Multi-ancestry genetic analysis of gene regulation in coronary arteries prioritizes disease risk loci
Hodonsky, Chani J; Turner, Adam W; Khan, Mohammad Daud; Barrientos, Nelson B; Methorst, Ruben; Ma, Lijiang; Lopez, Nicolas G; Mosquera, Jose Verdezoto; Auguste, Gaëlle; Farber, Emily; Ma, Wei Feng; Wong, Doris; Onengut-Gumuscu, Suna; Kavousi, Maryam; Peyser, Patricia A; van der Laan, Sander W; Leeper, Nicholas J; Kovacic, Jason C; Björkegren, Johan L M; Miller, Clint L
(2024) Cell genomics, volume 4, issue 1
(Article)
Abstract
Genome-wide association studies (GWASs) have identified hundreds of risk loci for coronary artery disease (CAD). However, non-European populations are underrepresented in GWASs, and the causal gene-regulatory mechanisms of these risk loci during atherosclerosis remain unclear. We incorporated local ancestry and haplotypes to identify quantitative trait loci for expression (eQTLs) and
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splicing (sQTLs) in coronary arteries from 138 ancestrally diverse Americans. Of 2,132 eQTL-associated genes (eGenes), 47% were previously unreported in coronary artery; 19% exhibited cell-type-specific expression. Colocalization revealed subgroups of eGenes unique to CAD and blood pressure GWAS. Fine-mapping highlighted additional eGenes, including TBX20 and IL5. We also identified sQTLs for 1,690 genes, among which TOR1AIP1 and ULK3 sQTLs demonstrated the importance of evaluating splicing to accurately identify disease-relevant isoform expression. Our work provides a patient-derived coronary artery eQTL resource and exemplifies the need for diverse study populations and multifaceted approaches to characterize gene regulation in disease processes.
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Keywords: coronary artery, eQTL, fine-mapping, gene regulation, genetic diversity, genome-wide association studies, RNA-seq, Genetics, Biochemistry, Genetics and Molecular Biology (miscellaneous), Journal Article
ISSN: 2666-979X
Publisher: Cell Press
Note: Publisher Copyright: © 2023 The Authors
(Peer reviewed)