GeneSet Information

Tier III GS115095 • Gene which contain SNPs with significant Association Results (p < 0.05) for Addiction and Alcohol Consumption in Young Women

DESCRIPTION:

Table 2. Association Results (p < 0.05) for 1,014 SNPs Associated Wllh Addiction and Alcohol Consumption in Young Women and the MOAFTS p-value

LABEL:

Female Human GWAS Alcohol

SCORE TYPE:

Correlation

DATE ADDED:

2011-04-04

DATE UPDATED:

2024-04-25

SPECIES:

AUTHORS:

Agrawal A, Lynskey MT, Todorov AA, Schrage AJ, Littlefield AK, Grant JD, Zhu Q, Nelson EC, Madden PA, Bucholz KK, Sher KJ, Heath AC

TITLE:

A Candidate Gene Association Study of Alcohol Consumption in Young Women*

JOURNAL:

Alcoholism, clinical and experimental research Dec 2010, Vol None, pp. None

ABSTRACT:

Background:  Excessive alcohol consumption contributes to significant morbidity and mortality. Heritable influences contribute to 50% of the variation in alcohol consumption, suggesting the important role of genes. We used data on a previously defined alcohol consumption factor score in a sample of 827 young women to investigate association with 1,014 single-nucleotide polymorphisms in genes related to addiction. Methods:  Data were drawn from the Missouri Adolescent Female Twin Study (MOAFTS) with replication in the college drinking sample (CDS). Genotypic and phenotypic data were available on 827 MOAFTS and 100 CDS women of European-American ancestry. Data on 1,014 single-nucleotide polymorphisms (SNPs) across 130 genes related to addiction were utilized. Association was conducted in QTDT, which allows for identity-by-descent information to account accurately for twin status in the analysis. The total association variance components model was used, with specification of variance components for relatedness in MOAFTS. Results:  The top signals included clusters of SNPs in tryptophan hydroxylase 2 (TPH2) (e.g., rs1386496, p = 0.0003) and dopa decarboxylase (DDC) (e.g., rs3779084, p = 0.0008), genes that encode proteins responsible for serotonin synthesis. Additional polymorphisms in ADH1B, ADH1C, ADH7, and ADH1A1 were also associated at p &lt; 0.05. The false discovery rate for the top signal (p = 0.0003) was 0.15, suggesting nominal significance only. Replication was limited and noted for 2 SNPs in ADH1C. Conclusions:  While no results survive the burden of multiple testing, nominal findings in TPH2 and DDC suggest the potential role of the serotonin synthesis pathway in alcohol consumption. PUBMED: 21143251
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Annotation Information

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Drinking (D004326)
Missouri (D008923)
Genetic Association Studies (D056726)
Serotonin (D012701)
Alcohol Drinking (D000428)
Tryptophan Hydroxylase (D014365)
Tryptophan (D014364)
Dihydroxyphenylalanine (D004295)
Adolescent (D000293)
Proteins (D011506)
Role (D012380)
Morbidity (D009017)
Zalcitabine (D016047)
Dopa Decarboxylase (D004296)
Methods (D008722)
Women (D014930)
Twins (D014427)
Mortality (D009026)
Polymorphism, Single Nucleotide (D020641)
Association (D001244)
Twin Study (D018486)
addiction (MP:0002555)
biosynthetic process (GO:0009058)
serotonin biosynthetic process (GO:0042427)

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Supported by NIH R01 AA18776 jointly funded by NIAAA and NIDA, and JAX Center for Precision Genetics NIH U54 OD 020351