Genome-wide Association Study of Alcohol Dependence

Overview

Journal Arch Gen Psychiatry

Specialty Psychiatry

Date 2009 Jul 8

PMID 19581569

Citations 213

Authors

Jens Treutlein

Sven Cichon

Monika Ridinger

Norbert Wodarz

Michael Soyka

Peter Zill

Wolfgang Maier

Rainald Moessner

Wolfgang Gaebel

Norbert Dahmen

Christoph Fehr

Norbert Scherbaum

Michael Steffens

Kerstin U Ludwig

Josef Frank

H Erich Wichmann

Stefan Schreiber

Nico Dragano

Wolfgang H Sommer

Fernando Leonardi-Essmann

Anbarasu Lourdusamy

Peter Gebicke-Haerter

Thomas F Wienker

Patrick F Sullivan

Markus M Nothen

Falk Kiefer

Rainer Spanagel

Karl Mann

Marcella Rietschel

Affiliations

Soon will be listed here.

Abstract

Context: Alcohol dependence is a serious and common public health problem. It is well established that genetic factors play a major role in the development of this disorder. Identification of genes that contribute to alcohol dependence will improve our understanding of the mechanisms that underlie this disorder.

Objective: To identify susceptibility genes for alcohol dependence through a genome-wide association study (GWAS) and a follow-up study in a population of German male inpatients with an early age at onset.

Design: The GWAS tested 524,396 single-nucleotide polymorphisms (SNPs). All SNPs with P < 10(-4) were subjected to the follow-up study. In addition, nominally significant SNPs from genes that had also shown expression changes in rat brains after long-term alcohol consumption were selected for the follow-up step.

Setting: Five university hospitals in southern and central Germany.

Participants: The GWAS included 487 male inpatients with alcohol dependence as defined by the DSM-IV and an age at onset younger than 28 years and 1358 population-based control individuals. The follow-up study included 1024 male inpatients and 996 age-matched male controls. All the participants were of German descent.

Main Outcome Measures: Significant association findings in the GWAS and follow-up study with the same alleles.

Results: The GWAS produced 121 SNPs with nominal P < 10(-4). These, together with 19 additional SNPs from homologues of rat genes showing differential expression, were genotyped in the follow-up sample. Fifteen SNPs showed significant association with the same allele as in the GWAS. In the combined analysis, 2 closely linked intergenic SNPs met genome-wide significance (rs7590720, P = 9.72 x 10(-9); rs1344694, P = 1.69 x 10(-8)). They are located on chromosome region 2q35, which has been implicated in linkage studies for alcohol phenotypes. Nine SNPs were located in genes, including the CDH13 and ADH1C genes, that have been reported to be associated with alcohol dependence.

Conclusions: This is the first GWAS and follow-up study to identify a genome-wide significant association in alcohol dependence. Further independent studies are required to confirm these findings.

Citing Articles

Human genetics and epigenetics of alcohol use disorder.

Zhou H, Gelernter J J Clin Invest. 2024; 134(16).

PMID: 39145449 PMC: 11324314. DOI: 10.1172/JCI172885.

Generalized genetic liability to substance use disorders.

Miller A, Bogdan R, Agrawal A, Hatoum A J Clin Invest. 2024; 134(11).

PMID: 38828723 PMC: 11142744. DOI: 10.1172/JCI172881.

Neuronal-specific methylome and hydroxymethylome analysis reveal significant loci associated with alcohol use disorder.

Andrade-Brito D, Nunez-Rios D, Martinez-Magana J, Nagamatsu S, Rompala G, Zillich L Front Genet. 2024; 15:1345410.

PMID: 38633406 PMC: 11021708. DOI: 10.3389/fgene.2024.1345410.

Neuronal-specific methylome and hydroxymethylome analysis reveal replicated and novel loci associated with alcohol use disorder.

Andrade-Brito D, Nunez-Rios D, Martinez-Magana J, Nagamatsu S, Rompala G, Zillich L medRxiv. 2023; .

PMID: 38105948 PMC: 10725575. DOI: 10.1101/2023.11.28.23299094.

Maternal pre-pregnancy BMI, offspring epigenome-wide DNA methylation, and childhood obesity: findings from the Boston Birth Cohort.

Si J, Meir A, Hong X, Wang G, Huang W, Pearson C BMC Med. 2023; 21(1):317.

PMID: 37612641 PMC: 10463574. DOI: 10.1186/s12916-023-03003-5.

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