Abstract

Significant genetic influences on psychoactive substance use (PSU) and psychoactive substance use disorders (PSUD) have been conclusively demonstrated. An extensive body of research has also implicated a range of environmental influences on risk for PSU and PSUD. The challenge facing current researchers is to clarify the interplay between these genetic and environmental risk factors which over time can lead to the initiation and subsequent abuse/dependence of psychoactive substances. This competitive renewal requests 4 years of support for a series of detailed analyses of a unique twin data set, collection of which is now nearing completion. This sample will consist ofapproximately 750 complete adult male-male pairs, on whom extensive data has been collected in two previous interview waves. The current interview obtains, using a life-history format interview, key risk and protective factors for PSU and PSUD over 5 developmental periods (ages 8-11, 12-14, 15-17, 18-21, and 22-25). In addition, in this sample, which has essentially completed its age at risk for PSU and PSUD, we have obtained, for a second time, detailed assessments of lifetime PSU and PSUD and a lifetime calender recording key life transitions and onsets, offsets and frequency of PSU. We seek to use this rich and valuable data set to further our understanding of the development of risk for PSU and PSUD. We articulate 4 primary aims: 1. The Development of PSUD. We will identify the nature and pattern of trajectories of PSUD and related risk factors across adolescence and young adulthood, and develop a comprehensive developmental framework for PSUD by exploring the associations between genes, environment, and PSUD. 2. Contextual Factors - We will clarify the extent to which genetic and environmental risk factors for PSU and PSUD are moderated by key developmental experiences including, peer deviance and access to illicit substances. 3. Heterogeneity - Multiple subtypes of PSUD probably exist. Using the adolescent limited versus life-course persistent antisocial behavior as a paradigm, we hope to develop meaningful typologies for PSUD that will map in a useful way on the range of available etiologic factors. 4. Sequella - Given an initial episode of PSU, we will explore what predicts further use and the development of PSUD. Given the development of PSUD, we will clarify the factors that predict subsequent adult outcomes. Our research team, a combination of clinicians, statisticians and geneticists, has a long track-record of innovative and rigorous data analytic approaches to complex problems in human genetic epidemiology such as the development of PSU and PSUD.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Project (R01)
Project #
5R01DA011287-08
Application #
7241525
Study Section
Behavioral Genetics and Epidemiology Study Section (BGES)
Program Officer
Weinberg, Naimah Z
Project Start
1998-06-15
Project End
2009-05-31
Budget Start
2007-06-01
Budget End
2009-05-31
Support Year
8
Fiscal Year
2007
Total Cost
$284,454
Indirect Cost

  Institution

Name
Virginia Commonwealth University
Department
Psychiatry
Type
Schools of Medicine
DUNS #
105300446
City
Richmond
State
VA
Country
United States
Zip Code
23298

  Publications

Otowa, Takeshi; York, Timothy P; Gardner, Charles O et al. (2014) The impact of childhood parental loss on risk for mood, anxiety and substance use disorders in a population-based sample of male twins. Psychiatry Res 220:404-9
Hsu, Kean J; Young-Wolff, Kelly C; Kendler, Kenneth S et al. (2014) Neuropsychological deficits in major depression reflect genetic/familial risk more than clinical history: a monozygotic discordant twin-pair study. Psychiatry Res 215:87-94
Kendler, Kenneth S; Myers, John; Damaj, M Imad et al. (2013) Early smoking onset and risk for subsequent nicotine dependence: a monozygotic co-twin control study. Am J Psychiatry 170:408-13
Hettema, John M; An, Seon-Sook; van den Oord, Edwin J C G et al. (2013) Genetic association between RGS1 and internalizing disorders. Psychiatr Genet 23:56-60
Otowa, Takeshi; Gardner, Charles O; Kendler, Kenneth S et al. (2013) Parenting and risk for mood, anxiety and substance use disorders: a study in population-based male twins. Soc Psychiatry Psychiatr Epidemiol 48:1841-9
Hettema, John M; Sun, Cuie; Chen, Xiangning et al. (2013) Genetic association study between RGS2 and anxiety-related phenotypes. Psychiatr Genet 23:92
Baker, Jessica H; Maes, Hermine H; Kendler, Kenneth S (2012) Shared environmental contributions to substance use. Behav Genet 42:345-53
van Beek, Jenny H D A; Kendler, Kenneth S; de Moor, Marleen H M et al. (2012) Stable genetic effects on symptoms of alcohol abuse and dependence from adolescence into early adulthood. Behav Genet 42:40-56
Gillespie, Nathan A; Lubke, Gitta H; Gardner, Charles O et al. (2012) Two-part random effects growth modeling to identify risks associated with alcohol and cannabis initiation, initial average use and changes in drug consumption in a sample of adult, male twins. Drug Alcohol Depend 123:220-8
Kendler, Kenneth S; Eaves, Lindon J; Loken, Erik K et al. (2011) The impact of environmental experiences on symptoms of anxiety and depression across the life span. Psychol Sci 22:1343-52

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