RH and Hagrass HA. Increased risk of premature coronary artery disease in Egyptians with ABCA1 (R219K), CETP (TaqIB), and LCAT (4886C/T) genes polymorphism.
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PMID: 25877294 [PubMed] Mokuno J et al: "ATP-binding cassette transporter A1 (ABCA1) R219K (G1051A, rs2230806) polymorphism and serum high-density lipoprotein cholesterol levels in a large Japanese population: cross-sectional data from the Daiko Study."
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2 The rate is lower in East Asian countries compared with Western countries. For example, the age-adjusted mortality rate (per 100,000 in 2004) was 32.1 in Japan, 40.3 in Korea, and 62.8 in China whereas it was ATP-binding cassette transporter A1 (ABCA1) R219K (G1051A, rs2230806) polymorphism and serum high-density lipoprotein cholesterol levels in a large Japanese population: cross-sectional data from the Daiko Study Junichiro Mokuno, Asahi Hishida, Emi Morita, Tae Sasakabe, Yuta Hattori, Shino Suma, Rieko Okada, Sayo Kawai, Mariko Naito and Kenji Wakai Department of Preventive Medicine, Nagoya University Graduate School of Medicine, Nagoya 466-8550, Japan Abstract.
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3 Among polymorphisms in ATP-binding cassette transporter A1 (ABCA1) gene, the available evidence demonstrates that the ABCA1 R219K polymorphism (G1051A, rs2230806) K allele is associated with a higher high-density lipoprotein cholesterol (HDL-C) level and may play a protective role against coronary artery disease (CAD) risk in Asians and Caucasians.
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13 In the multiple linear regression analysis to estimate the independent effects of the R219K polymorphism on HDL-C level, however, the number of K allele was significantly correlated with an increased level of HDL-C (trend P=0.033).
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15 The R219K polymorphism of ABCA1 independently associated with serum level of HDL-C in a large Japanese population.
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53 Therefore, to clarify the association of ABCA1 R219K polymorphism with serum HDL-C levels in a large Japanese population, we examined this associa- tive combined; to explain in detail, we first defined the 5 categories of drinking status as follows: nonhabitual drinker, former habitual drinker, or habitual drinker of ethanol at < 23, 23 - < 46, and > 46 g per day (equivalent to < 1 gou, 1-2 gou and > 2 gou of Japanese sake, respectively; where 1 gou [a unit for Japanese sake] = 180mL) per day, and then converted each category into indicator variables.
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56 Genotyping of ABCA1 R219K polymorphism DNA was extracted from buffy coat kept at -80&#b0;C using a Biorobot M48 (QIAGEN Group, Tokyo).
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65 The difference in the serum HDL-C level between the ABCA1 R219K genotypes by sex was tested by the analysis of variance (ANOVA).
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71 The logic of PCR-CTPP for R219K polymorphism (corresponding base change from A to G) can be explained as follows: as described in elsewhere [14], confronting pairs of primers are used; one pair is for the K allele and the other is for the R allele.
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77 In the multiple linear regression analysis to estimate the independent effects of the R219K polymorphism on HDL-C level (Table 3), the number of K allele was significantly associated with an increased level of HDL-C (trend P=0.033).
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80 Results Clinical profiles of subjects by ABCA1 R219K genotype were shown in Table 1.
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83 The mean HDL-C concentration was higher in men and women with RK or KK genotype than those with RR, although the difference between Table 1 Clinical Profiles of subjects by ABCA1 R219K (rs2230806) genotype (n =5,133) KK RK RR P (26.8%, n = 1,376) (49.3%, n = 2,532) (23.9%, n = 1,225) Female 988 (71.8%) 1,818 (71.8%) 869 (70.9%) 0.84 Age (years) 52.6 &#b1; 10.4 52.5 &#b1; 10.3 52.5 &#b1; 10.3 0.98 Body mass index (kg/m2 ) 21.8 &#b1; 3.3 21.7 &#b1; 3.1 21.7 &#b1; 3.1 0.65 Current smokers 163 (11.8%) 298 (11.8%) 146 (11.9%) 0.99 Current drinkers 757 (55.0%) 1,357 (53.6%) 663 (54.1%) 0.70 Hypertension 226 (16.4%) 363 (14.3%) 192 (15.7%) 0.19 Diabetes mellitus 54 (3.9%) 89 (3.5%) 42 (3.4%) 0.75 Values are expressed as means &#b1; standard deviation, or n (%).
