反复使用氟哌啶醇和氯氮平治疗增强对苯环利定诱导的过度活动的抑制作用的神经基础。

Neural basis of the potentiated inhibition of repeated haloperidol and clozapine treatment on the phencyclidine-induced hyperlocomotion.

机构信息

Department of Psychology, University of Nebraska-Lincoln, Lincoln, NE 685888, USA.

出版信息

Prog Neuropsychopharmacol Biol Psychiatry. 2012 Aug 7;38(2):175-82. doi: 10.1016/j.pnpbp.2012.03.007. Epub 2012 Mar 26.

DOI:10.1016/j.pnpbp.2012.03.007

PMID:22476004

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3389158/

Abstract

Clinical observations suggest that antipsychotic effect starts early and increases progressively over time. This time course of antipsychotic effect can be captured in a rat phencyclidine (PCP)-induced hyperlocomotion model, as repeated antipsychotic treatment progressively increases its inhibition of the repeated PCP-induced hyperlocomotion. Although the neural basis of acute antipsychotic action has been studied extensively, the system that mediates the potentiated effect of repeated antipsychotic treatment has not been elucidated. In the present study, we investigated the neuroanatomical basis of the potentiated action of haloperidol (HAL) and clozapine (CLZ) treatment in the repeated PCP-induced hyperlocomotion. Once daily for five consecutive days, adult Sprague-Dawley male rats were first injected with HAL (0.05 mg/kg, sc), CLZ (10.0 mg/kg, sc) or saline, followed by an injection of PCP (3.2 mg/kg, sc) or saline 30 min later, and motor activity was measured for 90 min after the PCP injection. C-Fos immunoreactivity was assessed either after the acute (day 1) or repeated (day 5) drug tests. Behaviorally, repeated HAL or CLZ treatment progressively increased the inhibition of PCP-induced hyperlocomotion throughout the five days of drug testing. Neuroanatomically, both acute and repeated treatment of HAL significantly increased PCP-induced c-Fos expression in the nucleus accumbens shell (NAs) and the ventral tegmental area (VTA), but reduced it in the central amygdaloid nucleus (CeA). Acute and repeated CLZ treatment significantly increased PCP-induced c-Fos expression in the ventral part of lateral septal nucleus (LSv) and VTA, but reduced it in the medial prefrontal cortex (mPFC). More importantly, the effects of HAL and CLZ in these brain areas underwent a time-dependent reduction from day 1 to day 5. These findings suggest that repeated HAL achieves its potentiated inhibition of the PCP-induced hyperlocomotion by acting on the NAs, CeA and VTA, while CLZ does so by acting on the mPFC, LSv and VTA.

摘要

临床观察表明，抗精神病药物的疗效在早期开始，并随着时间的推移逐渐增加。这种抗精神病药物的疗效可以在大鼠苯环己哌啶（PCP）诱导的过度活动模型中捕捉到，因为反复的抗精神病治疗逐渐增加了其对重复 PCP 诱导的过度活动的抑制作用。尽管急性抗精神病作用的神经基础已经得到了广泛的研究，但介导反复抗精神病治疗增强作用的系统尚未阐明。在本研究中，我们研究了氟哌啶醇（HAL）和氯氮平（CLZ）治疗在重复 PCP 诱导的过度活动中的增强作用的神经解剖学基础。连续五天，每天一次，成年 Sprague-Dawley 雄性大鼠首先皮下注射 HAL（0.05mg/kg）、CLZ（10.0mg/kg）或生理盐水，30 分钟后再注射 PCP（3.2mg/kg，sc）或生理盐水，然后在 PCP 注射后 90 分钟测量运动活性。在急性（第 1 天）或重复（第 5 天）药物测试后评估 C-Fos 免疫反应性。行为上，重复 HAL 或 CLZ 治疗逐渐增加了整个五天药物测试中对 PCP 诱导的过度活动的抑制作用。神经解剖学上，HAL 的急性和重复治疗均显著增加了 PCP 诱导的伏隔核壳（NAs）和腹侧被盖区（VTA）中的 c-Fos 表达，但减少了杏仁中央核（CeA）中的表达。急性和重复 CLZ 治疗显著增加了侧脑室隔核（LSv）和 VTA 中 PCP 诱导的 c-Fos 表达，但减少了内侧前额叶皮质（mPFC）中的表达。更重要的是，从第 1 天到第 5 天，HAL 和 CLZ 在这些脑区的作用呈时间依赖性减少。这些发现表明，重复 HAL 通过作用于 NAs、CeA 和 VTA 来实现其对 PCP 诱导的过度活动的增强抑制作用，而 CLZ 通过作用于 mPFC、LSv 和 VTA 来实现这一作用。

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