Enhanced Rewarding Properties of Morphine, but not Cocaine, in {beta}arrestin-2 Knock-Out Mice

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The Journal of Neuroscience, November 12, 2003, 23(32):10265-10273

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Behavioral/Systems/Cognitive
Enhanced Rewarding Properties of Morphine, but not Cocaine, in ${beta}$ arrestin-2 Knock-Out Mice
Laura M. Bohn,¹ Raul R. Gainetdinov,² Tatyana D. Sotnikova,² Ivan O. Medvedev,² Robert J. Lefkowitz,³ Linda A. Dykstra,⁴ and Marc G. Caron²
¹Department of Pharmacology, The Ohio State University College of Medicine and Public Health, Columbus, Ohio 43210, Departments of ²Cell Biology and ³Biochemistry and Medicine, Duke University Medical Center, Howard Hughes Medical Institute Laboratories, Durham, North Carolina 27710, and ⁴University of North Carolina at Chapel Hill, Department of Psychology, Chapel Hill, North Carolina 27599

The reinforcing and psychomotor effects of morphine involveopiate stimulation of the dopaminergic system via activationof µ-opioid receptors (µOR). Both µ-opioidand dopamine receptors are members of the G-protein-coupledreceptor (GPCR) family of proteins. GPCRs are known to undergodesensitization involving phosphorylation of the receptor andthe subsequent binding of ${beta}$ arrestins, which prevents furtherreceptor-G-protein coupling. Mice lacking ${beta}$ arrestin-2 ( ${beta}$ arr2)display enhanced sensitivity to morphine in tests of pain perceptionattributable to impaired desensitization of µOR. However,whether abrogating µOR desensitization affects the reinforcingand psychomotor properties of morphine has remained unexplored.In the present study, we examined this question by assessingthe effects of morphine and cocaine on locomotor activity, behavioralsensitization, conditioned place preference, and striatal dopaminerelease in ${beta}$ arr2 knock-out ( ${beta}$ arr2-KO) mice and their wild-type(WT) controls. Cocaine treatment resulted in very similar neurochemicaland behavioral responses between the genotypes. However, inthe ${beta}$ arr2-KO mice, morphine induced more pronounced increasesin striatal extracellular dopamine than in WT mice. Moreover,the rewarding properties of morphine in the conditioned placepreference test were greater in the ${beta}$ arr2-KO mice when comparedwith the WT mice. Thus, ${beta}$ arr2 appears to play a more importantrole in the dopaminergic effects mediated by morphine than thoseinduced by cocaine.

Key words: morphine; cocaine; dopamine; ${beta}$ arrestin; knock-out mice; locomotor activity; sensitization; microdialysis; conditioned place preference

Received June 30, 2003; revised September 11, 2003; accepted September 17, 2003.

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