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Vol. 298, Issue 1, 172-179, July 2001
Department of Psychology (S.B.H., J.E.K., M.T.B.) and College of
Pharmacy (L.P.D., P.A.C.), University of Kentucky, Lexington, Kentucky
-Lobeline inhibits d-amphetamine-evoked
dopamine release from striatal slices in vitro, appearing to reduce the
cytosolic pool of dopamine available for reverse transport by the
dopamine transporter. Based on this neurochemical mechanism of action, the present study determined if lobeline decreases
d-methamphetamine self-administration. Rats were
surgically implanted with jugular catheters and were trained to lever
press on a fixed ratio 5 schedule for intravenous
d-methamphetamine (0.05 mg/kg/infusion). To assess the
specificity of the effect of lobeline, another group of rats was
trained to lever press on a fixed ratio 5 schedule for sucrose reinforcement. Pretreatment of rats with lobeline (0.3-3.0 mg/kg, 15 min prior to the session) decreased responding for both
d-methamphetamine and sucrose reinforcement. Following
repeated lobeline (3.0 mg/kg) administration, tolerance developed to
the decrease in responding for sucrose; however, the lobeline-induced
decrease in responding for d-methamphetamine persisted.
Furthermore, the lobeline-induced decrease in responding for
d-methamphetamine was not surmounted by increasing the
unit dose of d-methamphetamine. These results suggest
that lobeline produces a nonspecific rate suppressant effect following
acute administration, to which tolerance develops following repeated
administration. Importantly, the results also suggest that repeated
administration of lobeline specifically decreases responding for
d-methamphetamine in a noncompetitive manner. Thus,
lobeline may be an effective, novel pharmacotherapy for
d-methamphetamine abuse.
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