GeneSet Information

Tier IV GS408353 • Genome-wide association study of stimulant dependence

DESCRIPTION:

A genome-wide association study for stimulant dependence was performed in a discovery cohort of African- (AA) and European-ancestry (EA) subjects ascertained for genetic studies of alcohol, opioid, and cocaine use disorders. The sample comprised individuals with DSM-IV stimulant dependence (393 EA cases, 5288 EA controls; 155 AA cases, 5603 AA controls). An independent cohort from the family-based Collaborative Study on the Genetics of Alcoholism (532 EA cases, 7635 EA controls; 53 AA cases, AA 3352 controls) was used for replication. One variant in SLC25A16 (rs2394476, p = 3.42 × 10-10, odds ratio [OR] = 3.70) was GWS in AAs. Four other loci showed suggestive evidence, including KCNA4 in AAs (rs11500237, p = 2.99 × 10-7, OR = 2.31) which encodes one of the potassium voltage-gated channel protein that has been linked to several other substance use disorders, and CPVL in the combined population groups (rs1176440, p = 3.05 × 10-7, OR = 1.35), whose expression was previously shown to be upregulated in the prefrontal cortex from users of cocaine, cannabis, and phencyclidine. Analysis of the top GWAS signals revealed a significant enrichment with nicotinic acetylcholine receptor genes (adjusted p = 0.04) and significant pleiotropy between stimulant dependence and alcohol dependence in EAs (padj = 3.6 × 10-3), an anxiety disorder in EAs (padj = 2.1 × 10-4), and ADHD in both AAs (padj = 3.0 × 10-33) and EAs (padj = 6.7 × 10-35). 

LABEL:

Genome-wide association study of stimulant dependence

SCORE TYPE:

Binary

DATE ADDED:

2024-03-26

DATE UPDATED:

2024-04-25

SPECIES:

AUTHORS:

Jiayi Cox, Richard Sherva, Leah Wetherill, Tatiana Foroud, Howard J Edenberg, Henry R Kranzler, Joel Gelernter, Lindsay A Farrer

TITLE:

Genome-wide association study of stimulant dependence.

JOURNAL:

Translational psychiatry Jun 2021, Vol 11, pp. 363

ABSTRACT:

Stimulant dependence is heritable, but specific genetic factors underlying the trait have not been identified. A genome-wide association study for stimulant dependence was performed in a discovery cohort of African- (AA) and European-ancestry (EA) subjects ascertained for genetic studies of alcohol, opioid, and cocaine use disorders. The sample comprised individuals with DSM-IV stimulant dependence (393 EA cases, 5288 EA controls; 155 AA cases, 5603 AA controls). An independent cohort from the family-based Collaborative Study on the Genetics of Alcoholism (532 EA cases, 7635 EA controls; 53 AA cases, AA 3352 controls) was used for replication. One variant in SLC25A16 (rs2394476, p = 3.42 × 10 PUBMED: 34226506
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Annotation Information

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Population (D011153)
Genetics (D005823)
Potassium (D011188)
Phencyclidine (D010622)
Population Groups (D044382)
Genome-Wide Association Study (D055106)
Odds Ratio (D016017)
Acetylcholine (D000109)
Prefrontal Cortex (D017397)
Cocaine (D003042)
Cannabis (D002188)
Anxiety Disorders (D001008)
Anxiety (D001007)
Association (D001244)
Alcoholism (D000437)
frontal association cortex (MA:0000906)
nicotinic acetylcholine-gated receptor-channel complex (GO:0005892)
Transcriptomics (EDAM_topic:0203)
Ala-Ala-Ser (CHEBI:73321)
demeton-S-methyl (CHEBI:38624)
pyraclofos (CHEBI:38876)
acetylcholine (CHEBI:15355)
cocaine(1+) (CHEBI:60056)
phencyclidine (CHEBI:8058)
protein polypeptide chain (CHEBI:16541)
propyzamide (CHEBI:34935)
potassium atom (CHEBI:26216)
Alcoholism (HP:0030955)
anxiety disorder (DOID:2030)
alcohol dependence (DOID:0050741)
anxiety disorder (EFO:0006788)
Caucasian (EFO:0003156)
atomic absorption spectrometry (MMO:0000232)
prefrontal bone (UBERON:0010750)
prefrontal cortex (UBERON:0000451)

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