Multi-omics integration analysis identifies novel genes for alcoholism with potential overlap with neurodegenerative diseases

Author:

Kapoor ManavORCID,Chao Michael J.,Johnson Emma C.ORCID,Novikova GloriiaORCID,Lai DongbingORCID,Meyers Jacquelyn L.ORCID,Schulman Jessica,Nurnberger John I.ORCID,Porjesz Bernice,Liu YunlongORCID,Hesselbrock Victor,Kuperman Samual,Kramer John,Kamarajan Chella,Pandey Ashwini,Bierut Laura,Rice John P.,Bucholz Kathleen K.,Schuckit Marc,Tischfield Jay,Brooks Andrew,Hart Ronald P.,Almasy Laura,Dick Danielle,Salvatore Jessica,Slesinger Paul,Foroud TatianaORCID,Edenberg Howard J.ORCID,Marcora EdoardoORCID,Agrawal ArpanaORCID,Goate AlisonORCID,

Abstract

AbstractIdentification of causal variants and genes underlying genome-wide association study (GWAS) loci is essential to understand the biology of alcohol use disorder (AUD) and drinks per week (DPW). Multi-omics integration approaches have shown potential for fine mapping complex loci to obtain biological insights to disease mechanisms. In this study, we use multi-omics approaches, to fine-map AUD and DPW associations at single SNP resolution to demonstrate that rs56030824 on chromosome 11 significantly reduces SPI1 mRNA expression in myeloid cells and lowers risk for AUD and DPW. Our analysis also identifies MAPT as a candidate causal gene specifically associated with DPW. Genes prioritized in this study show overlap with causal genes associated with neurodegenerative disorders. Multi-omics integration analyses highlight, genetic similarities and differences between alcohol intake and disordered drinking, suggesting molecular heterogeneity that might inform future targeted functional and cross-species studies.

Funder

U.S. Department of Health & Human Services | NIH | National Institute on Alcohol Abuse and Alcoholism

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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