给予吗啡、纳曲酮和地西泮后大鼠适口性饮酒。

Substance and alcohol actions/misuse Pub Date : 1982-01-01
S J Cooper
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引用次数: 0

摘要

在没有耗尽体液区室的情况下,大鼠摄入了过量的非常可口的0.005M糖精钠溶液。这种味道强烈地促进了饮酒,随之而来的液体消耗被证明对阿片受体阻断非常敏感。纳曲酮的剂量低至0.03 mg/kg,可显著减少在获得治疗的第一个小时内糖精溶液的消耗。纳曲酮治疗不影响饮酒潜伏期,其抑制作用是短暂的,表明它不会立即或持久地避免糖精溶液。纳曲酮诱导的抑制也不是由于引起的压力或焦虑,因为同时服用地西泮并没有逆转纳曲酮的作用。吗啡(0.3 ~ 3.0 mg/kg)在6小时的试验期内不能增加糖精溶液的摄入量。吗啡(10mg /kg)导致运动不动和长期抑制饮酒,随后出现继发性高渗反应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Palatability-induced drinking after administration of morphine, naltrexone and diazepam in the non-deprived rat.

Rats consumed excessive quantities of a highly palatable 0.005M sodium saccharin solution in the absence of depletion of body fluid compartments. The taste strongly promoted drinking, and the consequent fluid consumption proved to be very sensitive to opiate receptor blockade. Naltrexone, at a dose as small as 0.03 mg/kg, significantly attenuated consumption of the saccharin solution in the first hour of access. The naltrexone treatment did not affect latency to drink, and its suppressant effect was transient, indicating that it did not induce either immediate or lasting avoidance of the saccharin solution. The naltrexone-induced suppression was also not due to elicited stress or anxiety, since concurrent administration of diazepam did not reverse the naltrexone effect. Morphine (0.3-3.0 mg/kg) failed to enhance saccharin solution intake over a 6 hr test period. Morphine (10 mg/kg) produced immobility and an extended suppression of drinking, which was followed by a secondary hyperdipsic response.

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