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大鼠血清、脑脊液和纹状体中氯丙嗪的药代动力学分析。

Pharmacokinetic analysis of chlorpromazine in rat serum, cerebrospinal fluid and striatum.

作者信息

Sato S, Koshiro A

机构信息

Department of Pharmaceutics, Niigata College of Pharmacy, Japan.

出版信息

Biol Pharm Bull. 1995 Apr;18(4):593-9. doi: 10.1248/bpb.18.593.

Abstract

The time courses of the total concentration of chlorpromazine (CPZ) and its S-oxide (CPZSO) in serum after i.v. administration of CPZ are described by a two compartment model and a simple metabolism model, respectively. The time course of the free CPZ concentration in serum is predicted by the correlation between the ratio of CPZSO/CPZ and the free fraction of CPZ in serum which was established in the previous study. The time course of CPZ concentration in cerebrospinal fluid (CSF) is described by a basic physiological model in which the CSF compartment is connected with the serum compartment (free drug) by the apparent diffusion clearance. Equilibrium dialysis of the striatum homogenate was carried out to clarify the CPZ disposition in the striatum. Since the binding curves of CPZ in the striatum on the Langmuir plot and the Scatchard plot were a sigmoidal and an upward curve, the time course of the drug's concentration was analyzed on a simple kinetic model designed in conformity with a blood-flow limited model. The time course was described by a simple kinetic model for up to 8 h after CPZ administration. These pharmacokinetic models for CSF and the striatum will be used to analyze the relationship between the pharmacokinetics and pharmacodynamics of CPZ.

摘要

静脉注射氯丙嗪(CPZ)后,血清中氯丙嗪(CPZ)及其S - 氧化物(CPZSO)的总浓度随时间变化的过程分别用二室模型和简单代谢模型进行描述。血清中游离CPZ浓度随时间变化的过程是通过先前研究中建立的CPZSO/CPZ比值与血清中CPZ游离分数之间的相关性来预测的。脑脊液(CSF)中CPZ浓度随时间变化的过程用一个基本生理模型来描述,在该模型中,脑脊液隔室通过表观扩散清除率与血清隔室(游离药物)相连。进行纹状体匀浆的平衡透析以阐明CPZ在纹状体中的处置情况。由于CPZ在纹状体中的结合曲线在Langmuir图和Scatchard图上分别为S形曲线和上升曲线,因此根据符合血流限制模型设计的简单动力学模型对药物浓度随时间变化的过程进行分析。在CPZ给药后长达8小时内,该过程用简单动力学模型进行描述。这些用于脑脊液和纹状体的药代动力学模型将用于分析CPZ药代动力学和药效学之间的关系。

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