Abstract

This research component had its origins as part of the Human Genetics Core Resource in the original application for the Indiana Alcohol Research Center (ARC). It is now a separate component which consolidates and supports alcohol challenge studies in twins and families while continuing to rely on the Human Genetics and Database Core Resource for statistical support and zygosity confirmation. During the first years of the ARC, multiple physiological and biobehavioral variables were studied and many were found to have evidence for significant genetic effects. The strongest evidence for genetic control of the acute effects of alcohol was found for electroencephalographic (EEG) changes after alcohol. Variability within dizygotic (DZ) twin-pairs increased markedly after alcohol while the variability within monozygotic (MZ) pairs generally decreased indicating the presence of genetic influences. The relative changes in the within- pair variability for the two zygosities was so great that multiple additive heritability (estimates of the fraction of total variance due to genetic variance) values were found greater than the theoretical upper limit of 1.0. This suggested an upward bias of heritability due to gene interactions. The post-alcohol heritability values were the largest in the alpha-slow (7.6 - 10.0 Hertz) and beta-slow (12.6 - 20.0 Hertz) frequency bands and over the frontal lobes. The Human Genetics Research Component will continue twin studies of the acute effects of alcohol, development of acute tolerance to alcohol and placebo effects on EEG changes and related biobehavioral variables. These twin studies will be carried out both in a clinical research hospital ward in Indianapolis and in the Department of Psychology in Bloomington. Studies comparing family history positive and family history negative young adult males will also be carried out in Bloomington. The results of these studies will be used to develop a protocol designed to detect segregation of single genes in families of twins with extreme responses to alcohol.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Alcohol Abuse and Alcoholism (NIAAA)
Type
Specialized Center (P50)
Project #
5P50AA007611-08
Application #
3726035
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
8
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Indiana University Bloomington
Department
Type
DUNS #
006046700
City
Bloomington
State
IN
Country
United States
Zip Code
47401

  Publications

McClintick, Jeanette N; McBride, William J; Bell, Richard L et al. (2018) Gene expression changes in the ventral hippocampus and medial prefrontal cortex of adolescent alcohol-preferring (P) rats following binge-like alcohol drinking. Alcohol 68:37-47
Houck, Christa A; Grahame, Nicholas J (2018) Acute drug effects on habitual and non-habitual responding in crossed high alcohol preferring mice. Psychopharmacology (Berl) 235:2167-2175
Öztürk, Nail Can; Resendiz, Marisol; Öztürk, Hakan et al. (2017) DNA Methylation program in normal and alcohol-induced thinning cortex. Alcohol 60:135-147
Ding, Zheng-Ming; Ingraham, Cynthia M; Hauser, Sheketha R et al. (2017) Reduced Levels of mGlu2 Receptors within the Prelimbic Cortex Are Not Associated with Elevated Glutamate Transmission or High Alcohol Drinking. Alcohol Clin Exp Res 41:1896-1906
Linsenbardt, David N; Smoker, Michael P; Janetsian-Fritz, Sarine S et al. (2017) Impulsivity in rodents with a genetic predisposition for excessive alcohol consumption is associated with a lack of a prospective strategy. Cogn Affect Behav Neurosci 17:235-251
Bell, Richard L; Hauser, Sheketha R; Liang, Tiebing et al. (2017) Rat animal models for screening medications to treat alcohol use disorders. Neuropharmacology 122:201-243
Luczak, Susan E; Wall, Tamara L (2016) Gambling problems and comorbidity with alcohol use disorders in Chinese-, Korean-, and White-American college students. Am J Addict 25:195-202
Ding, Zheng-Ming; Ingraham, Cynthia M; Rodd, Zachary A et al. (2016) Alcohol drinking increases the dopamine-stimulating effects of ethanol and reduces D2 auto-receptor and group II metabotropic glutamate receptor function within the posterior ventral tegmental area of alcohol preferring (P) rats. Neuropharmacology 109:41-48
Kasten, C R; Frazee, A M; Boehm 2nd, S L (2016) Developing a model of limited-access nicotine consumption in C57Bl/6J mice. Pharmacol Biochem Behav 148:28-37
Zhou, Feng C; Resendiz, Marisol; Lo, Chiao-Ling et al. (2016) Cell-Wide DNA De-Methylation and Re-Methylation of Purkinje Neurons in the Developing Cerebellum. PLoS One 11:e0162063

Showing the most recent 10 out of 253 publications