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84 Table 2 Mean &#b1; standard deviation of HDL-C level (mg/dL) by sex and ABCA1 R219K (rs2230806) genotype and sex KK RK RR P* (n = 1,376) (n = 2,532) (n = 1,225) Male (n =1,458) 57.3 &#b1;15.0 56.4 &#b1; 13.7 55.7 &#b1; 14.0 0.31 Female (n =3,675) 68.7&#b1; 14.5 68.7 &#b1; 14.9 67.7 &#b1; 14.9 0.26 * By analysis of variance (ANOVA).
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88 Concerning ABCA1 R219K polymorphism, the frequency of K allele was reported to be 0.488 in Japanese [22] while that in the Caucasian population ranged between 0.25 and 0.46 [21].
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90 Moreover, there is a great variation and diversity in the effects of dietary and other lifestyle factors on lipid levels between ethnicities or study populations, which may also lead to the different interaction with the effect of this ABCA1 R219K polymorphism.
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97 R219K polymorphism is located in the two major extracellular loops of ABCA1 protein, which is important for the interaction with apoA-I and for cholesterol efflux.
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98 Therefore, it is likely that the R219K variant is a functional mutation to modulate HDL-C level.
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101 Either way, given that based on the functional analysis using SIFT and PolyPhen, this R219K variation of ABCA1 is suggested not to be functional in itself, it could rather be causal The analysis results of the association between ABCA1 R219K polymorphism and HDL-C level adjusted by drinking status and in males were substantially in the same direction compared to that of overall, with the b2;-coefficient of 0.840 for RK genotype, 1.818 for KK genotype, 0.911 with the number of K allele, with the P-values of 0.321, 0.058 and 0.057, respectively.
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102 The association between R219K of ABCA1 and triglyceride (TG) levels was neither statistically significant (data not shown).
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103 Discussion We found a significant association between the R219K polymorphism K allele of ABCA1 and a higher serum HDL-C level in a large Japanese population.
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104 Previous studies have reported that the R219K polymorphism was associated with increased circulating HDL-C.
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106 It was reported by Clee et al. that the R219K K allelle was associated with a higher level of HDL-C and a lower level of TG [15].
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107 Additional studies in Caucasian, Asian and multi-ethnic populations have also shown the association between the ABCA1 R219K polymorphism and the HDL-C level [6].
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108 Our data based on a Japanese population revealed consistent elevations in blood HDL-C levels associated with the K allele of ABCA1 R219K polymorphism.
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116 Given the considerably large sample size, the present study may have a significant impact by providing the first robust evidence for the protective effect of the K variant in the ABCA1 R219K polymorphism in Japanese.
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117 However, because we focused on ABCA1 R219K polymorphism, we could not evaluate the influence of other polymorphisms of ABCA1 gene.
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119 In summary, the R219K polymorphism of ABCA1 was independently associated with serum level of HDL-C in a large Japanese population.
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128 The effect of the K variant in the ABCA1 R219K polymorphism examined was in the same direction compared to that in the recent meta-analysis in the Asian populations [29], and in the opposite direction to that in the Japanese subjects [22].
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129 The forementioned recent meta-analysis of HDL-C and ABCA1 R219K consisted of mixture of cohort studies and hospital-based case-control studies; the population of which consisted of Caucasians, Chinese, Japanese and Iraqis, most of the Asian populations of which were Chinese.
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143 Ma XY, Liu JP, Song ZY (2011) Associations of the ATP-binding cassette transporter A1 R219K polymorphism with HDL-C level and coronary artery disease risk: a meta-analysis.
