Abstract

Alcohol abuse and alcoholism are significant problems in society, and ethanol (EtOH) withdrawal represents one of many serious consequences of chronic drinking. Given the fact that many individuals experience multiple EtOH withdrawal, and that repeated detoxifications have been shown to progressively intensity in severity, it is clear that treatment strategies need to be evaluated for their ability to effectively and (and safely) address this sensitization of """"""""kindling"""""""" of EtOH withdrawal syndromes. Our models of EtOH withdrawals is really suited to address this clinically relevant research issues since evaluations of pharmacologic treatments in preventing or blocking behavioral indices of sensitized withdrawal hyperexcitability may also be extended to evaluation of their effects against electrophysiological and molecular correlates of this withdrawal sensitization phenomenon. A series of anticonvulsant drugs that influence activity at GABAa and NMDA receptor systems (important neural substrates of EtOH withdrawal) will be evaluated for their ability to block or attenuate the development and/or expression of 1) behavioral indices of sensitized withdrawal-related CNS or attenuate the development and/or expression of 1) behavioral indices of sensitized withdrawal-related CNS hyperexcitability, 2) sensitization of electrographic measures of withdrawal-related CNS hyperexcitability and 3) molecular alterations (mRNA and protein expression) of GABAA and NMDA receptor subunits associated with repeated ethanol intoxication and withdrawal. Taken together, the proposed work will employ an established model of multiple EtOH withdrawals and a multi-disciplinary approach in evaluating the efficacy of pharmacologic agents in treating behavioral, electrophysiological and molecular indices of withdrawal sensitization. Results from these studies will provide clinically-relevant information about pharmacotherapy strategies for treating EtOH withdrawal and importantly, the potentially long-term deleterious consequences related to multiple EtOH withdrawal.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Alcohol Abuse and Alcoholism (NIAAA)
Type
Specialized Center (P50)
Project #
5P50AA010761-07
Application #
6563197
Study Section
Project Start
2002-01-01
Project End
2002-12-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
7
Fiscal Year
2002
Total Cost
$242,857
Indirect Cost

  Institution

Name
Medical University of South Carolina
Department
Type
DUNS #
183710748
City
Charleston
State
SC
Country
United States
Zip Code
29425

  Publications

Gioia, Dominic A; Xu, Minfu; Wayman, Wesley N et al. (2018) Effects of drugs of abuse on channelrhodopsin-2 function. Neuropharmacology 135:316-327
Anton, Raymond F; Latham, Patricia K; Voronin, Konstantin E et al. (2018) Nicotine-Use/Smoking Is Associated with the Efficacy of Naltrexone in the Treatment of Alcohol Dependence. Alcohol Clin Exp Res 42:751-760
Anderson, Ethan M; Larson, Erin B; Guzman, Daniel et al. (2018) Overexpression of the Histone Dimethyltransferase G9a in Nucleus Accumbens Shell Increases Cocaine Self-Administration, Stress-Induced Reinstatement, and Anxiety. J Neurosci 38:803-813
Osterndorff-Kahanek, Elizabeth A; Tiwari, Gayatri R; Lopez, Marcelo F et al. (2018) Long-term ethanol exposure: Temporal pattern of microRNA expression and associated mRNA gene networks in mouse brain. PLoS One 13:e0190841
Stewart, Scott H; Reuben, Adrian; Anton, Raymond F (2018) Reply: Carbohydrate Deficient Transferrin in Patients with Cirrhosis: A Tale of Bridges. Alcohol Alcohol 53:351-352
Kearney-Ramos, Tonisha E; Lench, Daniel H; Hoffman, Michaela et al. (2018) Gray and white matter integrity influence TMS signal propagation: a multimodal evaluation in cocaine-dependent individuals. Sci Rep 8:3253
Haun, Harold L; Griffin, William C; Lopez, Marcelo F et al. (2018) Increasing Brain-Derived Neurotrophic Factor (BDNF) in medial prefrontal cortex selectively reduces excessive drinking in ethanol dependent mice. Neuropharmacology 140:35-42
Schacht, Joseph P; Voronin, Konstantin E; Randall, Patrick K et al. (2018) Dopaminergic Genetic Variation Influences Aripiprazole Effects on Alcohol Self-Administration and the Neural Response to Alcohol Cues in a Randomized Trial. Neuropsychopharmacology 43:1247-1256
McGuier, Natalie S; Rinker, Jennifer A; Cannady, Reginald et al. (2018) Identification and validation of midbrain Kcnq4 regulation of heavy alcohol consumption in rodents. Neuropharmacology 138:10-19
Nimitvilai, Sudarat; Lopez, Marcelo F; Woodward, John J (2018) Effects of monoamines on the intrinsic excitability of lateral orbitofrontal cortex neurons in alcohol-dependent and non-dependent female mice. Neuropharmacology 137:1-12

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