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苯环利定急性和慢性给药对A10多巴胺能中脑边缘系统的影响:电生理和行为相关性

Effects of acute and chronic administration of phencyclidine on the A10 dopaminergic mesolimbic system: electrophysiological and behavioral correlates.

作者信息

French E D

机构信息

Maryland Psychiatric Research Center, University of Maryland, Baltimore 21228.

出版信息

Neuropharmacology. 1988 Aug;27(8):791-8. doi: 10.1016/0028-3908(88)90093-7.

DOI:10.1016/0028-3908(88)90093-7
PMID:3216958
Abstract

Electrophysiological and behavioral methods were used to evaluate the effects of chronic exposure to phencyclidine (PCP, 5 mg/kg/day for 30 days) on ventral tegmental A10 dopaminergic neurons and locomotor and ataxic behavior in the rat. Extracellular recordings from single neurons in the ventral tegmentum showed only minimal differences between rats chronically treated with either saline or PCP. A comparison of the rising portion of the cumulative dose-response curves indicated that the animals treated chronically with the drug required only 0.4 times more PCP than the controls to produce equivalent changes in neuronal firing rates. Also, the average maximum increase in activity in A10 neurons, induced by PCP, was 43% in the drug-treated rats compared to 60% in the controls. Although these were moderate quantitative changes, a marked qualitative difference in the response of A10 neurons to PCP was seen. Whereas PCP elicited a characteristic dose-dependent biphasic effect on the firing rates in the control group, the declining (inhibitory) component of the response was not present in the animals chronically treated with PCP. In parallel with the minimal electrophysiological changes, measurements of gross locomotor activity showed that the response to the thirtieth (30th) injection of PCP was virtually identical to that measured in the same animals following the first exposure. In contrast, however, the ataxia which accompanied the hyperactivity rapidly diminished over the course of treatment. It would appear, therefore, that chronic exposure to PCP did not substantially diminish the ability of PCP to activate the A10 neurons, comprising the mesocorticolimbic dopaminergic systems.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

采用电生理学和行为学方法,评估大鼠长期暴露于苯环己哌啶(PCP,5毫克/千克/天,持续30天)对腹侧被盖区A10多巴胺能神经元以及运动和共济失调行为的影响。腹侧被盖区单个神经元的细胞外记录显示,长期用生理盐水或PCP处理的大鼠之间仅有极小差异。累积剂量-反应曲线上升部分的比较表明,长期用该药物处理的动物产生与对照组神经元放电率等效变化所需的PCP仅为对照组的0.4倍。此外,PCP诱导的A10神经元活动平均最大增加量,药物处理组大鼠为43%,而对照组为60%。尽管这些是适度的定量变化,但A10神经元对PCP的反应存在明显的定性差异。在对照组中,PCP对放电率产生典型的剂量依赖性双相效应,而在长期用PCP处理的动物中,反应的下降(抑制)成分不存在。与极小的电生理变化并行的是,总体运动活动测量表明,对第30次注射PCP的反应与首次暴露后在同一动物中测量的反应几乎相同。然而,相比之下,伴随多动出现的共济失调在治疗过程中迅速减轻。因此,长期暴露于PCP似乎并未显著削弱PCP激活构成中脑皮质边缘多巴胺能系统的A10神经元的能力。(摘要截断于250字)

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