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176 Liu N, Hou M, Ren W, Cao J, Wu H, Zhou W (2015) The R219K polymorphism on ATP-binding cassette transporter A1 gene is associated with coronary heart disease risk in Asia population: evidence from a meta-analysis.
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185 Yin YW, Li JC, Gao D, Chen YX, Li BH et al. (2014) Influence of ATP-binding cassette transporter 1 R219K and M883I polymorphisms on development of atherosclerosis: a meta-analysis of 58 studies.
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211 Li J, Wang LF, Li ZQ, Pan W (2009) Effect of R219K polymorphism of the ABCA1 gene on the lipid-lowering effect of pravastatin in Chinese patients with coronary heart disease.
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214 Li Y, Zhang SZ, Ma YX, He Y, Dong JT, et al. (2005) Relationship between the R219K polymorphism of ATP-binding cassette transporter 1 gene and coronary heart disease.
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217 Zhao S, Xiao Z (2004) The study on ABCA1 R219K
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PMID: 26243156 [PubMed] Fawzy MS et al: "Functional and Structural Impact of ATP-Binding Cassette Transporter A1 R219K and I883M Gene Polymorphisms in Obese Children and Adolescents."
No. Sentence Comment
4 Two genetic variants in ABCA1 gene-R219K (rs2230806; G/A) and I883M (rs2066714; A/G)-were genotyped in 128 normal weight and 128 overweight/obese subjects using polymerase chain reaction-restriction fragment length polymorphism technology.
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6 Results Our findings suggest that the heterozygote GA genotype of R219K polymorphism increased susceptibility to obesity under the heterozygous model (odds ratio 2.75, 95 % CI 1.01-6.12; p = 0.014) compared with the control group.
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11 Conclusions The study results suggest that R219K and I883M SNPs of the ABCA1 gene may play a role in susceptibility to obesity in our Egyptian population; the former increases susceptibility and phenotype severity, and the latter is protective.
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14 & Manal S. Fawzy manal2_khashana@ymail.com & Eman A. Toraih emantoraih@gmail.com 1 Department of Medical Biochemistry, Faculty of Medicine, Suez Canal University, Ismailia, Egypt 2 Department of Medicine, Faculty of Medicine, Taibah University, Almadinah Almunawwarah, Kingdom of Saudi Arabia 3 Department of Chest Diseases, Faculty of Medicine, Cairo University, Giza, Egypt 4 Department of Cardiology, Faculty of Medicine, Suez Canal University, Ismailia, Egypt 5 Department of Rheumatology and Rehabilitation, Faculty of Medicine, Suez Canal University, Ismailia, Egypt 6 Department of Pediatrics, Faculty of Medicine, Suez Canal University, Ismailia, Egypt 7 Department of Histology and Cell Biology (Genetics Unit), Faculty of Medicine, Suez Canal University, Ismailia, Egypt Mol Diagn Ther (2015) 19:221-234 DOI 10.1007/s40291-015-0150-7 Key Points ABCA1 R219K and M883I polymorphisms may play a role in susceptibility to obesity in the Egyptian population.
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15 ABCA1 R219K and M883I polymorphisms showed significant association with lipid levels among different genotype carriers.
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16 The GA genotype of R219K polymorphism increased susceptibility to obesity under the heterozygous model, the A variant was associated with a higher degree of obesity, the G variant of I883M polymorphism significantly decreased the risk of obesity under all genetic models.
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37 One of the most common single nucleotide polymorphisms (SNPs) affecting the amino acid sequence is the R219K (rs2230806) that results from nucleotide change G[A in exon 7 at position 1060, causing substitution of lysine for arginine at amino acid 219 (electronic supplementary Table S1).
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39 Despite the high number of case-control studies conducted to investigate the functionality of R219K variant, the results have been inconclusive [10, 20-22].
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43 In this study, we investigated the prevalence of these frequently occurring variants of the ABCA1 gene, R219K and I883M polymorphisms, in association with anthropometric parameters and lipid profile in Egyptian overweight/obese children and adolescents.
