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大鼠乙醇强化行为:纳曲酮的作用

Ethanol-reinforced behaviour in the rat: effects of naltrexone.

作者信息

Bienkowski P, Kostowski W, Koros E

机构信息

Department of Pharmacology and Physiology of the Nervous System, Institute of Psychiatry and Neurology, Warsaw, Poland.

出版信息

Eur J Pharmacol. 1999 Jun 25;374(3):321-7. doi: 10.1016/s0014-2999(99)00245-9.

Abstract

It has been repeatedly reported that endogenous opioid pathways play an important role in ethanol drinking behaviour. In line with these findings, a non-selective opioid receptor antagonist, naltrexone, seems to reduce relapse rates in detoxified alcoholics. The aim of the present study was to evaluate the effects of naltrexone on (i) ethanol self-administration; (ii) extinction of responding for ethanol; (iii) reinstatement of ethanol-seeking induced by non-contingent presentations of ethanol-associated stimuli. Male Wistar rats were trained to lever-press for 8% ethanol in an operant procedure where ethanol was introduced in the presence of sucrose. The selectivity of naltrexone's actions was assessed by studying its effects on water-reinforced behaviour in separate control experiments. Acute injections of naltrexone (1 or 3 mg/kg) did not alter ethanol self-administration. Repeated treatment with naltrexone (3 mg/kg, before three consecutive self-administration sessions) progressively reduced ethanol intake. In the extinction procedure, acute administration of 3 mg/kg naltrexone suppressed responding previously reinforced with ethanol. Similarly, naltrexone (1-3 mg/kg) potently and dose-dependently inhibited reinstatement of ethanol-seeking produced by non-contingent deliveries of the liquid dipper filled with 8% ethanol. In the control experiments, lower doses of naltrexone (1-3 mg/kg) did not exert any effect on either reinforced or non-reinforced (extinction) lever-pressing for water. These results indicate that: (i) subchronic treatment with naltrexone leads to progressive reduction of ethanol self-administration; (ii) single doses of naltrexone may increase extinction and attenuate cue-induced reinstatement of ethanol-reinforced behaviour.

摘要

已有多次报道称内源性阿片肽通路在乙醇饮用行为中起重要作用。与这些发现一致,一种非选择性阿片受体拮抗剂纳曲酮似乎能降低戒酒者的复发率。本研究的目的是评估纳曲酮对以下方面的影响:(i)乙醇自我给药;(ii)对乙醇反应的消退;(iii)由非条件呈现与乙醇相关的刺激所诱导的乙醇寻求行为的恢复。雄性Wistar大鼠在一种操作性程序中接受训练,通过杠杆按压获取8%的乙醇,该程序中乙醇是在有蔗糖的情况下引入的。通过在单独的对照实验中研究纳曲酮对水强化行为的影响来评估其作用的选择性。急性注射纳曲酮(1或3毫克/千克)不会改变乙醇自我给药。用纳曲酮(3毫克/千克,在连续三次自我给药实验前)重复治疗可逐渐减少乙醇摄入量。在消退程序中,急性给予3毫克/千克纳曲酮可抑制先前由乙醇强化的反应。同样,纳曲酮(1 - 3毫克/千克)能有效且剂量依赖性地抑制由非条件给予装有8%乙醇的液体小勺所产生的乙醇寻求行为的恢复。在对照实验中,较低剂量的纳曲酮(1 - 3毫克/千克)对水的强化或非强化(消退)杠杆按压均无任何影响。这些结果表明:(i)用纳曲酮进行亚慢性治疗会导致乙醇自我给药逐渐减少;(ii)单剂量纳曲酮可能会增加消退并减弱线索诱导的乙醇强化行为的恢复。

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