RO-15-4513 SELECTIVELY ATTENUATES ETHANOL, BUT NOT SUCROSE, REINFORCED RESPONDING IN A CONCURRENT ACCESS PROCEDURE - COMPARISON TO OTHER DRUGS

被引:36
作者
PETRY, NM [1 ]
机构
[1] HARVARD UNIV,DEPT PSYCHOL,CAMBRIDGE,MA 02138
关键词
ETHANOL SELF-ADMINISTRATION; RO; 15-4513; CHLORDIAZEPOXIDE; NALOXONE; MORPHINE; LEVER-PRESS; RATS;
D O I
10.1007/BF02245630
中图分类号
Q189 [神经科学];
学科分类号
071006 ;
摘要
The experiments described in this report used a concurrent access procedure to study ethanol reinforcement. Rats were trained to lever press for a 10% sucrose solution and a 10% ethanol/10% sucrose mixture, and both reinforcers were available on variable-interval 5-s schedules. In baseline and vehicle injection sessions, the animals distributed their responding between both solutions. When injected with the partial inverse benzodiazepine agonist Ro 15-4513 (3, 9, and 18 mg/kg), responding for the ethanol solution decreased while responding for sucrose remained intact, Ethanol injections (0.5 and 1.0 g/kg) engendered a similar profile. Chlordiazepoxide led to an increase in ethanol mix responding at 2 mg/kg and a decrease in ethanol mix responding at higher doses; no dose affected sucrose responding. Morphine (0.5-16 mg/kg) decreased responding for both the ethanol mix and sucrose solutions, more or less simultaneously. Naloxone (0.125-20 mg/kg) selectively reduced ethanol mix responding at low doses, and decreased responding for both reinforcers at high doses. In another group of animals, isocaloric alternatives were concurrently available: 10% ethanol/0.25% saccharin versus 14% sucrose. Injections of Ro 15-4513 and chlordiazepoxide produced similar results as in the first group of rats: an increase in ethanol mix responding with low dose chlordiazepoxide, and a decrease in ethanol mix responding with Ro 15-4513. However, naloxone injections did not selectively affect responding for either of the reinforcers when they were isocaloric. These results are discussed in terms of ethanol's neuropharmacological actions.
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页码:192 / 203
页数:12
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