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60 The most frequent endocrine diseases causing obesity (such as Cushing syndrome, hypothyroidism, and pseudohypoparathyroidism), or genetic syndromes associated with obesity (such as Prader- Fig. 3 Workflow for PCR genotyping of R219K and I883M polymorphisms in the study population.
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80 Genotyping of ABCA1 R219K and I883M variations were conducted by polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) method.
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102 In R219K rs2230806, 174 bp- amplified fragment includes the genetic variant (AGG/AAG) existing in exon 7 (coordinates: 104,858,698-104,858,522) of two protein-coding transcripts (ABCA1-001 and ABCA1-002).
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111 R219K (rs2230806): M, DNA marker 50 bp each; Lanes 1, 6 AA genotype with two bands at 109 and 65 bp; Lanes 2, 5,7,9 GG genotype with only one band at 174 bp; Lanes 3, 4, 8 GA genotype with three bands at 174, 109, and 65 bp.
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124 Experimentally-genotyped polymorphisms (R219K and I883M) in the study population are shown in electronic supplementary Fig. 5.
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127 However, R219K (rs2230806) and I883M (rs2066714) are in linkage disequilibrium with other nearby intronic SNPs which might have deleterious effects on the protein function.
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129 Both ABCA1 R219K (g.1060G[A) and I883M (g.3044A[G) genotypes were in agreement with those expected by the HWE (p [ 0.05).
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130 In R219K polymorphism, there was a significant difference in genotype frequencies between overweight/obese and control groups (p = 0.042).
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135 R219K and I883M polymorphisms are far apart, existing in different haplotype blocks in the ABCA1 gene.
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138 3.3 ABCA1 Gene Polymorphisms in Relation to Clinical Characteristics AA-R219K genotype was associated with more BMI (p = 0.03) and showed a higher degree of obesity (p \ 0.001) (Table 3 and Fig. 6).
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142 However, overweight/obese subjects with AA-R219K had significantly higher levels of TC, LDL-c, and TC/HDL-c ratio, and lower HDL-c compared with non-carriers, while GG-I883M carriers had decreased levels of TC, HDL-c and LDL-c levels compared with those with other genotypes (p \ 0.05) (Table 3 and electronic supplementary Fig. 7).
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148 To the best of our knowledge, there are no published data on the screening of the ABCA1 R219K and I883M polymorphisms in association with obesity and lipid profile among the Egyptian population.
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153 In silico data analysis predicted our cSNPs (R219K and I883M) to be functionally neutral using the PolyPhen and MutPred web-based programs.
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155 In our study population, the R219K variant showed increased risk of developing obesity among GA heterozygote carriers, especially in children and females, whereas in I883M SNP analysis, carriers of the M allele (GA and GG genotypes) displayed reduced susceptibility to obesity in children and adolescents and in both genders compared with those with the AA genotype (I allele).
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156 This was consistent with others who reported that the presence of ABCA1 polymorphisms could be a risk Table 2 Genotype and allele frequencies of ABCA1 gene polymorphisms in the study groups Polymorphism Controls (n = 128) OW/OB (n = 128) Chi-square p value Crude OR (95 % CI) Adjusted OR (95 % CI) R219K (G/A) Genotypes GG 21 (16.4) 10 (7.8) 6.306 0.042 Reference Reference GA 51 (39.8) 67 (52.4) 2.75 (1.19-6.36) 2.75 (1.01-6.12) AA 56 (43.8) 51 (39.8) 1.91 (0.82-44.0) 1.04 (0.76-42.5) GA ?
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158 GG 91 (71.1) 62 (48.4) 0.38 (0.22-0.63) 0.37 (0.20-0.58) HWE-P 0.208 0.956 Alleles A 144 (56.2) 184 (71.9) 13.57 <0.001 Reference Reference G 112 (43.8) 72 (28.1) 0.50 (0.34-0.72) 0.49 (0.31-0.77) Data are expressed as n (%) Bold values indicate statistically significant at p \ 0.05 ABCA1 ATP-binding cassette transporter A1, OW/OB overweight/obese group, R219K c.656G[A, I883M c.2649A[G, adjusted OR (95 % CI) odds ratio for confidence interval adjusted for confounding variables (age, gender, degree of obesity, and dyslipidemia) Fig. 5 Linkage disequilibrium between R219K and I883M.
