ABCB1 p.Ala313Gly

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PMID: 16765145 [PubMed] Tran A et al: "Pharmacokinetics and toxicity of docetaxel: role of CYP3A, MDR1, and GST polymorphisms."
No. Sentence Comment
144 Genetic characteristics of patients (N ϭ 58) and toxicity data SNP Genotype Patients evaluable for febrile neutropenia Patients with febrile neutropenia (%) Patients evaluable for grade 3 or grade 4 neutropenia Patients with grade 3 or grade 4 neutropenia: Absolute neutrophil count Ͻ1000/␮L (%) Patients with grade 4 neutropenia: Absolute neutrophil count Ͻ500/␮L (%) CYP3A5 (A6986G) *1/*3 11 1 (9.1) 11 9 (77.8) 7 (63.6) *3/*3 47 6 (12.8) 45 35 (81.8) 21 (46.7) CYP3A4 (-A392G) *1A/*1A 54 7 (13.0) 52 41 (78.8) 26 (50.0) *1A/*1B 4 0 4 3 (75.0) 2 (50.0) MDR1 C3435T C/C 11 0 11 6 (54.5) 5 (45.5) C/T 36 6 (16.7) 35 28 (80.0) 16 (45.7) T/T 11 1 (9.1) 10 10 (100)† 7 (70.0) MDR1 G2677T G/G 25 3 (12.0) 24 17 (70.8) 11 (45.8) G/T 23 2 (8.7) 22 17 (77.3) 11 (50.0) T/T 10 2 (20.0) 10 10 (100) 6 (60.0) GSTM1 Wild type 22 2 (9.1) 21 17 (81.0) 11 (52.4) Absent allele 36 5 (13.9) 35 27 (77.1) 17 (48.6) GSTT1 Wild type 41 4 (9.8) 40 33 (82.5) 22 (55.0) Absent allele 17 3 (17.6) 16 11 (68.8) 6 (37.5) GSTP1 *A/*A 27 1 (3.7) 25 21 (84.0) 14 (56.0) *A (wild type) *A/*B 19 6 (31.6)† 19 15 (78.9) 10 (52.6) *B (A313G) *A/*C 3 0 3 2 (66.7) 1 (33.3) *C (A313G ϩ C341T) *B/*B 7 0 7 5 (71.4) 3 (42.9) *D (C341T) *B/*C 2 0 2 1 (50.0) 0 GSTM3 *A (wild type) *A/*A 40 5 (12.5) 39 29 (74.4) 19 (48.7) *B (A310C) *A/*B 18 2 (11.1) 17 15 (88.2) 9 (52.9) †P Ͻ .05. initely conclude that it is clinically relevant.
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ABCB1 p.Ala313Gly 16765145:144:1149
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ABCB1 p.Ala313Gly 16765145:144:1190
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PMID: 18095031 [PubMed] Huang MY et al: "Multiple Genetic Polymorphisms of GSTP1 313AG, MDR1 3435CC, and MTHFR 677CC highly correlated with early relapse of breast cancer patients in Taiwan."
No. Sentence Comment
4 Results: The results showed that the genotype distribution of GSTP1 A313G, MTHFR C677T, and TS 3R3R in Taiwanese subjects differed significantly from the distribution in Caucasians.
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ABCB1 p.Ala313Gly 18095031:4:68
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36 GSTP1 exon5 A313G, MDR1 C3435T, and MDR1 C3435T were restricted by BsmAI, DpnII, and HinfI, respectively.
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ABCB1 p.Ala313Gly 18095031:36:12
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54 PCR-RFLP Analysis Results of Chemotherapeutic Agent-Related Genetic Polymorphisms In our study, chemotherapeutic agent-related genetic polymorphisms are GSTP1 A313G, MDR1 C3435T, MTHFR C667T, and TS double or triple tandem repeat.
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ABCB1 p.Ala313Gly 18095031:54:159
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60 Comparison of Genotypes Distribution between Taiwanese Breast Cancer Patients and Other Races We compared the distribution of genetic polymorphisms, such as GSTP1 A313G (AA, AG, GG), MDR1 C3435T (CC, CT, TT), MTHFR C677T (CC, CT, TT), and TS tandem repeat (3R3R, 2R3R, 2R2R), in various races, including Caucasian, Korean, African American, Chinese, Japanese American, and Taiwanese subjects from our work and literature reviews.
