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西咪替丁对麻醉犬中氯氮䓬二钾处置的影响。

Cimetidine interaction with dipotassium clorazepate disposition in the anesthetized dog.

作者信息

Colin P, Sirois G, Lelorier J

出版信息

Arch Int Pharmacodyn Ther. 1984 Mar;268(1):12-24.

PMID:6145392
Abstract

Cimetidine (CIM) was used as an interacting agent on the disposition in dogs of dipotassium clorazepate ( CZP ) and its main metabolite nordiazepam (ND) in order to study some of the factors contributing to pharmacokinetic interspecies variation of benzodiazepines in dogs and man. A 0.5 mg/kg of body weight intravenous (i.v.) bolus dose of CZP was administered to 12 anesthetized mongrel dogs, 6 of them receiving also, 30 min before, a 1 mg/kg i.v. bolus dose of CIM followed by a constant i.v. infusion (1 mg/kg/hr) of CIM. Plasma ND and CZP concentrations were measured as a function of time with an high-performance liquid chromatography method. Plasma levels of CZP declined mono- and biexponentially in 1 and 5 dogs, respectively, for each group of animals. No statistically significant difference was found between CZP pharmacokinetic parameters when the 2 groups of dogs were compared. However, a 37% decrease in ND beta half-life, t1/2 beta, when CZP was associated with CIM, was found to be statistically significant. The i.v. administration of pure ND in two dogs, has shown that ND declines biexponentially with a t1/2 beta similar to the one estimated after CZP dosing in control animals. The hepatic metabolism of ND was found to be flow-independent and restrictive. The data, along with previously reported CIM interactions, suggest that several factors, which would be species-dependent, must be responsible of CIM effect on other drugs.

摘要

使用西咪替丁(CIM)作为相互作用剂,研究其对氯氮䓬二钾(CZP)及其主要代谢产物去甲西泮(ND)在犬体内处置的影响,以探讨导致苯二氮䓬类药物在犬和人体内药代动力学种间差异的一些因素。给12只麻醉的杂种犬静脉注射0.5mg/kg体重的CZP推注剂量,其中6只犬在30分钟前还接受了1mg/kg体重的CIM静脉推注剂量,随后以1mg/kg/小时的速度持续静脉输注CIM。采用高效液相色谱法测定血浆中ND和CZP浓度随时间的变化。每组动物中,分别有1只和5只犬的血浆CZP水平呈单指数和双指数下降。比较两组犬时,CZP药代动力学参数无统计学显著差异。然而,当CZP与CIM联用时,ND的β半衰期(t1/2β)降低了37%,具有统计学显著性。对两只犬静脉注射纯ND的结果表明,ND呈双指数下降,其t1/2β与对照动物中CZP给药后估计的t1/2β相似。发现ND的肝脏代谢不依赖血流且具有限制性。这些数据以及先前报道的CIM相互作用表明,几个可能因物种而异的因素必定是CIM对其他药物产生影响的原因。

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Arch Int Pharmacodyn Ther. 1984 Mar;268(1):12-24.
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