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Genome-wide characterization of shared and distinct genetic components that influence blood lipid levels in ethnically diverse human populations

  • Marc A. Coram
  • , Qing Duan
  • , Thomas J. Hoffmann
  • , Timothy Thornton
  • , Joshua W. Knowles
  • , Nicholas A. Johnson
  • , Heather M. Ochs-Balcom
  • , Timothy A. Donlon
  • , Lisa W. Martin
  • , Charles B. Eaton
  • , Jennifer G. Robinson
  • , Neil J. Risch
  • , Xiaofeng Zhu
  • , Charles Kooperberg
  • , Yun Li
  • , Alex P. Reiner
  • , Hua Tang
  • Stanford University
  • University of North Carolina at Chapel Hill
  • University of California at San Francisco
  • University of Washington
  • Alphabet Inc.
  • Kuakini Health System
  • University of Hawai'i at Mānoa
  • George Washington University
  • Brown University
  • University of Iowa
  • Kaiser Permanente
  • Case Western Reserve University
  • Fred Hutchinson Cancer Research Center

Research output: Contribution to journalArticlepeer-review

100 Scopus citations

Abstract

Blood lipid concentrations are heritable risk factors associated with atherosclerosis and cardiovascular diseases. Lipid traits exhibit considerable variation among populations of distinct ancestral origin as well as between individuals within a population. We performed association analyses to identify genetic loci influencing lipid concentrations in African American and Hispanic American women in the Women's Health Initiative SNP Health Association Resource. We validated one African-specific high-density lipoprotein cholesterol locus at CD36 as well as 14 known lipid loci that have been previously implicated in studies of European populations. Moreover, we demonstrate striking similarities in genetic architecture (loci influencing the trait, direction and magnitude of genetic effects, and proportions of phenotypic variation explained) of lipid traits across populations. In particular, we found that a disproportionate fraction of lipid variation in African Americans and Hispanic Americans can be attributed to genomic loci exhibiting statistical evidence of association in Europeans, even though the precise genes and variants remain unknown. At the same time, we found substantial allelic heterogeneity within shared loci, characterized both by population-specific rare variants and variants shared among multiple populations that occur at disparate frequencies. The allelic heterogeneity emphasizes the importance of including diverse populations in future genetic association studies of complex traits such as lipids; furthermore, the overlap in lipid loci across populations of diverse ancestral origin argues that additional knowledge can be gleaned from multiple populations.

Original languageEnglish
Pages (from-to)904-916
Number of pages13
JournalAmerican Journal of Human Genetics
Volume92
Issue number6
DOIs
StatePublished - Jun 6 2013

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