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ABCB1 p.Ala313Gly 18095031:60:163
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62 The distribution of GSTP1 A313G genotypes in our data show significant differences from that of Caucasian (P = .001) and African American populations (P = .001)13 but no significant differences from Chinese (P = .410)14 and Korean populations (P = .242).15 The distribution of MDR1 C3435T genotypes also revealed significant differences from the Caucasian population (P = .003).16 Significantly different distributions of MTHFR C677T (CC, CT, TT) genotypes are evident when comparing our data with Caucasian (P = .001),17 Chinese (P < .0001),18 Korean (P < .0001),19 African American (P < .0001),20 and Japanese American populations (P < .0001),21 but our study is consistent with the other Taiwanese report (P = .150).22 Our study and the another Taiwanese study22 both showed that MTHFR C677T CC appeared more frequently than CT and TT, while another racial study showed that MTHFR C677T CT was the most frequent genetic polymorphism.
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ABCB1 p.Ala313Gly 18095031:62:26
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64 Characteristics of the studied polymorphisms with primer sequences and restriction enzymes Gene polymorphism Primers PCR size PCR condition Restriction enzyme GSTP1Ile105Val (A313G) [F]:5'-GTAGTTTGCCCAAGGTCAAG-3' 433 Annealing: 62°C, 20 sec BsmAI [R]:5'-AGCCACCTGAGGGGTAAG-3' MDR1Ile1145Ile (C3435T) [F]:5'-gatctgtgaactcttgttttc-3' 244 Annealing: 58°C, 20 sec DpnII [R]:5'-GAAGAGAGACTTACATTAGGC-3' MTHFRAla222Val (C677T) [F]:5'-TGGCAGGTTACCCCAAAGGC-3' 400 Annealing: 70°C, 20 sec HinfI [R]:5'-ACTGTTGCTGGGTTTTGGGG-3' TS 28 bp tandem repeat [F]:5'-GTGGCTCCTGCGTTTCCCCC-3' 240 Annealing: 72°C, 15 sec - [R]:5'-TCCGAGCCGGCCACAGGCAT-3' patients presented TS 2R3R as the most frequent genetic polymorphism.
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ABCB1 p.Ala313Gly 18095031:64:175
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68 Correlation between Early Relapse and Genotypes of Chemotherapeutic Agent-Related Genes The correlation between genetic polymorphisms (MTHFR C677T, MDR1 C3435T, GSTP1 A313G, and TS double or triple tandem repeat) and patients with or without early relapse was analyzed.
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ABCB1 p.Ala313Gly 18095031:68:167
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78 GSTP1 exon5 A313G was restricted by BsmAI and resulted in: 329bp and 104bp GSTP1 313AA fragments; 329bp, 222bp, 107bp, and 104bp GSTP1 313AG fragments; and 222bp, 104bp, and 107bp GSTP1 313GG fragments.
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ABCB1 p.Ala313Gly 18095031:78:12
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107 (%) GSTP1 A313G Sweeney13 Kim15 Sweeney13 Egan14 AA 93 (48.4) 122 (71.3) 17 (35) 723 (63.5) - - 122 (64.2) AG 80 (41.7) 44 (25.7) 27 (56) 363 (31.9) - - 65 (33.9) GG 19 (9.9) 5 (2.9) 4 (8) 53 (4.6) - - 5 (1.9) MDR1 C3435T Kafka16 CC 21 (21) - - - - - 79 (41.1) CT 57 (57) - - - - - 79 (41.1) TT 22 (22) - - - - - 34 (17.8) MTHFR C677T Campbell17 Lee19 Martin20 Shrubsole18 Chou22 Le Marchand21 CC 140 (41.8) 58 (31.2) 114 (81) 355 (34.2) 73 (51.4) 135 (42.5) 112 (58.3) CT 162 (48.4) 96 (51.6) 27 (19) 507 (48.8) 51 (35.9) 140 (44.0) 67 (34.9) TT 33 (9.8) 32 (17.2) 0 (0) 176 (17.0) 18 (12.7) 43 (13.5) 13 (6.8) TS tandem repeat Largillier24 Zhai23 3R3R 27 (32.7) - - 279 (64.6) - - 129 (67.2) 2R3R 43 (50) - - 130 (30.1) - - 61 (31.8) 2R2R 13 (17.3) - - 23 (5.3) - - 2 (1) a authorn in this table are presented with reference number (n ) and the abbreviated name of the first author in the previously reported paper.
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ABCB1 p.Ala313Gly 18095031:107:10
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120 After comparing the Taiwanese with other races with regard to genetic polymorphism, we found that the Taiwanese, Korean, and Chinese demonstrate a higher frequency of GSTP1 A313G AA than Caucasians and African Americans do. Taiwanese demonstrate a higher frequency of MTHFR C677T CC than other races do. Caucasians demonstrate a higher frequency of MDR1 C3435T CT and TS tandem repeat 2R than the Taiwanese do. The differences in genetic polymorphisms may explain the variety of chemotherapeutic agent-related responses that occur worldwide.