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159 Experimentally-tested SNPs in ABCA1 gene: I883M (rs2066714) and R219K (rs2230806) are noted.
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169 Consistent with our results, Villard et al. reported R219K SNP to be associated with a significant modification of cholesterol efflux capacity in a sex-dependent manner [53].
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175 Intracellular ABCA1 domains could interact and hydrolyze ATP, generating energy for Table 3 Anthropometric measurements and lipid profile in overweight/obese subjects according to R219K and I883M genotypesa R219K (G/A) genotypes p value I883M (A/G) genotypes p value GG (n = 10) GA (n = 67) AA (n = 51) AA (n = 66) AG (n = 52) GG (n = 10) Age, years 11.3 &#b1; 3.1 12.5 &#b1; 3.8 12.5 &#b1; 3.5 0.61 12.9 &#b1; 3.3 12.1 &#b1; 3.6 14.8 &#b1; 2.5 0.05 Anthropometric data BMI, kg/m2 29.8 &#b1; 2.7 33.6 &#b1; 6.7 35.6 &#b1; 7.0b 0.03b 34.7 &#b1; 6.3 33.7 &#b1; 6.4 33.7 &#b1; 5.4 0.67 WHR 0.84 &#b1; 0.1 0.86 &#b1; 0.1 0.89 &#b1; 0.1 0.17 0.88 &#b1; 0.1 0.87 &#b1; 0.1 0.89 &#b1; 0.1 0.84 WHtR 0.63 &#b1; 0.1 0.64 &#b1; 0.1 0.68 &#b1; 0.2 0.30 0.70 &#b1; 0.2 0.66 &#b1; 0.1 0.68 &#b1; 0.2 0.43 Lipid profile TC, mg/dl 196.0 &#b1; 70.4 221.0 &#b1; 38.0 235.9 &#b1; 38.6b 0.02b 209.4 &#b1; 44.7 232.9 &#b1; 35.5b 166.0 &#b1; 38.4c <0.001b TG, mg/dl 74.7 &#b1; 18.2 92.9 &#b1; 30.4 99.8 &#b1; 34.4 0.07 94.1 &#b1; 35.6 96.6 &#b1; 30.2 100.0 &#b1; 33.0 0.84 HDL-c, mg/dl 67.0 &#b1;26.9 67.9 &#b1; 20.5 57.5 &#b1; 19.9c 0.03b 56.5 &#b1;18.0 69.4 &#b1; 19.6b 39.7 &#b1; 9.6b,c <0.001b LDL-c, mg/dl 114.0 &#b1; 43.0 132.2 &#b1; 30.6 158.0 &#b1; 37.2b,c <0.001b 134.2 &#b1; 39.8 140.9 &#b1; 31.6 106.7 &#b1; 25.6b,c 0.02b Values are expressed as mean &#b1; SD or n (%) Comparisons between genotypes of each polymorphism were performed by one-way ANOVA followed by Newman-Keuls multiple comparisons test Bold values indicate statistically significant at p \ 0.05 BMI body mass index, WHR waist/hip ratio, WHtR waist/height ratio, TC total cholesterol, TG triglycerides, HDL-c high-density lipoprotein cholesterol, LDL-c low-density lipoprotein cholesterol, ANOVA analysis of variance a Age and sex were used as covariates in the analysis to adjust for the genotyping effect.
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ABCA1 p.Arg219Lys 26243156:175:180
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ABCA1 p.Arg219Lys 26243156:175:207
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176 Degree of obesity was classified according to the BMI z score b Indicates significant difference from homozygous carriers of the wild allele in the same group at p \ 0.05 c Indicates significant difference from heterozygous carriers in the same group at p \ 0.05 0% 20% 40% 60% 80% 100% OW OB1 OB2 Degree of obesity R219K genotype GG (n=10) GA (n=67) AA (n=51) p<0.001* 0% 20% 40% 60% 80% 100% OW OB1 OB2 Degree of obesity I883M genotype AA (n=66) AG (n=52) GG (n=10) p=0.098 (b) (a) Fig. 6 Genotype frequencies according to the degree of obesity.
