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β-咔啉作为大鼠中地西泮辨别性刺激效应的拮抗剂。

Beta-carbolines as antagonists of the discriminative stimulus effects of diazepam in rats.

作者信息

Shannon H E, Hagen T J, Guzman F, Cook J A

机构信息

National Institute on Drug Abuse, Division of Research, Addiction Research Center, Lexington, Kentucky.

出版信息

J Pharmacol Exp Ther. 1988 Jul;246(1):275-81.

PMID:3392659
Abstract

Rats were trained to discriminate between saline and 1.0 mg/kg of diazepam in a two-choice procedure where responding was maintained under a fixed-ratio, 5-response schedule of stimulus shock termination. beta-Carboline-3-carboxylate-methyl ester (beta CCM), beta-carboline-3-carboxylate-ethyl ester (beta CCE) and beta-carboline-3-carboxylate-t-butyl ester (beta CCtB), compounds with alkylcarboxy substitutions on the 3-position of the beta-carboline ring structure, were effective antagonists of the discriminative effects of diazepam. The 3-hydroxymethyl-substituted compound (3HMC) was relatively ineffective in antagonizing the discriminative effects of diazepam. The order of potency in antagonizing the 1.0 mg/kg training dose of diazepam was beta CCtB greater than beta CCM greater than beta CCE much greater than 3 HMC. The greater potency of beta CCtB likely reflects its resistance to metabolism in vivo. beta CCE and beta CCtB produced dose-related, parallel shifts in the dose-response curve for the discriminative effects of diazepam, but the magnitude of the shifts was limited: the two highest doses of beta CCE and beta CCtB produced shifts that were not significantly different in magnitude. These latter results suggest that these beta-carbolines antagonize only a portion of the component(s) of action of diazepam in producing discriminative stimuli. In contrast, the 7-substituted beta-carbolines harmane, harmol and harmine were ineffective in antagonizing the discriminative effects of diazepam up to doses of the beta-carbolines which disrupted the ability of the animals to respond.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在一个两选择程序中,训练大鼠在生理盐水和1.0毫克/千克地西泮之间进行辨别,在该程序中,反应在固定比率、5次反应的刺激休克终止时间表下维持。β-咔啉-3-羧酸甲酯(βCCM)、β-咔啉-3-羧酸乙酯(βCCE)和β-咔啉-3-羧酸叔丁酯(βCCtB),这些在β-咔啉环结构的3位上有烷基羧基取代的化合物,是地西泮辨别效应的有效拮抗剂。3-羟甲基取代的化合物(3HMC)在拮抗地西泮的辨别效应方面相对无效。拮抗1.0毫克/千克训练剂量地西泮的效力顺序为βCCtB>βCCM>βCCE>>3HMC。βCCtB的更大效力可能反映了其在体内对代谢的抗性。βCCE和βCCtB在地西泮辨别效应的剂量反应曲线上产生了剂量相关的平行位移,但位移幅度有限:βCCE和βCCtB的两个最高剂量产生的位移在幅度上没有显著差异。这些结果表明,这些β-咔啉仅拮抗地西泮产生辨别刺激作用的一部分成分。相比之下,7-取代的β-咔啉哈尔满、去甲哈尔满和哈尔明在高达破坏动物反应能力的β-咔啉剂量下,对地西泮的辨别效应无效。(摘要截短于250字)

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