CDH13 promoter SNPs with pleiotropic effect on cardiometabolic parameters represent methylation QTLs

被引:0
|
作者
Margus Putku
Mart Kals
Rain Inno
Silva Kasela
Elin Org
Viktor Kožich
Lili Milani
Maris Laan
机构
[1] Institute of Molecular and Cell Biology,Human Molecular Genetics Group
[2] University of Tartu,Estonian Genome Center
[3] University of Tartu,Institute of Mathematical Statistics
[4] University of Tartu,Department of Biotechnology
[5] Institute of Molecular and Cell Biology,Department of Medicine/Division of Cardiology
[6] University of Tartu,Institute of Inherited Metabolic Diseases
[7] David Geffen School of Medicine,undefined
[8] UCLA,undefined
[9] Charles University,undefined
[10] First Faculty of Medicine,undefined
来源
Human Genetics | 2015年 / 134卷
关键词
Methylation Level; Adiponectin Level; CDH13 Gene; High Molecular Weight Adiponectin; CDH13 Promoter;
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学科分类号
摘要
CDH13 encodes T-cadherin, a receptor for high molecular weight (HMW) adiponectin and low-density lipoprotein, promoting proliferation and migration of endothelial cells. Genome-wide association studies have mapped multiple variants in CDH13 associated with cardiometabolic traits (CMT) with variable effects across studies. We hypothesized that this heterogeneity might reflect interplay with DNA methylation within the region. Resequencing and EpiTYPER™ assay were applied for the HYPertension in ESTonia/Coronary Artery Disease in Czech (HYPEST/CADCZ; n = 358) samples to identify CDH13 promoter SNPs acting as methylation Quantitative Trait Loci (meQTLs) and to investigate their associations with CMT. In silico data were extracted from genome-wide DNA methylation and genotype datasets of the population-based sample Estonian Genome Center of the University of Tartu (EGCUT; n = 165). HYPEST–CADCZ meta-analysis identified a rare variant rs113460564 as highly significant meQTL for a 134-bp distant CpG site (P = 5.90 × 10−6; β = 3.19 %). Four common SNPs (rs12443878, rs12444338, rs62040565, rs8060301) exhibited effect on methylation level of up to 3 neighboring CpG sites in both datasets. The strongest association was detected in EGCUT between rs8060301 and cg09415485 (false discovery rate corrected P value = 1.89 × 10−30). Simultaneously, rs8060301 showed association with diastolic blood pressure, serum high-density lipoprotein and HMW adiponectin (P < 0.005). Novel strong associations were identified between rare CDH13 promoter meQTLs (minor allele frequency <5 %) and HMW adiponectin: rs2239857 (P = 5.50 × 10−5, β = −1,841.9 ng/mL) and rs77068073 (P = 2.67 × 10−4, β = −2,484.4 ng/mL). Our study shows conclusively that CDH13 promoter harbors meQTLs associated with CMTs. It paves the way to deeper understanding of the interplay between DNA variation and methylation in susceptibility to common diseases.
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页码:291 / 303
页数:12
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