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ABCB1 p.Ala313Gly 18095031:120:173
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PMID: 18267032 [PubMed] Huang MY et al: "ERCC2 2251A>C genetic polymorphism was highly correlated with early relapse in high-risk stage II and stage III colorectal cancer patients: a preliminary study."
No. Sentence Comment
86 PCR-RFLP analysis and automated sequencing of GSTP1 A313GFigure 1 PCR-RFLP analysis and automated sequencing of GSTP1 A313G.
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ABCB1 p.Ala313Gly 18267032:86:118
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88 The GSTP1 exon5 A313G was restricted by BsmAI.
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ABCB1 p.Ala313Gly 18267032:88:16
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PMID: 19005482 [PubMed] Rocha V et al: "Association of drug metabolism gene polymorphisms with toxicities, graft-versus-host disease and survival after HLA-identical sibling hematopoietic stem cell transplantation for patients with leukemia."
No. Sentence Comment
14 Samples of 107 leukemia patients given HLA-identical HSCT and their respective donors were analyzed for the following candidate genes polymorphisms: P450 cytochrome family [CYP2B6*2(C64T), *3(C777A), *4(A785G), *5(C1459T), *6(G516T)] glutathione-S-transferases [GSTM1 (null), GSTT1 (null), GSTP1 (A313G)], Multidrug-resistance gene [MDR1 (C3435T)], Methylenetetrahydrofolate reductase [MTHFR (C677T, A1298C)], Vitamin D receptor [VDR (ApaI, TaqI and BsmI)].
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ABCB1 p.Ala313Gly 19005482:14:297
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53 However, both Table 2 Characteristics of genes and polymorphisms Allele polymorphisms Primers PCR 35 cycles Fragment enzyme References CYP2B6*2 50 -GCAGGGCAGTCAGACCAGGA-30 30 s 94 1C 215 bp 13 C64T 50 -GACCCCATTCGTCTGTGTCT-30 40 s 58 1C (Modified) Arg22 Cys 1 min 72 1C Hae II CYP2B6*3 50 -CACCACCCCTTCTTTCTTGC-30 30 s 94 1C 223 bp 14 C777A 50 -CCTTTTTCCTCTCCCAGACC-30 40 s 58 1C Ser259 Arg 1 min 72 1C Hae II CYP2B6*4 50 -GACAGAAGGATGAGGGAGGAA-30 30 s 94 1C 640 bp 13 A785G 50 -CTCCCTCTGTCTTTCATTGTGT-30 45 s 60 1C Lys262 Arg 1 min 72 1C StyI CYP2B6*5 50 -TGAGAATCAGTGGAAGCCATAGA-30 30 s 94 1C 1401 bp 13 C1459T 50 -TAATTTTCGATAATCTCACTCCTGC-30 40 s 58 1C Arg487 Cys 1 min 72 1C Bgl II CYP2B6*6 50 -CTTGACCTGCTGCTTCTTCC-30 30 s 94 1C 204 bp 14 G516T 50 -TCCCTCTCCGTCTCCCTG-30 40 s 58 1C Gln172 His 1 min 72 1C Bsr I GSTM1 50 -GAACTCCCTGAAAAGCTAAAGC-30 1 min 94 1C 215 bp 15 Present or null 50 -GTTGGGCTCAAATATACGGTGG-30 1 min 62 1C 1 min 72 1C GSTT1 50 -TTCCTTACTGGTCCTCACATCTC-30 1 min 94 1C 480 bp 15 Present or null 50 -TCACCGGATCATGGCCAGCA-30 1 min 62 1C 1 min 72 1C GSTP1 50 -ATCCCCAGTGACTGTGTGTT-30 30 s 94 1C 217 bp 16 A313G 50 -CTTTCTTTGTTCAGCCCCCA-30 40 s 53 1C (Modified) Ile105 Val 1 min 72 1C BsmAI MDR 50 - GATCTGTGAACTCTTGTTTTCA-30 30 s 94 1C 244 bp 17 C3435T 50 -GAAGAGAGACTTACATTAGGC-30 45 s 62 1C synonymous 1 min 72 1C Dpn II MTHFR 50 -AGGCGGTGCGGTGAGAGTG-30 50 s 94 1C 198 bp 18 C677T 50 -TGAAGGAGAAGGTGTCTGCGG GA-30 50 s 56 1C Ala222 Val 1 min 72 1C Hinf I MTHFR 50 -CTTTGGGGAGCTGAAGGACTACTAC-30 1 min 92 1C 163 bp 19 A1298C 50 -CAGTTTGTGACCATTCCGGTTTG-30 1 min 51 1C Glu429 Ala 30 s 72 1C Mbo II For each allele, the nucleotide and amino acid changes are indicated (when appropriate), together with the primer sequences, PCR conditions (35 cycles for all the amplification protocols), size of the fragment amplified and the restriction enzyme.
