Functional 3’-UTR Variants Identify Regulatory Mechanisms Impacting Alcohol Use Disorder and Related Traits

Author:

Chen Andy B.,Yu Xuhong,Thapa Kriti S.,Gao Hongyu,Reiter Jill L,Xuei Xiaoling,Tsai Andy P.,Landreth Gary E.,Lai Dongbing,Wang Yue,Foroud Tatiana M.,Tischfield Jay A.,Edenberg Howard J.,Liu YunlongORCID

Abstract

AbstractAlthough genome-wide association studies (GWAS) have identified loci associated with alcohol consumption and alcohol use disorder (AUD), they do not identify which variants are functional. To approach this, we evaluated the impact of variants in 3’ untranslated regions (3’-UTRs) of genes in loci associated with substance use and neurological disorders using a massively parallel reporter assay (MPRA) in neuroblastoma and microglia cells. Functionally impactful variants explained a higher proportion of heritability of alcohol traits than non-functional variants. We identified genes whose 3’-UTR activities are associated with AUD and alcohol consumption by combining variant effects from MPRA with GWAS results. We examined their effects by evaluating gene expression after CRISPR inhibition of neuronal cells and stratifying brain tissue samples by MPRA-derived 3’-UTR activity. A pathway analysis of differentially expressed genes identified inflammation response pathways. These analyses suggest that variation in response to inflammation contributes to the propensity to increase alcohol consumption.

Publisher

Cold Spring Harbor Laboratory

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