ABCA1 p.Arg1901Ser

[switch to full view]
Comments [show]
Publications
PMID: 19019193 [PubMed] Pisciotta L et al: "Severe HDL deficiency due to novel defects in the ABCA1 transporter."
No. Sentence Comment
200 We previously reported a 16-year-old girl with severe HDL deficiency due to ABCA1 mutations (p.H160FsX173/p.R1901S) who had a mild mental retardation and radial-ulnar synostosis [18].
X
ABCA1 p.Arg1901Ser 19019193:200:108
status: NEW
Login to comment

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
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.
X
ABCA1 p.Arg1901Ser 16429166:48:904
status: NEW
X
ABCA1 p.Arg1901Ser 16429166:48:1079
status: NEW
Login to comment

PMID: 15019541 [PubMed] Pisciotta L et al: "Familial HDL deficiency due to ABCA1 gene mutations with or without other genetic lipoprotein disorders."
No. Sentence Comment
2 Two mutations (R557X and H160FsX173) were predicted to generate short truncated proteins; two mutations (E284K and Y482C) were located in the first extracellular loop and two (R1901S and Q2196H) in the C-terminal cytoplasmic domain of ABCA1.
X
ABCA1 p.Arg1901Ser 15019541:2:176
status: NEW
Login to comment

72 The proband of Family 6 was a compound heterozygote for two ABCA1 mutations (H160FsX173 and R1901S).
X
ABCA1 p.Arg1901Ser 15019541:72:92
status: NEW
Login to comment

127 Transversion c.5703 A > C in exon 42 (R1901S) As this mutation introduces a Bsm I restriction site, a 223 bp PCR fragment encompassing exon 42 was digested with Bsm I (Roche Diagnostics GmbH, Mannheim, Germany).
X
ABCA1 p.Arg1901Ser 15019541:127:38
status: NEW
Login to comment

164 II.2 W/W 43 M 28.0 5.10 3.70 0.96 0.80 104 98 ε3ε4 III.3 M2/W 9 M - 3.00 1.94 0.75 0.70 92 52 ε3ε4 Family 4 II.1 M4/W 62 M 23.3 4.45 2.71 0.72 2.21 102 92 ε3ε3 +++ Family 5 II.1a M5/W 59 M 36.7 7.16 6.02 0.52 1.71 81 133 ε3ε4 +++ III.1a W/W 33 F 21.8 7.52 5.02 1.99 1.13 162 112 ε4ε4 III.2 M5/W 31 F 22.8 4.68 3.28 0.85 1.18 92 82 ε3ε4 III.3 M5/W 31 F 24.4 4.00 2.74 0.90 0.78 97 72 ε3ε4 Family 6 I.2 M6/W 53 F 40.2 4.76 3.00 1.16 1.31 104 81 ε3ε3 II.1 W/W 41 M 27.5 6.54 4.35 1.19 2.20 141 148 ε3ε4 II.2 M6/W 39 M 26.2 3.57 2.44 0.77 0.77 93 71 ε3ε4 II.3 M6/W 37 F 21.3 4.44 2.63 0.76 2.30 85 89 ε3ε4 II.4 M7/W 37 M 18.8 3.67 2.43 1.00 0.50 89 57 ε3ε3 III.1 M6/M7 16 F 25.4 3.33 2.45 0.18 1.55 12 102 ε3ε3 III.2 M7/W 10 F 14.2 2.66 1.34 0.98 0.76 103 38 ε3ε3 W, ABCA1 wild-type allele; M, ABCA1 mutant allele: M1 (E284K); M2 (N1800H); M3 (Y482C); M4 (Q2196H); M5 (R557X); M6 (H160FsX173); M7 (R1901S); ND: not determined.
X
ABCA1 p.Arg1901Ser 15019541:164:1034
status: NEW
X
ABCA1 p.Arg1901Ser 15019541:164:1062
status: NEW
Login to comment

184 position 173 (c.479 del A, H160FsX173); (ii) c.5703 A > C transversion (R1901S) in exon 42 (Fig. 5).
X
ABCA1 p.Arg1901Ser 15019541:184:72
status: NEW
Login to comment

200 of our series (Families 2 and 3), we are tempted to suggest that N1800H might be a recurrent mutation.
X
ABCA1 p.Arg1901Ser 15019541:200:230
status: NEW
Login to comment

201 The novel mutations we identified included: (a) one non-sense (R557X) and one frameshift (H160FsX173) mutation, both predicted to encode short peptides presumably devoid of any function; (b) four missense mutations (E284K, Y482C, R1901S and Q2196H) resulting in non-homologous amino acid substitutions.
X
ABCA1 p.Arg1901Ser 15019541:201:230
status: NEW
Login to comment

208 Interestingly, a cysteine for arginine substitution in the first extracellular loop (R230C) was reported in three Oji-Cree subjects with very low plasma HDL levels [11].
X
ABCA1 p.Arg1901Ser 15019541:208:34
status: NEW
Login to comment

209 The other two missence mutations (R1901S and Q2196H) we found in our patients are located in the C-terminal cytoplasmic region close to the NBD-2 domain.
X
ABCA1 p.Arg1901Ser 15019541:209:34
status: NEW
Login to comment