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Strategies for Enriching Variant Coverage in Candidate Disease Loci on a Multiethnic Genotyping Array

Citation

Bien, Stephanie A.; Wojcik, Genevieve L.; Zubair, Niha; Gignoux, Christopher R.; Martin, Alicia R.; Kocarnik, Jonathan M.; Martin, Lisa W.; Buyske, Steven G.; Haessler, Jeffrey; & Walker, Ryan W., et al. (2016). Strategies for Enriching Variant Coverage in Candidate Disease Loci on a Multiethnic Genotyping Array. PLOS ONE, 11(12), e0167758. PMCID: PMC5156387

Abstract

Investigating genetic architecture of complex traits in ancestrally diverse populations is imperative to understand the etiology of disease. However, the current paucity of genetic research in people of African and Latin American ancestry, Hispanic and indigenous peoples in the United States is likely to exacerbate existing health disparities for many common diseases. The Population Architecture using Genomics and Epidemiology, Phase II (PAGE II), Study was initiated in 2013 by the National Human Genome Research Institute to expand our understanding of complex trait loci in ethnically diverse and well characterized study populations. To meet this goal, the Multi-Ethnic Genotyping Array (MEGA) was designed to substantially improve fine-mapping and functional discovery by increasing variant coverage across multiple ethnicities at known loci for metabolic, cardiovascular, renal, inflammatory, anthropometric, and a variety of lifestyle traits. Studying the frequency distribution of clinically relevant mutations, putative risk alleles, and known functional variants across multiple populations will provide important insight into the genetic architecture of complex diseases and facilitate the discovery of novel, sometimes population-specific, disease associations. DNA samples from 51,650 self-identified African ancestry (17,328), Hispanic/Latino (22,379), Asian/Pacific Islander (8,640), and American Indian (653) and an additional 2,650 participants of either South Asian or European ancestry, and other reference panels have been genotyped on MEGA by PAGE II. MEGA was designed as a new resource for studying ancestrally diverse populations. Here, we describe the methodology for selecting trait-specific content for use in multi-ethnic populations and how enriching MEGA for this content may contribute to deeper biological understanding of the genetic etiology of complex disease.

URL

http://dx.doi.org/10.1371/journal.pone.0167758

Reference Type

Journal Article

Year Published

2016

Journal Title

PLOS ONE

Author(s)

Bien, Stephanie A.
Wojcik, Genevieve L.
Zubair, Niha
Gignoux, Christopher R.
Martin, Alicia R.
Kocarnik, Jonathan M.
Martin, Lisa W.
Buyske, Steven G.
Haessler, Jeffrey
Walker, Ryan W.
Cheng, Iona
Graff, Mariaelisa
Xia, Lucy
Franceschini, Nora
Matise, Tara C.
James, Regina Smith
Hindorff, Lucia A.
Le Marchand, Loic
North, Kari E.
Haiman, Christopher A.
Peters, Ulrike
Loos, Ruth J. F.
Kooperberg, Charles L.
Bustamante, Carlos D.
Kenny, Eimear E.
Carlson, Christopher S.

PMCID

PMC5156387