Genetic Underpinnings of the Transition From Alcohol Consumption to Alcohol Use Disorder: Shared and Unique Genetic Architectures in a Cross-Ancestry Sample.

Am J Psychiatry

Mental Illness Research, Education, and Clinical Center, Veterans Integrated Service Network 4, Crescenz Veterans Affairs Medical Center, Philadelphia (Kember, Vickers-Smith, Kranzler); Center for Studies of Addiction, Department of Psychiatry (Kember, Xu, Kranzler) and Department of Epidemiology, University of Kentucky College of Public Health, Lexington (Vickers-Smith); Center on Drug and Alcohol Research, Department of Behavioral Science, University of Kentucky College of Medicine, Lexington (Vickers-Smith); VA Connecticut Healthcare System, West Haven (Zhou, Dao, Justice, Gelernter); Department of Psychiatry (Zhou, Gelernter), Department of Genetics (Gelernter), Department of Neuroscience (Gelernter), and Department of Internal Medicine (Justice), Yale School of Medicine, New Haven, Conn.; School of Public Health, Yale University, New Haven, Conn. (Dao, Justice); Department of Psychiatry, University of California San Diego, San Diego (Jennings, Sanchez-Roige); Division of Genetic Medicine, Department of Medicine, Vanderbilt University Medical Center, Nashville, Tenn. (Davis, Sanchez-Roige).

Published: August 2023

AI Article Synopsis

Article Abstract

Objective: Recent genome-wide association studies (GWASs) of alcohol-related phenotypes have uncovered key differences in the underlying genetic architectures of alcohol consumption and alcohol use disorder (AUD), with the two traits having opposite genetic correlations with psychiatric disorders. Understanding the genetic factors that underlie the transition from heavy drinking to AUD has important theoretical and clinical implications.

Methods: The authors used longitudinal data from the cross-ancestry Million Veteran Program sample to identify 1) novel loci associated with AUD and alcohol consumption (measured by the score on the consumption subscale of the Alcohol Use Disorders Identification Test [AUDIT-C]), 2) the impact of phenotypic variation on genetic discovery, and 3) genetic variants with direct effects on AUD that are not mediated through alcohol consumption.

Results: The authors identified 26 loci associated with AUD and 22 loci associated with AUDIT-C score, including ancestry-specific and novel loci. In secondary GWASs that excluded individuals who report abstinence, the authors identified seven additional loci for AUD and eight additional loci for AUDIT-C score. Although the heterogeneity of the abstinent group biases the GWAS findings, unique variance between alcohol consumption and disorder remained after the abstinent group was excluded. Finally, using mediation analysis, the authors identified a set of variants with effects on AUD that are not mediated through alcohol consumption.

Conclusions: Differences in genetic architecture between alcohol consumption and AUD are consistent with their having different biological contributions. Genetic variants with direct effects on AUD are potentially relevant to understanding the transition from heavy alcohol consumption to AUD and may be targets for translational prevention and treatment efforts.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10731616PMC
http://dx.doi.org/10.1176/appi.ajp.21090892DOI Listing

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