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Kim, Youngdae
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Diversity and scale: Genetic architecture of 2068 traits in the VA Million Veteran Program

Author(s)
Verma, AnuragHuffman, Jennifer E.Rodriguez, AlexConery, MitchellLiu, MoleiHo, Yuk-LamKim, YoungdaeHeise, David A.Guare, LindsayPanickan, Vidul AyakulangaraGarcon, HeleneLinares, FrancielCosta, LaurenGoethert, IanTipton, RyanHonerlaw, JacquelineDavies, LauraWhitbourne, StaceyCohen, JeremyPosner, Daniel C.Sangar, RahulMurray, MichaelWang, XuanDochtermann, Daniel R.Devineni, PoornimaShi, YunlingNandi, Tarak NathAssimes, Themistocles L.Brunette, Charles A.Carroll, Robert J.Clifford, RoyceDuvall, ScottGelernter, JoelHung, AdrianaIyengar, Sudha K.Joseph, JacobKember, RachelKranzler, HenryKripke, Colleen M.Levey, DanielLuoh, Shiuh-WenMerritt, Victoria C.Overstreet, CassieDeak, Joseph D.Grant, Struan F APolimanti, RenatoRoussos, PanosShakt, GabrielleSun, Yan V.Tsao, NoahVenkatesh, SananVoloudakis, GeorgiosJustice, AmyBegoli, EdmonRamoni, RachelTourassi, GeorgiaPyarajan, SaijuTsao, PhilipO'Donnell, Christopher J.Muralidhar, SumitraMoser, JenniferCasas, Juan P.Bick, Alexander G.Zhou, WeiCai, TianxiVoight, Benjamin F.Cho, KellyGaziano, J MichaelMadduri, Ravi K.Damrauer, ScottLiao, Katherine P.
Issued Date
2024-07
DOI
10.1126/science.adj1182
URI
https://scholarworks.unist.ac.kr/handle/201301/83431
Citation
SCIENCE, v.385, no.6706, pp.eadj1182
Abstract
One of the justifiable criticisms of human genetic studies is the underrepresentation of participants from diverse populations. Lack of inclusion must be addressed at-scale to identify causal disease factors and understand the genetic causes of health disparities. We present genome-wide associations for 2068 traits from 635,969 participants in the Department of Veterans Affairs Million Veteran Program, a longitudinal study of diverse United States Veterans. Systematic analysis revealed 13,672 genomic risk loci; 1608 were only significant after including non-European populations. Fine-mapping identified causal variants at 6318 signals across 613 traits. One-third (n = 2069) were identified in participants from non-European populations. This reveals a broadly similar genetic architecture across populations, highlights genetic insights gained from underrepresented groups, and presents an extensive atlas of genetic associations.
Publisher
AMER ASSOC ADVANCEMENT SCIENCE
ISSN
0036-8075

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