Integromic analysis of genetic variation and gene expression identifies networks for cardiovascular disease phenotypes
Author(s)
Date
2015Source Title
Circulation
Publisher
Lippincott Williams & Wilkins
Volume
131
Issue
6
Pages
536 - 549
Language
English
Type
ArticleItem Usage Stats
268
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views
258
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downloads
Abstract
BACKGROUND - : Cardiovascular disease (CVD) reflects a highly coordinated complex of traits. Although genome-wide association studies have reported numerous single nucleotide polymorphisms (SNPs) to be associated with CVD, the role of most of these variants in disease processes remains unknown. METHODS AND RESULTS - : We built a CVD network using 1512 SNPs associated with 21 CVD traits in genome-wide association studies (at P≤5×10) and cross-linked different traits by virtue of their shared SNP associations. We then explored whole blood gene expression in relation to these SNPs in 5257 participants in the Framingham Heart Study. At a false discovery rate <0.05, we identified 370 cis-expression quantitative trait loci (eQTLs; SNPs associated with altered expression of nearby genes) and 44 trans-eQTLs (SNPs associated with altered expression of remote genes). The eQTL network revealed 13 CVD-related modules. Searching for association of eQTL genes with CVD risk factors (lipids, blood pressure, fasting blood glucose, and body mass index) in the same individuals, we found examples in which the expression of eQTL genes was significantly associated with these CVD phenotypes. In addition, mediation tests suggested that a subset of SNPs previously associated with CVD phenotypes in genome-wide association studies may exert their function by altering expression of eQTL genes (eg, LDLR and PCSK7), which in turn may promote interindividual variation in phenotypes. CONCLUSIONS - : Using a network approach to analyze CVD traits, we identified complex networks of SNP-phenotype and SNP-transcript connections. Integrating the CVD network with phenotypic data, we identified biological pathways that may provide insights into potential drug targets for treatment or prevention of CVD.
Keywords
Regulation networkCardiovascular disease
Gene expression/regulation
Genetic variation
Adult
Cardiovascular disease
Cardiovascular risk
Cross linking
Disease course
Female
Gene expression
Genetic analysis
Genetic association
Genetic variability
Human
Integromic analysis
Major clinical study
Male
Middle aged
Phenotype
Priority journal
Quantitative trait locus
Single nucleotide polymorphism
Permalink
http://hdl.handle.net/11693/24492Published Version (Please cite this version)
http://dx.doi.org/10.1161/CIRCULATIONAHA.114.010696Collections
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