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首页> 外文期刊>Biological psychiatry >D-cycloserine facilitates extinction of naloxone-induced conditioned place aversion in morphine-dependent rats.
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D-cycloserine facilitates extinction of naloxone-induced conditioned place aversion in morphine-dependent rats.

机译:D-环丝氨酸在吗啡依赖性大鼠中促进了纳洛酮诱导的条件性位置厌恶的灭绝。

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BACKGROUND: Cues paired with drug administration trigger relapse to drug seeking by inducing conditioned drug craving and withdrawal. Because drug cues hinder abstinence in addicts, therapies that reduce responsiveness to drug cues might facilitate rehabilitation. Extinction is a means of reducing conditioned responses and involves exposure to the conditioned stimulus in the absence of the unconditioned stimulus with which it was paired previously. We examined conditioned withdrawal extinction using naloxone-induced conditioned place aversion (CPA) in morphine-dependent rats. METHODS: Morphine-dependent rats were trained to associate an environment with naloxone-precipitated withdrawal. Subsequently, they received extinction training in which they were confined in the previously naloxone-paired environment in the absence of acute withdrawal. In some rats, the N-methyl-D-aspartate (NMDA) receptor partial agonist D-cycloserine (DCS) was administered before extinction training. RESULTS: Morphine withdrawal-induced CPA persists in the absence of extinction training. Administration of DCS before extinction training facilitates extinction. CONCLUSIONS: D-cycloserine facilitates extinction of morphine withdrawal-associated place aversion. This effect is qualitatively similar to the effect of DCS on extinction of conditioned fear, raising the possibility of common neural mechanisms. This work extends our understanding of drug cue responsivity and provides a rationale for the development of extinction-based treatments for addiction.
机译:背景:与药物管理相结合的线索通过诱导条件性药物渴望和停药来触发寻药的复发。由于药物提示会阻碍成瘾者戒酒,因此降低对药物提示的反应性的疗法可能会促进康复。消光是减少条件反应的一种手段,包括在没有先前配对的条件刺激的情况下暴露于条件刺激。我们在吗啡依赖性大鼠中使用纳洛酮诱导的条件性场所厌恶(CPA)检查了条件性戒断绝种。方法:对吗啡依赖的大鼠进行了训练,使其与纳洛酮沉淀的戒断环境相关联。随后,他们接受了灭绝训练,在这种训练中,他们被限制在先前的纳洛酮配对环境中,没有急性戒断。在一些大鼠中,在灭绝训练之前先给予N-甲基-D-天冬氨酸(NMDA)受体部分激动剂D-环丝氨酸(DCS)。结果:在没有消光训练的情况下,吗啡戒断引起的CPA持续存在。在灭绝训练之前施用DCS有助于灭绝。结论:D-环丝氨酸促进了吗啡戒断相关的地方厌恶的消失。这种作用在质量上类似于DCS对条件性恐惧的消退,从而增加了常见神经机制的可能性。这项工作扩展了我们对药物提示反应性的理解,并为开发基于灭绝的成瘾疗法提供了理论依据。

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