4.7 Article

Prenatal exposure to cocaine increases the rewarding potency of cocaine and selective dopaminergic agonists in adult mice

Journal

BIOLOGICAL PSYCHIATRY
Volume 63, Issue 2, Pages 214-221

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.biopsych.2007.01.014

Keywords

brain stimulation-reward; BSR; gestation; ICSS; in utero; intracranial self-stimulation; psychostimulant

Funding

  1. NIDA NIH HHS [DA015429, R29 DA008648, R01 DA012736-02, DA012736, K08 DA015429, K02 DA000354, DA000354, K08 DA015429-04, K02 DA000354-07, R01 DA008648-07, R01 DA008648, R01 DA012736, R01 DA012736-01A2, K02 DA000354-05, R01 DA012736-03, DA008648, R01 DA008648-08, K02 DA000354-06A2] Funding Source: Medline

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Background: Substance abuse during pregnancy results in persistent affective and behavioral deficits in drug-exposed children, and increased rates of substance abuse have been observed in young adults prenatally exposed to drugs of abuse. Animal models of prenatal cocaine exposure have yielded differing results depending on the behavioral method used to assess drug potency. Methods: The effects of cocaine, the dopamine D1 agonists SKF-81297 and SKF-82958, and the D2 agonist quinpirole on intracranial self-stimulation were measured in adult Swiss-Webster mice exposed to cocaine in utero (40 mg/kg/day) and vehicle controls with the curve-shift method of brain stimulation-reward (BSR) threshold determination. Results: The reward-potentiating effects of cocaine (0.3-30 mg/kg IP) and SKF-82958 but not SKF-81297 on BSR were increased in adult male but not female mice after prenatal cocaine exposure. Quinpirole exerted biphasic effects on BSR, both elevating (0.1-0.3 mg/kg IP) and lowering (1.0-10 mg/kg IP) reward thresholds. Both effects of quinpirole were also enhanced in adult male mice after prenatal cocaine exposure. Conclusions: Prenatal cocaine exposure results in increased reward-potentiating potency of cocaine on BSR in adult mice in a sexually-dimorphic manner. This augmented rewarding effect of cocaine is also associated with increased sensitivity to both D1- and D2-selective agonists.

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