Author
Listed:
- Samantha G. Malone
(Department of Medical and Clinical Psychology
Henry M. Jackson Foundation for the Advancement of Military Medicine Inc.)
- Christal N. Davis
(Crescenz VA Medical Center
University of Pennsylvania)
- Zachary Piserchia
(Department of Medical and Clinical Psychology
Henry M. Jackson Foundation for the Advancement of Military Medicine Inc.)
- Michael R. Setzer
(Department of Medical and Clinical Psychology)
- Sylvanus Toikumo
(Crescenz VA Medical Center
University of Pennsylvania)
- Hang Zhou
(Veterans Affairs Connecticut Healthcare System
Yale University School of Medicine
Yale University School of Medicine)
- Emma L. Winterlind
(Department of Medical and Clinical Psychology
Henry M. Jackson Foundation for the Advancement of Military Medicine Inc.)
- Joel Gelernter
(Veterans Affairs Connecticut Healthcare System
Yale University School of Medicine)
- Amy Justice
(Veterans Affairs Connecticut Healthcare System
Yale University School of Medicine
Yale University School of Public Health)
- Lorenzo Leggio
(National Institutes of Health
Brown University
Johns Hopkins University
Georgetown University Medical Center)
- Christopher T. Rentsch
(Yale University School of Medicine
London School of Hygiene and Tropical Medicine)
- Henry R. Kranzler
(Crescenz VA Medical Center
University of Pennsylvania)
- Joshua C. Gray
(Department of Medical and Clinical Psychology)
Abstract
Despite neurobiological overlap, alcohol use disorder (AUD) and body mass index (BMI) show minimal genetic correlation (rg), possibly due to mixed directions of shared variants. Here we applied MiXeR to investigate shared genetic architecture between AUD and BMI, conjunctional false discovery rate to detect shared loci and their directional effect, local analysis of (co)variant association for local rg, functional mapping and annotation to identify lead single-nucleotide polymorphisms, Genotype-Tissue Expression (GTEx) to examine tissue enrichment and BrainXcan to assess associations with brain phenotypes. MiXeR indicated 82.2% polygenic overlap, despite an rg of −0.03. The conjuctional false discovery rate method identified 132 shared lead single-nucleotide polymorphisms, with 53 novel, showing both concordant and discordant effects. GTEx analyses identified overexpression in multiple brain regions. Amygdala and caudate nucleus volumes were associated with AUD and BMI. Opposing variant effects explain the minimal rg between AUD and BMI, with implicated brain regions involved in executive function and reward, clarifying their polygenic overlap and neurobiological mechanisms.
Suggested Citation
Samantha G. Malone & Christal N. Davis & Zachary Piserchia & Michael R. Setzer & Sylvanus Toikumo & Hang Zhou & Emma L. Winterlind & Joel Gelernter & Amy Justice & Lorenzo Leggio & Christopher T. Rent, 2025.
"Alcohol use disorder and body mass index show genetic pleiotropy and shared neural associations,"
Nature Human Behaviour, Nature, vol. 9(5), pages 1056-1066, May.
Handle:
RePEc:nat:nathum:v:9:y:2025:i:5:d:10.1038_s41562-025-02148-y
DOI: 10.1038/s41562-025-02148-y
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