首页> 美国卫生研究院文献>The Journal of Neuroscience >Relapse to heroin-seeking in rats under opioid maintenance: the effects of stress heroin priming and withdrawal
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Relapse to heroin-seeking in rats under opioid maintenance: the effects of stress heroin priming and withdrawal

机译:阿片维持下大鼠海洛因复发:压力海洛因启动和戒断的影响

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摘要

It is widely believed that opioid withdrawal symptoms contribute to relapse to opioid use, but relapse is highly probable in experienced users even after prolonged abstinence and during opioid maintenance therapy. We have found using an animal model of relapse, the reinstatement procedure, that the two events that reliably reinstate heroin-seeking behavior are reexposure to heroin, and brief exposure to footshock stress. Contrary to expectation, opioid antagonist-induced withdrawal does not reinstate heroin-seeking. We now report on reinstatement of heroin-seeking in rats trained to self-administer heroin and subsequently exposed to a maintenance dose of heroin via minipump and allowed to self-administer saline. With the minipump in, naloxone-induced withdrawal did not reinstate drug-seeking, a priming injection on heroin was only mildly effective, and footshock was highly effective. Twenty-four hours after removal of the minipump (spontaneous withdrawal), animals reinitiated heroin-seeking and, subsequently, both heroin and footshock reinstated heroin-seeking. In summary, brief exposure to stress reinstated heroin-seeking in both heroin-maintained and withdrawn animals. The heroin prime reliably reinstated drug- seeking only in the absence of the minipump; opioid “withdrawal,” as such, did not reinstate drug-seeking behavior. Naloxone given to heroin- maintained animals induced withdrawal symptoms, caused a mild depression in the levels of dopamine and its metabolites in the nucleus accumbens septi (NAS), but did not reinstate drug-seeking. Reinstatement of heroin-seeking during spontaneous withdrawal was not accompanied by reductions in basal dopamine and its metabolites in NAS.
机译:人们普遍认为,阿片类药物戒断症状会导致使用阿片类药物复发,但是即使在长期禁欲和维持阿片类药物治疗期间,经验丰富的使用者也很可能复发。我们发现,使用复发的动物模型即恢复程序,可以可靠地恢复海洛因寻求行为的两个事件是再次暴露于海洛因,以及短暂暴露于休克压力。与预期相反,阿片类药物拮抗剂引起的戒断并没有恢复海洛因的寻求。现在,我们报道了在训练自律服用海洛因并随后通过微型泵暴露于维持剂量的海洛因的老鼠中恢复海洛因寻找的情况,并允许其自我给予盐水。微型泵进入后,纳洛酮引起的戒断并没有恢复吸毒,海洛因的初次注射仅适度有效,而休克疗法则非常有效。移除微型泵(自发退出)后二十四小时,动物重新开始寻求海洛因,随后海洛因和休克都恢复了对海洛因的寻找。总而言之,短暂暴露于压力会使海洛因维持和戒断动物的海洛因寻求恢复。只有在没有微型泵的情况下,海洛因素才能可靠地恢复寻药。因此,阿片类药物“戒断”并没有恢复吸毒行为。给维持海洛因的动物服用纳洛酮会引起戒断症状,​​使伏隔核(NAS)中的多巴胺及其代谢物水平轻度降低,但并未恢复寻求药物的状态。自发戒断期间恢复海洛因的行为并未伴有基础多巴胺及其在NAS中的代谢产物减少。

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