Title of article
Replication of Genetic Association Studies in Aortic Stenosis in Adults
Author/Authors
Gaudreault، نويسنده , , Nathalie and Ducharme، نويسنده , , Valérie and Lamontagne، نويسنده , , Maxime and Guauque-Olarte، نويسنده , , Sandra and Mathieu، نويسنده , , Patrick and Pibarot، نويسنده , , Philippe and Bossé، نويسنده , , Yohan، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2011
Pages
6
From page
1305
To page
1310
Abstract
Only a handful of studies have attempted to unravel the genetic architecture of calcific aortic valve stenosis (AS). The goal of this study was to validate genes previously associated with AS. Seven genes were assessed: APOB, APOE, CTGF, IL10, PTH, TGFB1, and VDR. Each gene was tested for a comprehensive set of single-nucleotide polymorphisms (SNPs). SNPs were genotyped in 457 patients who underwent surgical aortic valve replacement, and allele frequencies were compared to 3,294 controls. A missense mutation in the APOB gene was significantly associated with AS (rs1042031, E4181K, p = 0.00001). A second SNP located 5.6 kilobases downstream of the APOB stop codon was also associated with the disease (rs6725189, p = 0.000013). Six SNPs surrounding the IL10 locus were strongly associated with AS (0.02 >p >6.2 × 10−11). The most compelling association for IL10 was found with a promoter polymorphism (rs1800872) well known to regulate the production of the encoded anti-inflammatory cytokine. The frequency of the low-producing allele was greater in cases compared to controls (30% vs 20%, p = 6.2 × 10−11). SNPs in PTH, TGFB1, and VDR had nominal p values <0.05 but did not resist Bonferroni correction. In conclusion, this study suggests that subjects carrying specific polymorphisms in the IL10 and APOB genes are at higher risk for developing AS.
Journal title
American Journal of Cardiology
Serial Year
2011
Journal title
American Journal of Cardiology
Record number
1901488
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