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肾脏疾病与药物代谢:概述

Renal disease and drug metabolism: an overview.

作者信息

Gibson T P

出版信息

Am J Kidney Dis. 1986 Jul;8(1):7-17. doi: 10.1016/s0272-6386(86)80148-2.

Abstract

Renal disease will perturb the disposition of drugs that primarily depend upon renal excretory function for elimination. While changes in drug half-life (T1/2) are often cited as evidence of altered drug disposition, it must be remembered that T1/2 is a dependent variable whose magnitude varies directly with volume of distribution (Vd) and indirectly with total body clearance (ClT). ClT is the one term that succinctly describes drug elimination. ClT is defined as the sum of the renal (ClR) and nonrenal (ClNR), or metabolic, clearances of a drug. Renal failure has been shown to alter the hepatic microsomal mixed-function oxidase system of drug metabolizing enzymes. Therefore, in end-stage renal failure, the potential exists for the modification of the disposition of drugs whose elimination is primarily hepatic. The kidneys themselves contain many of the enzymes important in hepatic drug metabolism. Drugs such as morphine, paracetamol, and p-aminobenzoic acid are metabolized in the kidney and experimental renal disease has been shown to reduce drug metabolism in the diseased kidney compared with the contralateral normal kidney. Renal disease, then, has the potential to alter not only the renal clearance of unchanged drug but also may substantially modify the metabolic transformation of drugs in both the liver and the kidneys. It can no longer be assumed that the pharmacokinetics of drugs that are disposed mainly by metabolism will be unaltered in renal failure.

摘要

肾脏疾病会扰乱主要依赖肾脏排泄功能进行消除的药物的处置。虽然药物半衰期(T1/2)的变化常被引为药物处置改变的证据,但必须记住,T1/2是一个因变量,其大小直接随分布容积(Vd)而变化,间接随总体清除率(ClT)而变化。ClT是一个简洁描述药物消除的术语。ClT被定义为药物肾脏清除率(ClR)与非肾脏清除率(ClNR)(即代谢清除率)之和。肾衰竭已被证明会改变药物代谢酶的肝微粒体混合功能氧化酶系统。因此,在终末期肾衰竭中,对于主要经肝脏消除的药物,其处置存在被改变的可能性。肾脏自身含有许多在肝脏药物代谢中起重要作用的酶。诸如吗啡、对乙酰氨基酚和对氨基苯甲酸等药物在肾脏中代谢,并且与对侧正常肾脏相比,实验性肾脏疾病已被证明会降低患病肾脏中的药物代谢。那么,肾脏疾病不仅有可能改变原形药物的肾脏清除率,还可能显著改变肝脏和肾脏中药物的代谢转化。再也不能假定主要通过代谢进行处置的药物在肾衰竭时其药代动力学不会改变。

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