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ABCA1 p.Arg219Lys 26243156:176:316
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181 Thus, we could propose the hypothesis that homo- or heterodimerization could have differential effects on the function of the protein, and this could provide a possible explanation for the increased obesity risk in our study among GA heterozygotes of R219K polymorphism compared with homozygotes.
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ABCA1 p.Arg219Lys 26243156:181:251
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189 However, patients with GA and AA genotypes of R219K SNP exhibited higher frequency of severe obesity and more BMI levels compared with other genotypes.
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ABCA1 p.Arg219Lys 26243156:189:46
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192 R219K polymorphism is located at the binding site of the lipid acceptor ApoA-1, and thus is strongly associated with protein activity and stabilization against ABCA1 degradation [6].
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ABCA1 p.Arg219Lys 26243156:192:0
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198 In the current study, overweight/obese subjects with the AA-R219K genotype had an unfavorable lipid profile; mainly higher levels of TC, LDL-c, TG/HDL-c ratio, and TC/HDL-c ratio, and lower HDL-c compared with other genotypes.
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ABCA1 p.Arg219Lys 26243156:198:60
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206 In healthy-weight subjects, R219K SNP was shown to be associated with altered HDL-c phenotype [65, 66].
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ABCA1 p.Arg219Lys 26243156:206:28
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207 Homozygotes of the A allele of R219K were associated with increased LDL-C and TC and decreased HDL-c concentrations in Turkish population [54].
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ABCA1 p.Arg219Lys 26243156:207:31
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209 In obesity, the K allele of the R219K polymorphism was also associated with lower HDL-c levels than controls among overweight/ obese Thai males, with no difference in HDL-c concentrations among genotypes of I883M polymorphism [10].
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ABCA1 p.Arg219Lys 26243156:209:32
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212 The AA genotype of the R219K polymorphism was significantly associated with increased concentrations of HDL-C in the Tunisian population [47], and the GG genotype had lower HDL-c levels than those with the AA genotype in the Chinese population [69].
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ABCA1 p.Arg219Lys 26243156:212:23
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220 Moreover, in the ABCA1 gene, a strong linkage disequilibrium exists between R219K/V771M and M825I/I883M (D0 [ 0.9) [21].
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ABCA1 p.Arg219Lys 26243156:220:76
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221 The two SNPs (V771M and M825I) were previously found to be associated with increased plasma HDL-c and cholesterol concentration, respectively, thus speculating the probability that R219K and I883M may not be the true associated variants, but could instead reflect the functional impact of other nearby linked gene polymorphisms.
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ABCA1 p.Arg219Lys 26243156:221:181
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228 5 Conclusions The present study suggested that the R219K (rs2230806) polymorphism of the ABCA1 gene is associated with higher susceptibility to obesity and unfavorable outcome in the Egyptian population, while I883M (rs2066714) polymorphism is associated with a reduced risk of obesity in childhood and adolescence.
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ABCA1 p.Arg219Lys 26243156:228:51
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PMID: 26579206 [PubMed] Jacobo-Albavera L et al: "Dietary fat and carbohydrate modulate the effect of the ATP-binding cassette A1 (ABCA1) R230C variant on metabolic risk parameters in premenopausal women from the Genetics of Atherosclerotic Disease (GEA) Study."
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87 A larger study using food frequency questionnaires reported that high saturated fat intake was associated with higher triacylglycerol serum levels in Inuit individuals bearing the CC genotype of ABCA1/R219K (rs2230806), with no gender effect reported [36].
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ABCA1 p.Arg219Lys 26579206:87:201
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291 Liu H, Lin J, Zhu X, Li Y, Fan M, Zhang R, et al. Effects of R219K polymorphism of ATP-binding cassette transporter 1 gene on serum lipids ratios induced by a high-carbohydrate and low-fat diet in healthy youth.
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ABCA1 p.Arg219Lys 26579206:291:61
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