Alcohol and nicotine polygenic scores are associated with the development of alcohol and nicotine use problems from adolescence to young adulthood

Joseph D Deak; D Angus Clark; Mengzhen Liu; Jonathan D Schaefer; Seon Kyeong Jang; C Emily Durbin; William G Iacono; Matt McGue; Scott Vrieze; Brian M Hicks

doi:10.1111/add.15697

Alcohol and nicotine polygenic scores are associated with the development of alcohol and nicotine use problems from adolescence to young adulthood

Addiction. 2022 Apr;117(4):1117-1127. doi: 10.1111/add.15697. Epub 2021 Oct 24.

Authors

Joseph D Deak^{1

2}, D Angus Clark³, Mengzhen Liu⁴, Jonathan D Schaefer⁴, Seon Kyeong Jang⁴, C Emily Durbin⁵, William G Iacono⁴, Matt McGue⁴, Scott Vrieze⁴, Brian M Hicks³

Affiliations

¹ Yale University, New Haven, CT, USA.
² VA CT Healthcare System, West Haven, CT, USA.
³ University of Michigan, Ann Arbor, MI, USA.
⁴ University of Minnesota, Minneapolis, MN, USA.
⁵ Michigan State University, East Lansing, MI, USA.

Abstract

Background and aims: Molecular genetic studies of alcohol and nicotine use have identified many genome-wide association study (GWAS) loci. We measured associations between drinking and smoking polygenic scores (PGS) and trajectories of alcohol and nicotine use outcomes from late childhood to early adulthood, substance-specific versus broader-liability PGS effects, and if PGS performance varied for consumption versus problematic substance use.

Design, setting, participants and measurements: We fitted latent growth curve models with structured residuals to scores on measures of alcohol and nicotine use and problems from ages 14 to 34 years. We then estimated associations between the intercept (initial status) and slope (rate of change) parameters and PGSs for drinks per week (DPW), problematic alcohol use (PAU), cigarettes per day (CPD) and ever being a regular smoker (SMK), controlling for sex and genetic principal components. All data were analyzed in the United States. PGSs were calculated for participants of the Minnesota Twin Family Study (n = 3225) using results from the largest GWAS of alcohol and nicotine consumption and problematic use to date.

Findings: Each PGS was associated with trajectories of use for their respective substances [i.e. DPW (β_mean = 0.08; β_range = 0.02-0.12) and PAU (β_mean = 0.12; β_range = -0.02 to 0.31) for alcohol; CPD (β_mean = 0.08; β_range = 0.04-0.14) and SMK (β_mean = 0.18; β_range = 0.05-0.36) for nicotine]. The PAU and SMK PGSs also exhibited cross-substance associations (i.e. PAU for nicotine-specific intercepts and SMK for alcohol intercepts and slope). All identified SMK PGS effects remained as significant predictors of nicotine and alcohol trajectories (β_mean = 0.15; β_range = 0.02-0.33), even after adjusting for the respective effects of all other PGSs.

Conclusions: Substance use-related polygenic scores (PGSs) vary in the strength and generality versus specificity of their associations with substance use and problems over time. The regular smoking PGS appears to be a robust predictor of substance use trajectories and seems to measure both nicotine-specific and non-specific genetic liability for substance use, and potentially externalizing problems in general.

Keywords: Alcohol; developmental trajectories; nicotine; polygenic risk scores; smoking; substance use.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Adolescent
Adult
Alcohol Drinking / epidemiology
Alcohol Drinking / genetics
Genome-Wide Association Study
Humans
Multifactorial Inheritance
Nicotine*
Smoking / epidemiology
Smoking / genetics
Tobacco Products*
Young Adult

Substances

Nicotine

Abstract

Publication types

MeSH terms

Substances

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