Sequencing-based fine-mapping and in silico functional characterization of the 10q24.32 arsenic metabolism efficiency locus across multiple arsenic-exposed populations
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Published:2023-01-20
Issue:1
Volume:19
Page:e1010588
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ISSN:1553-7404
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Container-title:PLOS Genetics
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language:en
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Short-container-title:PLoS Genet
Author:
Chernoff Meytal BatyaORCID,
Delgado Dayana,
Tong Lin,
Chen LinORCID,
Oliva MeritxellORCID,
Tamayo Lizeth I.ORCID,
Best Lyle G.,
Cole Shelley,
Jasmine Farzana,
Kibriya Muhammad G.ORCID,
Nelson Heather,
Huang Lei,
Haack Karin,
Kent Jack,
Umans Jason G.ORCID,
Graziano Joseph,
Navas-Acien Ana,
Karagas Margaret R.,
Ahsan Habib,
Pierce Brandon L.ORCID
Abstract
Inorganic arsenic is highly toxic and carcinogenic to humans. Exposed individuals vary in their ability to metabolize arsenic, and variability in arsenic metabolism efficiency (AME) is associated with risks of arsenic-related toxicities. Inherited genetic variation in the 10q24.32 region, near the arsenic methyltransferase (AS3MT) gene, is associated with urine-based measures of AME in multiple arsenic-exposed populations. To identify potential causal variants in this region, we applied fine mapping approaches to targeted sequencing data generated for exposed individuals from Bangladeshi, American Indian, and European American populations (n = 2,357, 557, and 648 respectively). We identified three independent association signals for Bangladeshis, two for American Indians, and one for European Americans. The size of the confidence sets for each signal varied from 4 to 85 variants. There was one signal shared across all three populations, represented by the same SNP in American Indians and European Americans (rs191177668) and in strong linkage disequilibrium (LD) with a lead SNP in Bangladesh (rs145537350). Beyond this shared signal, differences in LD patterns, minor allele frequency (MAF) (e.g., rs12573221 ~13% in Bangladesh ~0.2% among American Indians), and/or heterogeneity in effect sizes across populations likely contributed to the apparent population specificity of the additional identified signals. One of our potential causal variants influencesAS3MTexpression and nearby DNA methylation in numerous GTEx tissue types (with rs4919690 as a likely causal variant). Several SNPs in our confidence sets overlap transcription factor binding sites and cis-regulatory elements (from ENCODE). Taken together, our analyses reveal multiple potential causal variants in the 10q24.32 region influencing AME, including a variant shared across populations, and elucidate potential biological mechanisms underlying the impact of genetic variation on AME.
Funder
National Institute of Health
National Institutes of Health
U.S National Institutes of General Medicine
National Heart, Lung, and Blood Institute
National Institute of Environmental Health Sciences
National Institute of General Medicine
The National Institute of Environmental Health Sciences
Susan G. Komen
National Institute of Aging
The Common Fund of the Office of the Director of the National Institutes of Health, and by NCI, NHGRI, NHLBI, NIDA, NIMH, and NINDS
Publisher
Public Library of Science (PLoS)
Subject
Cancer Research,Genetics (clinical),Genetics,Molecular Biology,Ecology, Evolution, Behavior and Systematics
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