Smoking-informed methylation and expression QTLs in human brain and colocalization with smoking-associated genetic loci-Reference-Cited by-同舟云学术

Smoking-informed methylation and expression QTLs in human brain and colocalization with smoking-associated genetic loci

Published:2024-06-04 Issue:11 Volume:49 Page:1749-1757
ISSN:0893-133X
Container-title:Neuropsychopharmacology
language:en
Short-container-title:Neuropsychopharmacol.

Author:

Carnes Megan Ulmer,Quach Bryan C.^ORCID,Zhou Linran,Han Shizhong,Tao Ran,Mandal Meisha,Deep-Soboslay Amy,Marks Jesse A.,Page Grier P.^ORCID,Maher Brion S.,Jaffe Andrew E.,Won Hyejung^ORCID,Bierut Laura J.^ORCID,Hyde Thomas M.^ORCID,Kleinman Joel E.^ORCID,Johnson Eric O.^ORCID,Hancock Dana B.^ORCID

Abstract

AbstractSmoking is a leading cause of preventable morbidity and mortality. Smoking is heritable, and genome-wide association studies (GWASs) of smoking behaviors have identified hundreds of significant loci. Most GWAS-identified variants are noncoding with unknown neurobiological effects. We used genome-wide genotype, DNA methylation, and RNA sequencing data in postmortem human nucleus accumbens (NAc) to identify cis-methylation/expression quantitative trait loci (meQTLs/eQTLs), investigate variant-by-cigarette smoking interactions across the genome, and overlay QTL evidence at smoking GWAS-identified loci to evaluate their regulatory potential. Active smokers (N = 52) and nonsmokers (N = 171) were defined based on cotinine biomarker levels and next-of-kin reporting. We simultaneously tested variant and variant-by-smoking interaction effects on methylation and expression, separately, adjusting for biological and technical covariates and correcting for multiple testing using a two-stage procedure. We found >2 million significant meQTL variants (padj < 0.05) corresponding to 41,695 unique CpGs. Results were largely driven by main effects, and five meQTLs, mapping to NUDT12, FAM53B, RNF39, and ADRA1B, showed a significant interaction with smoking. We found 57,683 significant eQTL variants for 958 unique eGenes (padj < 0.05) and no smoking interactions. Colocalization analyses identified loci with smoking-associated GWAS variants that overlapped meQTLs/eQTLs, suggesting that these heritable factors may influence smoking behaviors through functional effects on methylation/expression. One locus containing MUSTN1 and ITIH4 colocalized across all data types (GWAS, meQTL, and eQTL). In this first genome-wide meQTL map in the human NAc, the enriched overlap with smoking GWAS-identified genetic loci provides evidence that gene regulation in the brain helps explain the neurobiology of smoking behaviors.

Funder

U.S. Department of Health & Human Services | NIH | National Institute on Drug Abuse

Publisher

Springer Science and Business Media LLC

Link

https://www.nature.com/articles/s41386-024-01885-4.pdf

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