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ABCB1 p.Ala313Gly 19005482:53:1127
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61 of donors (%) CYP2B6*2A Cyclophosphamide CC (wt) Not described 92 (86) 91 (85) C64T CT 14 (13) 15 (14) TT 1 (1) 1 (1) CYP2B6*4 AA (wt) AG or GG trend to lower expression of the enzyme13 59 (55) 60 (56) A785G AG 38 (36) 37 (35) GG 10 (9) 10 (9) CYP2B6*5 CC (wt) CT or TT Significantly lower S-mephentytoin N-demethylase activity13 81 (76) 89 (83) C1459T CT 25 (23) 16 (15) TT 1 (1) 2 (2) CYP2B6*6 GG (wt) GT or TT decreased protein level and impact on CY 4-hydroxylation.8 Enhance 7-ethoxycoumarin O-deethylase activity14 61 (57) 63 (59) G516T1 GT 36 (34) 35 (33) A785G TT 10 (9) 9 (9) GSTM1* Null Reduced or no enzyme activity and therefore may be unable to eliminate electrophilic carcinogens24 61 (57) 60 (56) Busulfan Non-null 46 (43) 47 (44) GSTT1* Melphalan Null 20 (19) 27 (25) Cyclophosphamide Non-null 87 (81) 80 (75) GSTP1 AA (wt) Reduced ability to detoxify chemotherapeutic agents thereby increasing the effective dose of the drug within the cell.25 46 (43) 52 (49) A313G GA 53 (49) 42 (39) GG 8 (8) 13 (12) MTHFR Methotrexate CC (wt) It leads to a thermolabile variant of the enzyme and it is associated with reduced enzyme activity (70% for TT and 40% for CT), increased homocysteine levels18 45 (42) 41 (38) C677T CT 53 (50) 51 (48) TT 9 (8) 15 (14) MTHFR AA (wt) Reduced enzyme activity without increasing homocysteine levels.26 50 (47) ND A1298C AC 56 (52) ND CC 1 (1) ND MDR-1 Cyclosporine A C3435T Tracolimus CC (wt) CsA oral clearance is significantly higher in subjects who carried at least one T allele27 30 (28) 29 (27) CT 56 (52) 56 (52) TT 21 (20) 22 (21) VDR apaI aa Increased femoral and vertebral bone density.28 25 (23) 20 (19) Aa 57 (53) 56 (52) AA 25 (23) 31 (29) VDR taqI Cyclosporine A** tt Intervertebral disc degeneration in males29 Periodontal disease30 and infections31 13 (12) 15 (14) Tt 46 (43) 52 (49) Immunoregulatory activities of 1a,25-(OH)2D3 TT 48 (45) 40 (37) VDR bsmI bb Increased femoral and vertebral bone density.28 50 (47) 40 (37) Bb 34 (32) 41 (38) BB 23 (21) 26 (24) Abbreviations: ND, not done; wt, wild type.
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ABCB1 p.Ala313Gly 19005482:61:977
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105 In univariate analysis we found that donor GSTP1 (A313G) genotype (GG or GA) was associated with higher incidence of chronic GvHD.
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ABCB1 p.Ala313Gly 19005482:105:50
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PMID: 22761669 [PubMed] Yin JY et al: "Meta-analysis on pharmacogenetics of platinum-based chemotherapy in non small cell lung cancer (NSCLC) patients."
No. Sentence Comment
4 MDR1 C3435T (OR = 1.97, 95% CI: 1.11-3.50, P = 0.02), G2677A/T (OR = 2.61, 95% CI: 1.44-4.74, P = 0.002) and GSTP1 A313G (OR = 0.32, 95% CI: 0.17-0.58, P = 0.0002) were significantly correlated with platinum-based chemotherapy in Asian NSCLC patients.
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ABCB1 p.Ala313Gly 22761669:4:115
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5 Conclusion: Attention should be paid to MDR1 C3435T, G2677A/T and GSTP1 A313G for personalized chemotherapy treatment for NSCLC patients in Asian population in the future.
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ABCB1 p.Ala313Gly 22761669:5:72
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23 The same situation exists for GSTP1 A313G [9-11].
