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Vol. 289, Issue 1, 110-122, April 1999
Department of Psychiatry, University of California at San Francisco
and San Francisco Veterans Affairs Medical Center, San Francisco,
California (B.K.T., L.B.H., L.M.F., K.H., S.P.B.); and
Psychobiology
Section, National Institute on Drug Abuse-Intramural Research Program,
National Institutes of Health, Baltimore, Maryland (A.H.N., J.L.K.)
The current studies evaluated the novel diphenylmethoxytropane analog
4-chlorobenztropine (4-Cl-BZT), cocaine, and combinations of the two
drugs for their abilities to stimulate locomotor activity, produce
cocaine-like discriminative stimulus effects, and elevate extracellular
dopamine (DA) in the nucleus accumbens (NAc) as measured by in vivo
microdialysis. Peripherally administered cocaine was approximately
twice as efficacious as 4-Cl-BZT as a locomotor stimulant and was
behaviorally active at a lower dose than was 4-Cl-BZT. Cocaine also was
more efficacious than 4-Cl-BZT in producing discriminative-stimulus
effects in rats trained to discriminate i.p. injections of 10 mg/kg
cocaine from saline. The time course of behavioral activation differed
markedly between the two drugs, with much shorter onset and duration of
locomotor stimulant effects for cocaine relative to 4-Cl-BZT.
Similarly, i.p. cocaine (10 and 40 mg/kg) induced a pronounced, rapid,
and short-lived increase in DA in the NAc, whereas i.p. 4-Cl-BZT was
effective only at the higher dose and produced a more gradual, modest,
and sustained (
2 h) elevation in accumbens DA. In contrast to i.p.
administration, local infusion of 4-Cl-BZT (1-100 µM) into the NAc
through the microdialysis probe elevated extracellular DA to a much
greater extent than did local cocaine (nearly 2000% of baseline
maximally for 4-Cl-BZT versus 400% of baseline for cocaine) and
displayed a much longer duration of action than cocaine. However, when
microinjected bilaterally into the NAc at 30 or 300 nmol/side, cocaine
remained a more efficacious locomotor stimulant than 4-Cl-BZT. Finally, pretreatment with i.p. 4-Cl-BZT dose dependently enhanced the locomotor
stimulant, discriminative stimulus effects, and NAc DA response to a
subsequent low-dose i.p. cocaine challenge. The diphenylmethoxytropane
analog also facilitated the emergence of stereotyped behavior and
convulsions induced by high-dose cocaine. The current results
demonstrate that DA transporter ligands that do not share the
neurochemical and behavioral profiles of cocaine nevertheless may
enhance the effects of cocaine in vivo.
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