Alcohol and drug use increase the risk for violence, HIV, and injuries. Excessive alcohol use is a leading cause of preventable death, associated with over $200 billion in economic costs. Thus, it is a priority to understand the determinants of alcohol and drug use, particularly in youth. Low overall serotonergic (5-HT) functioning plays a role in the etiology of alcohol and drug involvement. However, the mechanisms underlying this relation are less clear as very few longitudinal studies on this topic have been conducted. Understanding the early mediating mechanisms in this relation would be informative for the etiology, prevention and intervention of alcohol and drug involvement. Measured genetic data can be leveraged to model variability in overall 5-HT function. Unfortunately, candidate gene studies have widely recognized limitations, including lack of replication, small effect sizes, and poor understanding of biological mechanisms. To address these gaps and limitations, the proposed study will prospectively examine childhood temperament characteristics and early adolescent psychopathology as potential mechanisms of influence in the relation between low overall serotonergic functioning and mid/late adolescent alcohol and drug involvement. It will test these models in two longitudinal studies of adolescents and will combine the results and account for heterogeneity across studies using meta-analytic techniques.
Aim 1 will model genetic risk for low 5-HT function by using information from multiple single nucleotide polymorphisms (SNPs) to create a biologically based genetic risk score. SNPs in 5- HT genes will be selected for inclusion in the risk score by using bioinformatics tools, like the Encyclopeda of DNA Elements, to identify SNPs with functional effects on gene expression and/or regulation.
Aim 2 will provide the first prospective test of childhood effortful control, sadness, and anger as moderated mediators in the relation between a genetic risk score indexing low 5-HT function and mid/late adolescent alcohol and drug involvement.
Aim 3 will provide the first prospective test of early adolescent pure conduct problems (CP), pure depressive symptoms (DEP), and co-occurring CP/DEP as mediators in the relation between a genetic risk score indexing low 5-HT function and mid/late adolescent alcohol and drug involvement.
Aim 3 will account for methodological limitations of previous studies by simultaneously accounting for art factual CP/DEP comorbidity and controlling for baseline alcohol/drug involvement and other adolescent psychopathology. The study has implications for understanding developmental pathways to alcohol and drug involvement and will be the first to prospectively study childhood temperament and early adolescent psychopathology as mechanisms of risk in the relation between a genetic risk score indexing low 5-HT function and alcohol and drug involvement in youth.

Public Health Relevance

Alcohol and drug use are typically initiated during adolescence, making it particularly important to study the risk factors for alcohol and drug involvement in youth. The proposed study will prospectively examine childhood temperament characteristics and early adolescent psychopathology as potential mechanisms of influence in the relation between low overall serotonergic functioning and alcohol and drug involvement. Findings will inform prevention and intervention efforts that may decrease the high economic costs and adverse mental and physical health outcomes associated with alcohol and drug involvement.

Agency
National Institute of Health (NIH)
Institute
National Institute on Alcohol Abuse and Alcoholism (NIAAA)
Type
Predoctoral Individual National Research Service Award (F31)
Project #
5F31AA023128-02
Application #
8963297
Study Section
Special Emphasis Panel (ZAA1)
Program Officer
Scott, Marcia S
Project Start
2014-07-21
Project End
2017-01-20
Budget Start
2015-07-21
Budget End
2016-07-20
Support Year
2
Fiscal Year
2015
Total Cost
Indirect Cost
Name
Arizona State University-Tempe Campus
Department
Psychology
Type
Schools of Arts and Sciences
DUNS #
943360412
City
Tempe
State
AZ
Country
United States
Zip Code
85287
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Wang, Frances L; Chassin, Laurie (2018) Negative Urgency Mediates the Relation between Genetically-Influenced Serotonin Functioning and Alcohol Problems. Clin Psychol Sci 6:106-122
Wang, Frances L; Chassin, Laurie; Lee, Matthew et al. (2017) Roles of Response Inhibition and Gene-Environment Interplay in Pathways to Adolescents' Externalizing Problems. J Res Adolesc 27:258-277
Elam, Kit K; Chassin, Laurie; Lemery-Chalfant, Kathryn et al. (2017) Affiliation with substance-using peers: Examining gene-environment correlations among parent monitoring, polygenic risk, and children's impulsivity. Dev Psychobiol 59:561-573
Elam, Kit K; Wang, Frances L; Bountress, Kaitlin et al. (2016) Predicting substance use in emerging adulthood: A genetically informed study of developmental transactions between impulsivity and family conflict. Dev Psychopathol 28:673-88
Wang, Frances L; Pandika, Danielle; Chassin, Laurie et al. (2016) Testing the Relations Among Family Disorganization, Delay Discounting, and Adolescent Alcohol Use: A Genetically Informed Study. Alcohol Clin Exp Res 40:846-56
Wang, Frances L; Eisenberg, Nancy; Valiente, Carlos et al. (2016) Role of temperament in early adolescent pure and co-occurring internalizing and externalizing problems using a bifactor model: Moderation by parenting and gender. Dev Psychopathol 28:1487-1504
Wang, Frances L; Chassin, Laurie; Geiser, Christian et al. (2016) Mechanisms in the relation between GABRA2 and adolescent externalizing problems. Eur Child Adolesc Psychiatry 25:67-80
Wang, Frances L; Chassin, Laurie; Eisenberg, Nancy et al. (2015) Effortful Control Predicts Adolescent Antisocial-Aggressive Behaviors and Depressive Symptoms: Co-Occurrence and Moderation by Impulsivity. Child Dev 86:1812-29