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ABCB1 p.Ala313Gly 22761669:23:36
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96 Genes Polymorphisms NCBI SNP ID Allele Responders Non-responders References ERCC1 C354T rs11615 C 210 285 [6-8,22,59-64] (Asn118Asn) T 199 308 C8092A rs3212986 C 85 87 [9,22,65] A 85 93 XPD G934A rs1799793 G 114 174 [7-9,59,63,66-68] (Asp312Asn) A 93 181 A2251C rs13181 A 259 528 [7-9,59,63,65-70] (Lys751Gln) C 172 372 XPG T138C rs1047768 C 13 20 [23,24] (His46His) T 41 131 XRCC1 G1196A rs25487 G 60 110 [9,23,68,69] (Arg399Gln) A 71 152 MDR1 C3435T rs1045642 C 49 46 [8,32,60,63,71] (Ile1145Ile) T 88 141 G2677T/A rs2032582 G 31 22 [32,60,71] (Ala893Ser/Thr) T/A 44 67 GSTP1 A313G rs1695 A 64 181 [9-11,72] (Ile105Val) G 67 113 GSTM1 Deletion NR presence 31 63 [9,62] deletion 38 40 RRM1 C-37A NR C 87 123 [8,36,63] A 65 92 NR: not reported.
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ABCB1 p.Ala313Gly 22761669:96:578
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143 GSTP1 A313G was the most widely studied polymorphism.
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ABCB1 p.Ala313Gly 22761669:143:6
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148 The result showed no association between GSTP1 A313G and platinum-based chemotherapy (OR = 0.61, 95% CI: 0.2921.28, P = 0.19) (Figure 6A).
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ABCB1 p.Ala313Gly 22761669:148:47
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156 As showed in Figure 6 B and C, GSTP1 A313G was only significantly associated with drug response in Asian population.
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ABCB1 p.Ala313Gly 22761669:156:37
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167 The results showed that MDR1 C3435T, G2677A/T and GSTP1 A313G were significantly correlated with platinum-based chemotherapy in the Asian NSCLC patients.
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ABCB1 p.Ala313Gly 22761669:167:56
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187 Another polymorphism found to be significantly correlated with drug response was GSTP1 A313G, which is a non-synonymous SNP located in exon 5 [33].
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ABCB1 p.Ala313Gly 22761669:187:87
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190 Previous study showed that GSTP1 A313G resulted in reduced glutathione conjugating ability [33].
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ABCB1 p.Ala313Gly 22761669:190:33
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210 Meta-analysis of association between GSTP1 A313G and platinum-based chemotherapy in overall (A), Asian (B) and Caucasian (C) NSCLC patients.
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ABCB1 p.Ala313Gly 22761669:210:43
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223 Although most of the separately analyzed results were consistent with overall population, two polymorphisms (MDR1 C3435T and GSTP1 A313G) showed ethnic difference.
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ABCB1 p.Ala313Gly 22761669:223:131
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276 In conclusion, we identified that MDR1 C3435T, G2677A/T and GSTP1 A313G were significantly correlated with platinum-based chemotherapy in Asian NSCLC patients.
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ABCB1 p.Ala313Gly 22761669:276:66
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137 Authors Year Ethnicity (Country) Number of patients Disease stageGenotyping method Chemotherapeutic drugs Genes and polymorphism Reference Camps et al. 2003 Caucasian (Spain) 38 IIIB-IV Direct sequencing Cisplatin/Gemcitabine XPD: G934A XPD: A2251C [67] Isla et al. 2004 Caucasian (Spain) 62 IIIB-IV TaqMan genotyping assay Cisplatin/Docetaxel ERCC1: C354T MDR1: C3435T RRM1: A-37C XPD: G934A XPD: A2251C [8] Ryu et al. 2004 Asian (Korea) 108 IIIB-IV SNaPShot assay Platinum-based chemotherapy ERCC1: C354T XPD: G934A XPD: A2251C [59] Booten et al. 2006 Caucasian (UK) 89 III-IV Direct sequencing Platinum-based chemotherapy GSTP1:A313G [11] Booton et al. 2006 Caucasian (UK) 89 III-IV PCR-RFLP Direct sequencing Platinum-based chemotherapy XPD: G934A XPD: A2251C [66] Su et al. 2007 Asian (China) 76 IIIA-IV TaqMan genotyping assay Platinum-based chemotherapy ERCC1: C354T [6] Giachino et al. 2007 Caucasian (Italy) 188 IIIA-IV PCR-RFLP Platinum-based chemotherapy XRCC1: G1196A XPD: A2251C [69] Tibaldi et al. 2008 Caucasian (Italy) 65 IIIB-IV TaqMan genotyping assay Cisplatin/Gemcitabine ERCC1: C354T XPD: G934A XPD: A2251C [7] Pan