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The GABA A Receptor α 1 Subtype in the Ventral Pallidum Regulates Alcohol-Seeking Behaviors

2002; Society for Neuroscience; Volume: 22; Issue: 9 Linguagem: Inglês

10.1523/jneurosci.22-09-03765.2002

1529-2401

Scott C. Harvey, Katrina Foster, Pete F. McKay, Michelle Carroll, Regat Seyoum, James E. Woods, Collette Grey, Cecily M. Jones, Shannan McCane, Rancia Cummings, Dynesha Mason, Chunrong Ma, James M. Cook, Harry L. June,

Memory and Neural Mechanisms

We investigated the potential role of the α 1 -containing GABA A receptor in regulating the reinforcing properties of alcohol. To accomplish this, we developed 3-propoxy-β-carboline hydrochloride (3-PBC), a mixed agonist–antagonist benzodiazepine site ligand with binding selectivity at the α 1 receptor. We then tested the capacity of 3-PBC to block alcohol-maintained responding in the ventral pallidum (VP), a novel alcohol reward substrate, which primarily expresses the α 1 -receptor isoform. Our results demonstrated that bilateral microinfusion of 3-PBC (0.5–40 μg) in the anterior and medial VP produced marked reductions in alcohol-maintained responding in a genetically selected rodent model of alcohol drinking. The VP infusions showed both neuroanatomical and reinforcer specificity because no effects were seen in sites dorsal to the VP (e.g., nucleus accumbens, caudate putamen). The saccharin-maintained responding was reduced only with the highest dose (40 μg). Parenteral injections of 3-PBC (1–20 mg/kg) also showed a similar selectivity on alcohol-maintained responding. Complementary in vitro studies revealed that 3-PBC exhibited a low partial agonist efficacy profile at recombinant diazepam-sensitive receptors (e.g., α 1 β 3 γ 2 , α 2 β 3 γ, and α 3 β 3 γ 2 ). The selective suppression of 3-PBC on alcohol-maintained responding after central and parenteral administrations, together with its low-efficacy agonist profile, suggest that the reduction in alcohol-maintained behaviors was not attributable to a general suppression on consummatory behaviors. These results demonstrate that the α 1 -containing GABA A receptors in both the anterior and medial VP are important in regulating the reinforcing properties of alcohol. These receptors represent novel targets in the design and development of pharmacotherapies for alcohol-dependent subjects.