John C. DeFries - US grants

A Drug Abuse Research Center (DARC) is proposed to be established at the Institute for Behavioral Genetics (IBG), University of Colorado, Boulder. Faculty members of IBG are nationally and internationally known for their research in quantitative genetics of human behavioral characters (including cognition, reading disability, personality development, and responses to alcohol) and in behavioral pharmacogenetics. Thus, establishment of a DARC at IBG would facilitate a multidisciplinary approach to the problem of vulnerability to drug abuse. The Research Components proposed include (1) quantitative genetic analyses of the cigarette withdrawal syndrome; (2) a study of the families of severe substance-abusing teenagers; 3) assessment of the tension-reduction hypothesis of nicotine's action and development of animal models of cigarette withdrawal; (4) studies of the effects of amphetamine, cocaine, ethanol, and morphine on neurotensin and dopamine levels in mesolimbic and mesocortical dopaminergic pathways in 8 strains of mice; (5) application of genetic strategies to delineate predispositional factors for cocaine hepatotoxicity, and studies of their potential application to cocaine use and toxicity in humans: (6) studies of the development of tolerance and physical dependence to cocaine and amphetamine in lines of mice selected for high or low open-field activity, and the effects of these drugs on learning and memory in these lines; (7) bi-directional selective breeding to produce replicate lines of mice which differ in responses to nicotine, and to cocaine; and (8) determination of the relationship between cocaine initial sensitivity, tolerance or sensitization acquisition, and withdrawal severity in inbred strains of mice. The investigators will benefit by sharing scientific resources such as the specific-pathogen-free mouse facility and twin/adoptee registers, and from comparing results derived from a common database of inbred strains and selected lines of mice to those derived from human subjects. Results obtained from research conducted within the proposed DARC should contribute to a better understanding of the etiology of individual differences in drug- related behaviors, and should add a valuable knowledge base for clinical intervention strategies for the individual.

The long-range objective of the Colorado Learning Disabilities Research Center are the identification, characterization, validation and amelioration of etiologically distinct subtypes or dimensions of learning disabilities. To accomplish these objectives, test batteries that include psychometric measures of cognitive and academic abilities (Research Project 2), reading, language and perceptual processes (Research Project 3), and ADHD and executive functions (Research Project 3 will be administered to a sample of 50 pairs of identical twins and 50 pairs of fraternal twin in which at least one member of each pair is reading disabled, to an independent sample of 50 pairs of identical twins and 50 pairs of fraternal twins in which at least one member of each pair has ADHD, and to a comparison group of 50 pairs of identical twins and 50 pairs of fraternal twins with no school history of learning disabilities or ADHD. Resulting data will be used to asses the genetic and environmental etiologies of reading deficits and ADHD, as well as their covariation with measures of mathematics performance, phonological and orthographic coding, and executive functions. In order to map major genes and/or quantitative trait loci that influence learning disabilities, blood samples will be drawn from fraternal twin pairs and subjected to genetic linkage analyses (Research Project 4). Concurrently, a longitudinal at-risk sample of 100 children will be administered differential computer-based remediation to test for possible subtype-by-treatment interactions (Research Project 5). In order to assess genetic and environmental correlates of neurobiological factors and reading deficits, MRI scans will be obtained from 100 twin pairs in which at least one member of each pair is reading disabled and from 25 pairs of control twin pairs and then subjected to state-of-the-art morphometric analyses (Research Project 6). An administrative core unit will be responsible for coordinating the activities of the six research projects; maintaining communication among the participating investigators; ascertaining and scheduling subjects; obtaining questionnaire data from families of twins; obtaining blood samples from families of fraternal twins; compiling and managing a master file of combined data sets; and administering the Center budget and other fiscal matters.

The long-range objectives of Research Project 1 are the identification, characterization, and validation of etiologically distinct subtypes or dimensions of learning disabilities. To accomplish these objectives, an extensive psychometric test battery will be administered to a sample of 50 pairs of identical twins and 50 pairs of fraternal twins in which at least one member of each pair is reading disabled, to an independent sample of 50 pairs of identical twins and 50 pairs of fraternal twins in which at least one member of each pair has ADHD, and to a comparison sample of 50 pairs of identical twins and 50 pairs of fraternal twins with a school history of no significant reading deficits or behavioral problems. In collaboration with investigators from Research Projects 2-6, resulting data will be used to assess the genetic and environmental etiologies of reading deficits and ADHD, as well as their covariation with measures of reading, language and perceptual processes, mathematics performance, executive functions, and brain morphometry. Reading performance data will also be used to test hypotheses of differential etiology as a function of age, gender, and cognitive ability, and to test the hypothesis that the etiology of deviant scores differs from that of individual differences within the normal range.

DESCRIPTION: Objective: The proposed research aims to build knowledge about family determinants of children's social and economic well being as children come into their own and make the transition to adulthood. Specific hypotheses address familial influences on educational attainment, family determinants of union- and family-formation choices of young adults, and how the quality of early family relationships shapes adult child-parent relationships. Methods: The investigators address these questions in the context of an adoption design which offers an opportunity to carry out especially powerful tests of socialization and social-psychological theories. The adoption design is 'powerful' because it allows them to test family determinants of children's outcomes independently of genetic influences. They capitalize on the resources of the Colorado Adoption Project (CAP), a long-term, longitudinal adoption study of 245 adoptive families and 245 nonadoptive families. The CAP children, their siblings, and their home environments have been assessed repeatedly since infancy using a broad, multivariate battery of social, environmental, and behavioral measures. The investigators propose to interview the probands and their siblings as they reach adulthood. Significance: The proposed research is innovative, both in the fields of behavioral genetics and in social demography, in that it brings behavioral genetic methods to bear 1) on sociological and social-demographic phenomena and 2) on the study of life-course developmental process. The marriage of behavioral genetics and social demography promises to advance understanding of how family factors influence children's life chances and to enrich socializ-ation models of life-course development.