et al. 2008 Asian (China) 69 IIIB-IV PCR-RFLP Cisplatin/Vinorelbine MDR1: C3435T MDR1: G2677A/T [71] Yu et al. 2008 Asian (China) 117 NR Direct sequencing Carboplatin/Etoposide ERCC1: C354T ERCC1: C8092A [22] Kalikaki et al. 2009 Caucasian (Greece) 119 IIIA-IV PCR-RFLP Direct sequencing Platinum-based chemotherapy ERCC1: C354T ERCC1: C8092A GSTP1: A313G GSTM1: deletion XPD: G934A XPD: A2251C XRCC1: G1196A [9] Feng et al. 2009 Asian (China) 214 IIB-IV PCR-RFLP Platinum-based chemotherapy RRM1: A-37C [36] Yao et al. 2009 Asian (China) 102 IIIB-IV PCR-RFLP Platinum-based chemotherapy XRCC1: G1196A [68] Sun et al. 2009 Asian (China) 90 IV 3-D polyacrylamide gel-based DNA microarray Platinum-based chemotherapy XRCC1: G1196A [23] Pan et al. 2009 Asian (China) 54 IIIB-IV PCR-RFLP Cisplatin/Docetaxel MDR1: C3435T MDR1: G2677A/T [32] Zhou et al. 2010 Asian (China) 130 IIIB-IV TaqMan genotyping assay Platinum-based chemotherapy ERCC1: C354T [61] Chen et al. 2010 Asian (China) 95 IIIB-IV Ligase detection reactions (LDR) Platinum-based chemotherapy ERCC1: C354T MDR1: C3435T MDR1: G2677A/T [60] Sun et al. 2010 Asian (China) 113 IIIA-IV 3-D polyacrylamide gel-based DNA microarray Platinum-based chemotherapy GSTP1: A313G [10] Li et al. 2010 Asian (China) 115 IIIB-IV 3-D polyacrylamide gel-based DNA microarray Platinum-based chemotherapy ERCC1: C354T XPD: A2251C [65] Vinolas et al. 2011 Caucasian (Spain) 94 IIIB-IV 59 nuclease allelic discrimination assay Cisplatin/Vinorelbine ERCC1: C354T XPD: G934A XPD: A2251C MDR1: C3435T RRM1: A-37C [63] Zhou et al. 2011 Asian (China) 111 IV Direct sequencing Platinum-based chemotherapy GSTP1: A313G [72] Li et al. 2012 Asian (China) 58 NR PCR-RFLP Platinum-based chemotherapy GSTM1:deletion [62] Chen et al. 2012 Asian (China) 355 IIIB-IV TaqMan genotyping assay Platinum-based chemotherapy XPD: A2251C [70] Cheng et al. 2012 Asian (China) 142 IIIB-IV Direct sequencing Platinum-based chemotherapy ERCC1: C354T [64] NR: not reported.
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ABCB1 p.Ala313Gly 22761669:137:1486
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ABCB1 p.Ala313Gly 22761669:137:2356
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ABCB1 p.Ala313Gly 22761669:137:2779
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144 GSTP1 A313G was the most widely studied polymorphism.
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ABCB1 p.Ala313Gly 22761669:144:6
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149 The result showed no association between GSTP1 A313G and platinum-based chemotherapy (OR = 0.61, 95% CI: 0.2921.28, P = 0.19) (Figure 6A).
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ABCB1 p.Ala313Gly 22761669:149:47
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157 As showed in Figure 6 B and C, GSTP1 A313G was only significantly associated with drug response in Asian population.
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ABCB1 p.Ala313Gly 22761669:157:37
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168 The results showed that MDR1 C3435T, G2677A/T and GSTP1 A313G were significantly correlated with platinum-based chemotherapy in the Asian NSCLC patients.
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ABCB1 p.Ala313Gly 22761669:168:56
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188 Another polymorphism found to be significantly correlated with drug response was GSTP1 A313G, which is a non-synonymous SNP located in exon 5 [33].
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ABCB1 p.Ala313Gly 22761669:188:87
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191 Previous study showed that GSTP1 A313G resulted in reduced glutathione conjugating ability [33].
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ABCB1 p.Ala313Gly 22761669:191:33
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211 Meta-analysis of association between GSTP1 A313G and platinum-based chemotherapy in overall (A), Asian (B) and Caucasian (C) NSCLC patients.
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ABCB1 p.Ala313Gly 22761669:211:43
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224 Although most of the separately analyzed results were consistent with overall population, two polymorphisms (MDR1 C3435T and GSTP1 A313G) showed ethnic difference.
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ABCB1 p.Ala313Gly 22761669:224:131
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277 In conclusion, we identified that MDR1 C3435T, G2677A/T and GSTP1 A313G were significantly correlated with platinum-based chemotherapy in Asian NSCLC patients.
