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Microinjections of dopamine agonists in the nucleus accumbens increase ethanol-reinforced responding

pmid: 1357676
Long-Evans rats (N = 3) were trained to lever press on a fixed-ratio 4 (FR 4) schedule with ethanol (10% v/v) presented as the reinforcer. Each rat received a total of six bilateral nucleus accumbens microinjections, one per week. They were tested with one physiological saline control, three 20.0-microgram/brain d-amphetamine, and two 6.0-microgram/brain quinpirole injections given 10 min prior to operant sessions. Ethanol-reinforced responding terminated after approximately 10 min during control sessions. Microinjections of the D2 agonist quinpirole and the nonspecific dopamine (DA) agonist d-amphetamine increased total responding but produced slowed response rates that continued for 45-60 min. The slowed response rate produced by d-amphetamine resulted in a peak increase in interresponse times (IRTs) between 8-10 s, whereas quinpirole increased IRTs in the 14- to 16-s range, indicating that nonspecific DA activation resulted in higher rates of ethanol-reinforced responding than specific D2 activation although both drugs decreased local response rates. These data indicate that the amount and temporal extent of ethanol-reinforced responding are increased by microinjections of DA agonists in the nucleus accumbens and support the hypothesis that DA activity in this region is involved in the regulation of ethanol-reinforced responding.
- University of Mary United States
- Washington State University United States
Male, Dextroamphetamine, Quinpirole, Ethanol, Microinjections, Dopamine Agents, Nucleus Accumbens, Rats, Animals, Conditioning, Operant, Ergolines, Reinforcement, Psychology
Male, Dextroamphetamine, Quinpirole, Ethanol, Microinjections, Dopamine Agents, Nucleus Accumbens, Rats, Animals, Conditioning, Operant, Ergolines, Reinforcement, Psychology
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