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Vol. 294, Issue 2, 613-619, August 2000
Departments of Cellular Biology, Neurobiology and Anatomy (Z.-X.X.,
E.A.S.), Psychiatry and Behavioral Medicine (E.A.S.), Pharmacology and
Toxicology (E.A.S.), and The Biophysics Research Institute
(E.A.S.), Medical College of Wisconsin, Milwaukee, Wisconsin
Opiate reinforcement has been hypothesized to be mediated by an
inhibition of mesolimbic 
-aminobutyric acid (GABA) release that
subsequently disinhibits ventral tegmental area (VTA) dopamine neurons.
In support of this hypothesis, this study demonstrates that when
administered directly into the lateral ventricle, the VTA, or the
ventral pallidum, but not the nucleus accumbens, -vinyl-GABA (GVG, an irreversible GABA-transaminase inhibitor, 20-50 µg) dose dependently blocked heroin (0.06 mg/kg) self-administration (SA), as
assessed by an increase in heroin SA at low doses of GVG and an initial
increase followed 1 to 2 h later by a blockade of heroin SA at
higher GVG doses. This effect lasted 3 to 5 days. In drug-naïve rats, intra-VTA GVG pretreatment also prevented or delayed acquisition of heroin SA for 2 days. This GVG effect was prevented or reversed by
systemic or intra-VTA pretreatment with the GABAB
antagonist 2-hydroxysaclofen, but not the GABAA antagonist
bicuculline. Similarly, coadministration of heroin with
aminooxy-acetic acid (1-4 mg/kg) or
ethanolamine-O-sulfate (50-100 mg/kg), two reversible
GABA transaminase inhibitors, dose dependently reduced heroin
reinforcement. Coadministration of (±)-nipecotic acid (0.1-5 mg/kg)
with heroin, or intra-VTA or -ventral pallidum pretreatment with
(±)-nipecotic acid (10 µg) or NO-711 (2 µg), two GABA
uptake inhibitors, significantly increased heroin SA behavior, an
effect also blocked by systemic 2-hydroxysaclofen, but not bicuculline.
Taken together, these experiments, for the first time, demonstrate that
pharmacological elevation of mesolimbic GABA concentration blocks
heroin reinforcement by activating GABAB receptors,
supporting the GABAergic hypothesis of opiate reinforcement and the
incorporation of GABA agents in opiate abuse treatment.
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