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隔核在大鼠单次吗啡注射诱导的行为敏化发展中起关键介导作用。

Septal nuclei critically mediate the development of behavioral sensitization to a single morphine injection in rats.

机构信息

National Institute on Drug Dependence, Peking University, Beijing 100191, PR China.

出版信息

Brain Res. 2012 May 15;1454:90-9. doi: 10.1016/j.brainres.2012.03.027. Epub 2012 Mar 17.

DOI:10.1016/j.brainres.2012.03.027
PMID:22502977
Abstract

Behavioral sensitization to a single morphine injection is a unique model to study the neuroanatomical substrates of long-lasting behavioral plasticity associated with opioid reward and abuse. Earlier observations have demonstrated that septal nuclei are critically involved in the processes of reward, learning and memory. In the present study, we investigated the effects of septal nuclei lesions on behavioral sensitization to a single morphine injection, morphine induced conditioned place preference and antinociception in rats. Behavioral sensitization was established by a single injection of 3-30 mg/kg morphine in rats. Bilateral electrical lesions of septal nuclei were carried out 7 days before morphine pretreatment. Acute morphine injection induced hyperactivity in the non-surgery control, sham surgery and septal nuclei-lesioned rats. Seven days later, the challenge injection with 3mg/kg morphine induced significant behavioral sensitization in rats with no surgery and sham surgery, but failed to induce behavioral sensitization in septal nuclei-lesioned rats. When the septal nuclei ablation was carried out after acute morphine pretreatment, the expression of behavioral sensitization was unaffected and not different among rats. In addition, septal nuclei lesions did not impact the rewarding and antinociceptive effects of 10 mg/kg morphine when the rats were tested in a conditioned place preference test and tail-flick test, respectively. Collectively, these results suggest that septal nuclei may be selectively involved in the initiation of behavioral sensitization to morphine, which is separable from the effects of morphine for exerting its rewarding and antinociceptive effects.

摘要

单次吗啡注射引起的行为敏化是研究与阿片类药物奖赏和滥用相关的持久行为可塑性的神经解剖学基础的独特模型。早期的观察表明,隔核在奖赏、学习和记忆过程中起着至关重要的作用。在本研究中,我们研究了隔核损伤对单次吗啡注射、吗啡诱导的条件位置偏好和大鼠镇痛作用的行为敏化的影响。通过单次注射 3-30mg/kg 吗啡在大鼠中建立行为敏化。在吗啡预处理前 7 天,对双侧隔核进行电损伤。急性吗啡注射引起非手术对照组、假手术组和隔核损伤组大鼠的过度活跃。7 天后,用 3mg/kg 吗啡进行挑战注射,在没有手术和假手术的大鼠中引起明显的行为敏化,但在隔核损伤的大鼠中不能引起行为敏化。当在急性吗啡预处理后进行隔核消融时,行为敏化的表达在大鼠中不受影响,也没有差异。此外,当大鼠在条件位置偏好测试和尾部闪烁测试中分别接受 10mg/kg 吗啡的奖赏和镇痛作用测试时,隔核损伤对其无影响。总之,这些结果表明,隔核可能选择性地参与吗啡引起的行为敏化的启动,而这与吗啡发挥其奖赏和镇痛作用的效应是分离的。

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