Abstract

The overall goal of this Mentored Research Scientist Development Award (K01) Application is to become an expert in applying translational methods to study the etiology of substance use, by identifying specific genetic and neurobiological pathways that mediate individual risk to substance use and its related behavioral disorders. Exposure to prenatal smoking provides an excellent model with which to obtain these skills, while simultaneously tackling a serious public health problem. Despite the overall declining trends, smoking during pregnancy remains a leading cause of preventable illness among both mothers and offspring. Offspring of mothers who smoke during pregnancy are at heightened risk for a range of neonatal, as well as long-term behavioral and substance use disorders. Even though mothers who smoke while pregnant are likely to continue smoking during other times in the child's life, at least some of the above associations appear specific to prenatal exposure, suggesting an underlying biological mechanism. In the proposed study, I will examine the roles that genes and brain circuitry play in mediating the relationships between prenatal exposures and offspring behavioral and substance use disorders. The study will build upon a longitudinal three-generation cohort that has been prospectively followed for up to 25 years on a range of diagnostic measures, and now further includes genetic (DNA) markers and MRI scans. I will implement an additional assessment schedule that follows the cohort prospectively on new diagnostic as well as behavioral measures related to smoking, drug and alcohol use. I will first examine the association between prenatal exposure and the above outcome measures, while controlling for potential confounds, and examine the progression from behavioral problems to substance use disorders (Aim 1). I will then test the hypothesis that functionally altering variations within the monoamine oxidase A gene (as well as other genes of interest, particularly within the nicotinic and dopaminergic families) moderate the risk to offspring conferred by exposure to maternal smoking (Aim 2). Using an fMRI task that indexes response inhibition (the Simon Spatial Incompatibility Task), I will next assess whether disruptions to behavioral circuits involved in self-regulatory behaviors mediate the association between prenatal smoking and offspring psychopathology (Aim 3). Finally, I will integrate the genetic and neuroimaging data to explore whether genotype moderates the association between prenatal exposure and cortical circuitry, and explore how genes, exposures, and cortical circuitry interact on the pathway to risk (Aim 4). Even though I bring to this application strength in psychiatric and imaging research, I need to (1) develop further expertise in the epidemiology, etiology, and assessment of substance use and its related syndromes. This will thus form a backbone of my 5-year training plan. In addition, I will seek training in (2) genetics, including methods of genetic analysis and the integration of imaging and genetic data, as well as (3) further methodological expertise in the use of longitudinal epidemiological and healthcare data to address trajectories of smoking and substance use. Finally, I will continue to receive training in the ethical conduct of research. To achieve these goals, I am fortunate to have Myrna M. Weissman, Ph.D., the Chief of the Division of Epidemiology, as my primary mentor, supported by Frances R. Levin, M.D., Deborah S. Hasin, Ph.D. as co- mentors for training in substance use, and Steven P. Hamilton, M.D., Ph.D., for additional training in genetics. Few studies have examined the role of genes in moderating outcomes of prenatal exposures, and none with further indices of brain function. If funded, this study would be the first to directly test the role of genetic variation and brain circuitry in the context of risks conferred by prenatal exposures. The execution of the research plan, in conjunction with the training aims, will enable me (1) learn about and test biological pathways mediating behavioral disorders;(2) to identify offspring groups who may be at greatest risk for these disorders and may require earlier or more targeted intervention;and ultimately (3) to export these skills to study other exposures, genetic pathways, and behavioral outcomes relevant to addictive disorders. The study will be conducted at New York State Psychiatric Institute and Columbia University Department of Psychiatry, which together form an active academic medical center and leading teaching hospital, and include a distinguished group of research scientists devoted to the study of psychiatric and substance use disorders. Should this award be funded, I will commit to devoting at least 75% of my full time effort on this project, and the institution has guaranteed to provide me the freedom to do so.

Public Health Relevance

Fetal exposure to maternal smoking during pregnancy is associated with a range of long-term offspring developmental, behavioral, and substance use disorders. This project is the first to use genetic and neuroimaging approaches to target mechanisms underlying these associations. Findings from this study will provide insights into biological mediators of behavioral and addictive disorders, and ultimately allow us to identify offspring groups who may be at greatest risk for these disorders.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Scientist Development Award - Research & Training (K01)
Project #
5K01DA029598-04
Application #
8505464
Study Section
Special Emphasis Panel (ZDA1-KXH-C (15))
Program Officer
Sirocco, Karen
Project Start
2010-08-01
Project End
2015-07-31
Budget Start
2013-08-01
Budget End
2014-07-31
Support Year
4
Fiscal Year
2013
Total Cost
$182,874
Indirect Cost
$13,546

  Institution

Name
New York State Psychiatric Institute
Department
Type
DUNS #
167204994
City
New York
State
NY
Country
United States
Zip Code
10032

  Publications

Hao, Xuejun; Talati, Ardesheer; Shankman, Stewart A et al. (2017) Stability of Cortical Thinning in Persons at Increased Familial Risk for Major Depressive Disorder Across 8 Years. Biol Psychiatry Cogn Neurosci Neuroimaging 2:619-625
Talati, Ardesheer; Wickramaratne, Priya J; Wesselhoeft, Rikke et al. (2017) Prenatal tobacco exposure, birthweight, and offspring psychopathology. Psychiatry Res 252:346-352
Talati, Ardesheer; Odgerel, Zagaa; Wickramaratne, Priya J et al. (2017) Associations between serotonin transporter and behavioral traits and diagnoses related to anxiety. Psychiatry Res 253:211-219
Joelsson, Petteri; Chudal, Roshan; Talati, Ardesheer et al. (2016) Prenatal smoking exposure and neuropsychiatric comorbidity of ADHD: a finnish nationwide population-based cohort study. BMC Psychiatry 16:306
Talati, Ardesheer; Odgerel, Zagaa; Wickramaratne, Priya J et al. (2016) Brain derived neurotrophic factor moderates associations between maternal smoking during pregnancy and offspring behavioral disorders. Psychiatry Res 245:387-391
Talati, A; Keyes, K M; Hasin, D S (2016) Changing relationships between smoking and psychiatric disorders across twentieth century birth cohorts: clinical and research implications. Mol Psychiatry 21:464-71
Teel, Karen Shoum; Verdeli, Helen; Wickramaratne, Priya et al. (2016) Impact of a Father Figure's Presence in the Household on Children's Psychiatric Diagnoses and Functioning in Families at High Risk for Depression. J Child Fam Stud 25:588-597
Talati, Ardesheer; Pantazatos, Spiro P; Hirsch, Joy et al. (2015) A pilot study of gray matter volume changes associated with paroxetine treatment and response in social anxiety disorder. Psychiatry Res 231:279-85
Talati, Ardesheer; Guffanti, Guia; Odgerel, Zagaa et al. (2015) Genetic variants within the serotonin transporter associated with familial risk for major depression. Psychiatry Res 228:170-3
Pantazatos, Spiro P; Talati, Ardesheer; Schneier, Franklin R et al. (2014) Reduced anterior temporal and hippocampal functional connectivity during face processing discriminates individuals with social anxiety disorder from healthy controls and panic disorder, and increases following treatment. Neuropsychopharmacology 39:425-34

Showing the most recent 10 out of 19 publications