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ABCB1 p.Ala313Gly 22761669:277:66
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PMID: 15261376 [PubMed] Robert J et al: "[Pharmacogenetics and pharmacogenomics of cancers]."
No. Sentence Comment
88 Un polymorphisme g&#e9;n&#e9;tique a &#e9;t&#e9; r&#e9;cemment identifi&#e9; [20] : il s`agit d`une mutation ponctuelle A313G conduisant &#e0; une substitution Ile105val et &#e0; une diminution de l`activit&#e9; de l`enzyme. Dans une &#e9;tude sur 107 patients trait&#e9;s pour cancer colorectal par 5-FU et oxaliplatine, les dix homozygotes porteurs de la variation ont pr&#e9;sent&#e9; une survie trois fois sup&#e9;rieure &#e0; la survie des homozygotes &#ab; sauvages &#bb;.
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ABCB1 p.Ala313Gly 15261376:88:120
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PMID: 22310978 [PubMed] Ji M et al: "Polymorphisms in genes involved in drug detoxification and clinical outcomes of anthracycline-based neoadjuvant chemotherapy in Chinese Han breast cancer patients."
No. Sentence Comment
17 The polymorphism of GSTP1 A313G and null variants of GSTM1 and GSTT1 that lead to the diminished or abolished enzyme activity have been associated with increased drug treatment benefit in some cancer patients.5,7 In addition to these enzymes, drug transporters are increasing recognized to be important to drug disposition and response.
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ABCB1 p.Ala313Gly 22310978:17:26
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48 The combined effects of GSTP1 A313G and MDR1 C3435T were greater than those for either polymorphism alone, and an increased response with decreasing number of adverse genotypes was observed (14.3 vs. 66.0 vs. 82.2%; p = 0.000).
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ABCB1 p.Ala313Gly 22310978:48:30
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84 The combined adverse genotypes in GSTP1 A313G and MDR1 C3435T and clinical response to anthracycline-based chemotherapy Adverse genotype No. Clinical response x2 p RR (CI 95%)a CR + PR (%) SD + PD (%) GSTP1 313AA and MDR1 3435TT 0 45 37 (82.2) 5 (17.8) 26.223 0.000 1.0 (Ref.) 1 (AA or TT) 94 62 (66.0) 32 (34.0) 3.82 (1.37-10.66) 2 (AA + TT) 14 2 (14.3) 12 (85.7) 44.40 (7.61-259.20) a The relative risk (RR) of not responding to treatment with a 95% confidence interval.
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ABCB1 p.Ala313Gly 22310978:84:40
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102 Volume 13 Issue 5 Single nucleotide polymorphisms (SNPs) of MnSOD (T47C), CAT (C-262T), GSTP1 (A313G) and the deletion polymorphisms of GSTM1 and GSTT1 were determined using allele-specific oligonucleotide ligation reaction (ASOLR) and a multiplex PCR developed in our laboratory, respectively.28 ASOLR was a technique for multiplex genetic typing.
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ABCB1 p.Ala313Gly 22310978:102:95
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103 The assay was implemented via three steps: a triplex PCR that resulted in the amplified target sequences with MnSOD T47C, CAT C-262T and GSTP1 A313G loci, a triplex allele-specific oligonucleotide probe ligation reaction that generates the ligation between perfectly matched probes at their junctions while no ligation occurred between mismatched ones and an analysis of genotype-specific ligation products by both fluorescence and size after electrophoresis on ABI PRISM 377 DNA sequencer.28,29 MDR1 C3435T, G2677T/A and C1236T polymorphisms were analyzed by PCR-RFLP as described by Ni et al. PCR reaction was performed on a DNA thermal cycler (Bio-Rad iCycle).
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ABCB1 p.Ala313Gly 22310978:103:143
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PMID: 23357434 [PubMed] Gong LL et al: "Genetic risk factors for glucocorticoid-induced osteonecrosis: a meta-analysis."
