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Vol. 293, Issue 3, 1017-1026, June 2000
Harvard Medical School, New England Regional Primate Research
Center, Southborough, Massachusetts
Previous studies suggest that D1 receptor partial agonists may be
viable candidates for development as pharmacotherapies for cocaine
addiction. This study investigated the ability of the D1 receptor
partial agonists SKF 83959 and SKF 77434 to modulate the behavioral
effects of cocaine and compared these effects with those of the
reference D1 receptor antagonist SCH 39166 and D1 receptor agonists SKF
81297 and 6-Br-APB. Squirrel monkeys were trained either to respond
under a fixed-interval schedule of stimulus-shock termination or to
discriminate cocaine from vehicle (procedures useful for evaluating the
behavioral stimulant and subjective effects of cocaine, respectively).
Additional monkeys were studied with quantitative observational
techniques to evaluate the effects of the drugs on various forms of
motor behavior. Like SCH 39166, but unlike SKF 81297 and 6-Br-APB, the
D1 receptor partial agonists attenuated the behavioral stimulant and
discriminative stimulus effects of cocaine in a dose-dependent manner,
although maximum antagonism produced by SKF 77434 was not always as
great as that produced by SKF 83959 or SCH 39166. In observational
studies, SKF 83959 and SKF 77434 produced less severe disruptions in
motor behavior than did SCH 39166 and, for SKF 83959, showed a greater separation between the dose required to antagonize the behavioral effects of cocaine and the dose that induced catalepsy (
33-fold). These results suggest that D1 receptor partial agonists can act as
functional cocaine antagonists with less severe behavioral effects than
D1 receptor antagonists. The prominent cocaine-antagonist properties
and the low incidence of motoric side effects of SKF 83959 may reflect
its unique binding profile at D1 as well as nondopaminergic receptors.
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