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三杆操作法下咪达唑仑的药物辨别分析。II:苯二氮䓬受体激动剂的差异效应。

Drug discrimination analysis of midazolam under a three-lever procedure. II: Differential effects of benzodiazepine receptor agonists.

作者信息

Sannerud C A, Ator N A

机构信息

Preclinical Pharmacology Laboratory, NIDA Intramural Research Program, Baltimore, Maryland, USA.

出版信息

J Pharmacol Exp Ther. 1995 Oct;275(1):183-93.

PMID:7562548
Abstract

Twelve rats were trained to discriminate 0.32 and 3.2 mg/kg s.c. midazolam from no drug under a three-lever, multiple trials drug discrimination procedure. In cumulative dose-response tests, midazolam s.c. (0.032-10 mg/kg) and i.p. (0.1-10 mg/kg) occasioned dose-dependent increases first in 0.32 mg/kg (low-dose) lever responding and then in 3.2 mg/kg (high-dose) lever responding. The benzodiazepines diazepam (0.032-18 mg/kg) and triazolam (0.0032-3.2 mg/kg) produced patterns of generalization similar to that of midazolam; however, chlordiazepoxide (0.1-32 mg/kg), lorazepam (0.032-10 mg/kg), flurazepam (0.01-10 mg/kg), bretazenil (0.01-32 mg/kg) and the imidazopyridazine zolpidem (0.032-3.2 mg/kg) dose-dependently occasioned > 80% responding on the low- but not the high-dose midazolam lever. Clonazepam (0.1-10 mg/kg) occasioned 0% responding on the high-dose lever, but also failed to occasion full generalization to the low-dose midazolam lever in 40% of the rats. Bretazenil has been well-characterized as a partial benzodiazepine agonist and zolpidem as benzodiazepine-receptor-subtype selective; the present results are consistent with their partial or selective agonist effects in those other paradigms. The differential effects of the classic 1,4 benzodiazepine agonists tested suggest that the discriminative stimulus effects of these other compounds may be more differentiable than previous drug discrimination studies have suggested. This three-choice drug discrimination procedure appears to be a useful model for studying relative intrinsic efficacies of this class of compounds.

摘要

在一个三杠杆、多次试验的药物辨别程序中,训练12只大鼠区分皮下注射0.32和3.2毫克/千克咪达唑仑与无药物状态。在累积剂量-反应测试中,皮下注射咪达唑仑(0.032 - 10毫克/千克)和腹腔注射(0.1 - 10毫克/千克)首先引起0.32毫克/千克(低剂量)杠杆反应的剂量依赖性增加,然后是3.2毫克/千克(高剂量)杠杆反应的增加。苯二氮䓬类药物地西泮(0.032 - 18毫克/千克)和三唑仑(0.0032 - 3.2毫克/千克)产生的泛化模式与咪达唑仑相似;然而,氯氮䓬(0.1 - 32毫克/千克)、劳拉西泮(0.032 - 10毫克/千克)、氟西泮(0.01 - 10毫克/千克)、布瑞氮䓬(0.01 - 32毫克/千克)和咪唑并吡啶类药物唑吡坦(0.032 - 3.2毫克/千克)剂量依赖性地引起在低剂量但不是高剂量咪达唑仑杠杆上>80%的反应。氯硝西泮(0.1 - 10毫克/千克)在高剂量杠杆上引起0%的反应,但在40%的大鼠中也未能完全泛化到低剂量咪达唑仑杠杆。布瑞氮䓬已被充分表征为部分苯二氮䓬激动剂,唑吡坦为苯二氮䓬受体亚型选择性;目前的结果与它们在其他范式中的部分或选择性激动剂作用一致。所测试的经典1,4 - 苯二氮䓬激动剂的差异效应表明,这些其他化合物的辨别性刺激效应可能比以前的药物辨别研究表明的更具可区分性。这种三选择药物辨别程序似乎是研究这类化合物相对内在效能的有用模型。

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