No. Sentence Comment
82 Gene rs No./genotype Number of cases/ controls Case Control Number of studies Refs. 11 12 22 11 12 22 1 PAI-1 -675 4G/5G 108/917 50 46 12 225 455 237 4 [8,10,24,36] rs6092 89/281 59 29 1 240 41 0 2 [31,35] 2 MTHFR C677T 103/537 61 31 11 324 168 45 5 [10,23-25,31] A1298C 25/39 8 15 2 16 21 2 1 [23] 3 Factor V Leiden N/A 26/39 24 2 0 35 4 0 2 [10,25] 4 Prothrombin G20210A 26/39 26 0 0 35 4 0 2 [10,25] 5 CBP rs3751845 113/246 68 23 22 105 36 105 2 [14,29] 6 ABCB1 C3435T 148/462 83 55 10 210 171 81 6 [14,21,23,30,31,34] G2677T/A 136/268 48 45 13 82 124 62 4 [21,23,30,34] 7 TYMS Enhancer repeat 25/39 5 13 7 16 19 4 2 [23,31] 8 VDR rs2228570 T/C 68/299 42 26 187 112 2 [23,31] Intron 8 G/A 25/39 12 8 5 14 18 7 1 [23] 9 ApoB C7623T 66/244 54 12 230 14 2 [12,14] G12619A 34/123 33 1 112 11 1 [12] 10 ApoA1 -75G/A 33/120 22 11 86 34 1 [12] C83T 33/120 29 4 106 14 1 [12] 11 LRP5 rs2306862 T/C 40/212 18 22 113 99 1 [31] 12 NR3C1 A1220G 25/39 25 0 0 38 1 0 1 [23] rs6196 T/C 34/123 31 3 0 115 8 0 1 [29] rs2282800 34/123 1 2 31 8 22 93 1 [29] 13 SREBP-2 T8408C 56/270 16 31 9 77 138 55 1 [32] G342T 54/422 32 20 2 241 149 32 1 [32] G414A 56/271 22 30 4 132 120 19 1 [32] G1667A 56/266 22 26 8 116 121 29 1 [32] 14 CYP3A4 /1B A/G 25/39 23 2 0 34 2 3 1 [23] rs3735451 34/123 24 9 1 77 46 0 1 [29] 15 CYP2D6 EM/IM/PM 26/54 21 5 0 45 9 0 1 [22] 16 CYP2C19 EM/PM 54/26 46 0 8 23 0 3 1 [22] 17 CYP3A5 /3 G/A 25/39 20 5 0 29 7 3 1 [23] 18 UGT1A1 /28 25/39 11 9 5 14 20 5 1 [23] 19 GSTM1 257 bp deletion (non-null/null) 25/39 14 11 26 13 1 [23] 20 GSTP1 A313G 25/39 5 16 4 13 19 7 1 [23] 21 GSTT1 Deletion (non-null/null) 24/39 18 6 32 7 1 [23] 22 TMPT /1//3 25/39 22 3 0 37 2 0 1 [23] 23 RFC G80A 25/39 10 11 4 12 18 9 1 [23] 24 NOS 27 bp repeat polymorphism in intron 4 29/103 0 3 26 0 5 98 1 [26] D298E 29/103 0 4 25 0 20 83 1 [26] 25 HIF C2755A 59/237 20 29 10 78 117 42 1 [27] T41224C 56/236 28 25 3 135 84 17 1 [27] C45319T 59/236 52 7 0 219 16 1 1 [27] C51610T 56/234 35 18 3 156 68 10 1 [27] 26 PPAR A796G 55/330 36 16 3 223 95 12 1 [28] C34G 54/328 51 3 0 296 32 0 1 [28] C82466T 55/333 39 15 1 242 85 6 1 [28] 27 NcoA2 rs2272670 C/T 34/123 22 11 1 62 50 11 1 [29] 28 BGLAP rs1800247 T/C 36/203 32 4 183 20 1 [31] 29 ESR1 rs2234693 C/T 32/190 13 19 95 95 1 [31] 30 PTH rs6254 A/G 44/229 19 25 115 114 1 [31] 31 PTHR rs1138518 C/T 35/213 16 19 117 96 1 [31] 32 ACP5 rs2229531 A/G 43/222 5 38 31 191 1 [31] rs2305799 T/C 43/235 8 35 54 181 1 [31] 33 TNFa T-1031C 15/35 6 8 1 28 7 0 1 [33] C-863A 16/37 9 7 0 33 4 0 1 [33] C-857T 16/37 12 4 0 26 11 0 1 [33] A-572C 16/37 16 0 0 36 1 0 1 [33] G-308A 16/37 14 2 0 32 4 1 1 [33] G-238A 16/37 13 3 0 33 4 0 1 [33] 34 VEGF A-2575C 74/160 5 24 45 9 68 83 1 [37] A-1154G 74/160 0 11 63 6 46 108 1 [37] C-634G 136/380 35 66 35 65 198 117 2 [37,39] C405G 74/160 19 33 22 25 84 51 1 [37] 35 Hapatic lipase rs59644784 A/G 143/96 20 69 54 16 43 37 1 [38] rs1800588 C/T 143/96 58 68 17 41 42 13 1 [38] 11 Indicate wild type genotype, 12 indicate heterozygous genotype, 22 indicate mutant genotype.
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ABCB1 p.Ala313Gly 23357434:82:1545
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