Genome-wide association study of peripheral artery disease in the Million Veteran Program

被引:0
|
作者
Derek Klarin
Julie Lynch
Krishna Aragam
Mark Chaffin
Themistocles L. Assimes
Jie Huang
Kyung Min Lee
Qing Shao
Jennifer E. Huffman
Pradeep Natarajan
Shipra Arya
Aeron Small
Yan V. Sun
Marijana Vujkovic
Matthew S. Freiberg
Lu Wang
Jinbo Chen
Danish Saleheen
Jennifer S. Lee
Donald R. Miller
Peter Reaven
Patrick R. Alba
Olga V. Patterson
Scott L. DuVall
William E. Boden
Joshua A. Beckman
J. Michael Gaziano
John Concato
Daniel J. Rader
Kelly Cho
Kyong-Mi Chang
Peter W. F. Wilson
Christopher J. O’Donnell
Sekar Kathiresan
Philip S. Tsao
Scott M. Damrauer
机构
[1] Boston VA Healthcare System,Center for Genomic Medicine
[2] Massachusetts General Hospital,Program in Medical and Population Genetics
[3] Harvard Medical School,Department of Surgery
[4] Broad Institute of MIT and Harvard,VA Informatics and Computing Infrastructure, Department of Veterans Affairs
[5] Massachusetts General Hospital,Center for Healthcare Organization and Implementation Research
[6] Salt Lake City Health Care System,Department of Medicine
[7] University of Massachusetts College of Nursing & Health Sciences,Massachusetts Veterans Epidemiology Research and Information Center
[8] Edith Nourse Rogers Memorial VA Hospital,Department of Health Law, Policy & Management
[9] VA Palo Alto Health Care System,Cardiovascular Research Center
[10] Stanford University School of Medicine,Department of Surgery
[11] VA Boston Healthcare System,Department of Medicine
[12] Boston University School of Public Health,Department of Epidemiology
[13] Massachusetts General Hospital,Department of Biomedical Informatics
[14] Stanford University School of Medicine,Department of Biostatistics, Epidemiology, and Informatics
[15] Corporal Michael J. Crescenz VA Medical Center,Center for Healthcare Organization and Implementation Research
[16] Yale University School of Medicine,Division of Epidemiology, Department of Internal Medicine
[17] Atlanta VA Health Care System,Cardiovascular Division
[18] Emory University Rollins School of Public Health,Department of Medicine
[19] Emory University School of Medicine,Clinical Epidemiology Research Center
[20] Emory University School of Medicine,Department of Medicine, Perlman School of Medicine
[21] Perelman School of Medicine,Cardiovascular Medicine Division, Department of Medicine
[22] VA Tennessee Valley Healthcare System,Department of Surgery, Perlman School of Medicine
[23] Vanderbilt University Medical Center,Center for Drug Evaluation and Research
[24] Edith Nourse Rogers Memorial Veterans Hospital,undefined
[25] Boston University School of Medicine,undefined
[26] Phoenix Veterans Affairs Health Care System,undefined
[27] University of Utah School of Medicine,undefined
[28] Vanderbilt University Medical Center,undefined
[29] Brigham and Women’s Hospital,undefined
[30] Harvard Medical School,undefined
[31] VA Connecticut Healthcare System,undefined
[32] University of Pennsylvania,undefined
[33] Emory Clinical Cardiovascular Research Institute,undefined
[34] Brigham and Women’s Hospital,undefined
[35] Harvard Medical School,undefined
[36] University of Pennsylvania,undefined
[37] US Food and Drug Administration,undefined
来源
Nature Medicine | 2019年 / 25卷
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摘要
Peripheral artery disease (PAD) is a leading cause of cardiovascular morbidity and mortality; however, the extent to which genetic factors increase risk for PAD is largely unknown. Using electronic health record data, we performed a genome-wide association study in the Million Veteran Program testing ~32 million DNA sequence variants with PAD (31,307 cases and 211,753 controls) across veterans of European, African and Hispanic ancestry. The results were replicated in an independent sample of 5,117 PAD cases and 389,291 controls from the UK Biobank. We identified 19 PAD loci, 18 of which have not been previously reported. Eleven of the 19 loci were associated with disease in three vascular beds (coronary, cerebral, peripheral), including LDLR, LPL and LPA, suggesting that therapeutic modulation of low-density lipoprotein cholesterol, the lipoprotein lipase pathway or circulating lipoprotein(a) may be efficacious for multiple atherosclerotic disease phenotypes. Conversely, four of the variants appeared to be specific for PAD, including F5 p.R506Q, highlighting the pathogenic role of thrombosis in the peripheral vascular bed and providing genetic support for Factor Xa inhibition as a therapeutic strategy for PAD. Our results highlight mechanistic similarities and differences among coronary, cerebral and peripheral atherosclerosis and provide therapeutic insights.
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页码:1274 / 1279
页数:5
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