Abstract

Previous in vivo electrophysiological studies across differing brain regions demonstrated ethanol enhancement of GABA responses from some, but not all, neurons. This differential effect of ethanol was attributed to a variable action on diverse GABAA receptor subtypes. In contrast to ethanol's consistent enhancement of GABA function in vivo, GABA responses from isolated neurons in vitro were rarely enhanced by ethanol (Preliminary Data). Based upon the contrast of our in vivo and in vitro results, it was proposed that a factor, not available to isolated neurons in vitro, allowed ethanol's action in vivo. Based upon the presence of auxiliary binding sites on GABAA receptors, it was hypothesized that endogenous compounds acting on one or more of the auxiliary sites were important for ethanol to alter the action of GABA responsiveness in vitro. In support of this explanation, our laboratory recently discovered that ethanol enhanced GABA responses from most dissociated substantia nigra reticulata (SNR) neurons in the presence of a neurosteroid agonist, alphaxalone, while having no effect on GABA responses in the absence of this neurosteroid (Preliminary Data). Therefore, the present proposal will test the hypothesis that activation of specific neurosteroid sites on GABAA receptors facilitates ethanol enhancement of GABA responses from isolated neurons.
Four Specific Aims will test this view.
In Specific Aim I, several classes of neurosteroids will be examined for their ability to allow ethanol enhancement of GABA activity from isolated SNR cells. It is assumed that the differing neurosteroids will not have identical effects on the action of ethanol to enhance GABA responses.
Specific Aim II will determine if a GABA-enhancing neurosteroid will result in ethanol having a differential influence on responsiveness to GABA from neurons isolated from selected brain regions where ethanol in vivo has varying effects on GABA function.
Specific Aim III will determine the mRNAs for the GABAA receptor subunits in individual neurons sensitive and insensitive to ethanol's action to enhance GABA responses in the presence of neurosteroid. From the mRNAs in individual neurons, """"""""candidate"""""""" GABAA receptors responsible for the differential actions of ethanol will be identified with correlational analysis. This will allow further testing of the hypothesis that selected GABAA receptor subtypes account for the variable actions of ethanol on GABA responsiveness in the presence of a neurosteroid.
For Specific Aim I V, cDNAs for the """"""""candidate"""""""" receptor subunits will be transfected into modified HEK cells to validate that neurosteroids will result in the expected response pattern to ethanol on GABA function observed from neurons. Additionally, neurons and cells with a preponderance of type-l-BZD receptors will be transduced with selected GABAA receptor subunit mutants to explore the potential molecular sites responsible for the neurosteroid influence on ethanol's action. Completion of the Aims will allow critical new information to emerge concerning the molecular basis of neurosteroid action on GABAA receptor function that allows ethanol to enhance GABA function in vitro.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Alcohol Abuse and Alcoholism (NIAAA)
Type
Research Project (R01)
Project #
5R01AA012655-04
Application #
6640781
Study Section
Alcohol and Toxicology Subcommittee 4 (ALTX)
Program Officer
Twombly, Dennis
Project Start
2000-06-01
Project End
2005-05-31
Budget Start
2003-06-01
Budget End
2004-05-31
Support Year
4
Fiscal Year
2003
Total Cost
$291,000
Indirect Cost

  Institution

Name
University of North Carolina Chapel Hill
Department
Psychiatry
Type
Schools of Medicine
DUNS #
608195277
City
Chapel Hill
State
NC
Country
United States
Zip Code
27599

  Publications

Kelm, M Katherine; Criswell, Hugh E; Breese, George R (2011) Ethanol-enhanced GABA release: a focus on G protein-coupled receptors. Brain Res Rev 65:113-23
Breese, George R; Sinha, Rajita; Heilig, Markus (2011) Chronic alcohol neuroadaptation and stress contribute to susceptibility for alcohol craving and relapse. Pharmacol Ther 129:149-71
Huang, Mae M; Overstreet, David H; Knapp, Darin J et al. (2010) Corticotropin-releasing factor (CRF) sensitization of ethanol withdrawal-induced anxiety-like behavior is brain site specific and mediated by CRF-1 receptors: relation to stress-induced sensitization. J Pharmacol Exp Ther 332:298-307
Breese, George R; Knapp, Darin J; Overstreet, David H et al. (2008) Repeated lipopolysaccharide (LPS) or cytokine treatments sensitize ethanol withdrawal-induced anxiety-like behavior. Neuropsychopharmacology 33:867-76
Breese, G R; Criswell, H E; Carta, M et al. (2006) Basis of the gabamimetic profile of ethanol. Alcohol Clin Exp Res 30:731-44
Breese, George R; Overstreet, David H; Knapp, Darin J (2005) Conceptual framework for the etiology of alcoholism: a ""kindling""/stress hypothesis. Psychopharmacology (Berl) 178:367-80
Criswell, Hugh E; Ming, Zhen; Pleasant, Nathanial et al. (2004) Macrokinetic analysis of blockade of NMDA-gated currents by substituted alcohols, alkanes and ethers. Brain Res 1015:107-13
Breese, George R; Knapp, Darin J; Overstreet, David H (2004) Stress sensitization of ethanol withdrawal-induced reduction in social interaction: inhibition by CRF-1 and benzodiazepine receptor antagonists and a 5-HT1A-receptor agonist. Neuropsychopharmacology 29:470-82
Knapp, Darin J; Overstreet, David H; Moy, Sheryl S et al. (2004) SB242084, flumazenil, and CRA1000 block ethanol withdrawal-induced anxiety in rats. Alcohol 32:101-11
Criswell, Hugh E; Ming, Zhen; Griffith, Benjamin L et al. (2003) Comparison of effect of ethanol on N-methyl-D-aspartate- and GABA-gated currents from acutely dissociated neurons: absence of regional differences in sensitivity to ethanol. J Pharmacol Exp Ther 304:192-9

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