Examining the role of common genetic variants on alcohol, tobacco, cannabis and illicit drug dependence: genetics of vulnerability to drug dependence.
- Authors
- Palmer, Rohan H C; Brick, Leslie; Nugent, Nicole R; Bidwell, L Cinnamon; McGeary, John E; Knopik, Valerie S; Keller, Matthew C
- Year
- 2015
- Journal
- Addiction (Abingdon, England)
- PMID
- 25424661
- DOI
- 10.1111/add.12815
- PMCID
- PMC4329043
BACKGROUND AND AIMS: Twin and family studies suggest that genetic influences are shared across substances of abuse. However, despite evidence of heritability, genome-wide association and candidate gene studies have indicated numerous markers of limited effects, suggesting that much of the heritability remains missing. We estimated (1) the aggregate effect of common single nucleotide polymorphisms (SNPs) on multiple indicators of comorbid drug problems that are typically employed across community and population-based samples, and (2) the genetic covariance across these measures. PARTICIPANTS: A total of 2596 unrelated subjects from the Study of Addiction: Genetics and Environment provided information on alcohol, tobacco, cocaine, cannabis and other illicit substance dependence. Phenotypic measures included: (1) a factor score based on DSM-IV drug dependence diagnoses (DD), (2) a factor score based on problem use (PU; i.e. 1+ DSM-IV symptoms) and (3) dependence vulnerability (DV; a ratio of DSM-IV symptoms to the number of substances used). FINDINGS: Univariate and bivariate genome-wide complex trait analyses of this selected sample indicated that common SNPs explained 25-36% of the variance across measures, with DD and DV having the largest effects [h(2) SNP (standard error)β= 0.36 (0.13) and 0.33 (0.13), respectively; PU = 0.25 (0.13)]. Genetic effects were shared across the three phenotypic measures of comorbid drug problems [rDD-PU = 0.92 (0.08), rDD-DV = 0.97 (0.08) and rPU-DV = 0.96 (0.07)]. CONCLUSION: At least 20% of the variance in the generalized vulnerability to substance dependence is attributable to common single nucleotide polymorphisms. The additive effect of common single nucleotide polymorphisms is shared across important indicators of comorbid drug problems.
The Common Pathway Model. The observed phenotypic variance/covariance of the measured dependence phenotypes (rectangles) represent alternate manifestations of a generalized vulnerability to dependence (indicated by the latent trait (solid circle), Substance Dependence Vulnerability). Variation in the latent trait and the variance in the observed phenotypes are decomposable into genetic (G) and environmental/residual (E) influences (dashed-circles).
Proportion of variance explained (VG/VP) of individual chromosomes on each phenotype while imposing strict QC and adjusting for cryptic relatedness. Note: Additive effects attributable to variants across chromosome were estimated at 1E-6 across all phenotypes. Abbreviations: DD = Dependence Diagnosis Factor; PU = Problem Use Factor; DV = Dependence Vulnerability Score.
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