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人体肝脏药物氧化能力的体内年龄相关性变化。

In vivo age-related changes in hepatic drug-oxidizing capacity in humans.

作者信息

Tanaka E

机构信息

Institute of Community Medicine, University of Tsukuba, Ibaraki-ken, Japan.

出版信息

J Clin Pharm Ther. 1998 Aug;23(4):247-55. doi: 10.1046/j.1365-2710.1998.00164.x.

DOI:10.1046/j.1365-2710.1998.00164.x
PMID:9867310
Abstract

Very few studies have been carried out looking at how the effects of drugs and their toxicity in humans change during their lifespan (developing and ageing). The purpose of this study is to review the literature on the changes in probe-drug metabolism, classified by cytochrome P450 (P450 or CYP) at five stages in life: neonates < 4 weeks, infants < 12 months, children < 19 years, young/mature adults 20-64 years, and elderly adults > 65 years. The main probe drugs include caffeine and theophylline, whose metabolism is catalysed by CYP1A2, tolbutamide, phenytoin and ibuprofen, catalysed by CYP2C9, amitriptyline and nortriptyline, catalysed by CYP2C19, acetaminophen, catalysed by CYP2E1 and lidocaine, midazolam and terfenadine, catalysed by 3A3/4. From the published in vivo studies two different patterns of drug metabolism can be identified: (i) activity is low immediately after birth, increases, then peaks at the young/mature adult level and, finally, decreases in old age (drugs catalysed by CYP1A2, CYP2C9, CYP2C19, CYP2D6 and CYP3A3/4) and (ii) activity increases rapidly after birth to reach a level equivalent to that in the young/mature adult, then gradually decreases and finally decreasing faster in old age (drugs catalysed by CYP2E1). Further study of the changes in P450 with age is warranted to help prevent adverse reactions and to guide us in tailoring therapy better for the individual patient.

摘要

很少有研究关注药物效应及其在人体中的毒性在整个生命周期(发育和衰老阶段)是如何变化的。本研究的目的是回顾关于在生命五个阶段按细胞色素P450(P450或CYP)分类的探针药物代谢变化的文献,这五个阶段分别为:小于4周的新生儿、小于12个月的婴儿、小于19岁的儿童、20 - 64岁的青年/成熟成年人以及大于65岁的老年人。主要的探针药物包括咖啡因和茶碱,其代谢由CYP1A2催化;甲苯磺丁脲、苯妥英和布洛芬,由CYP2C9催化;阿米替林和去甲替林,由CYP2C19催化;对乙酰氨基酚,由CYP2E1催化;利多卡因、咪达唑仑和特非那定,由3A3/4催化。从已发表的体内研究中可以识别出两种不同的药物代谢模式:(i)出生后立即活性较低,随后增加,然后在青年/成熟成年人水平达到峰值,最后在老年时降低(由CYP1A2、CYP2C9、CYP?、CYP2D6和CYP3A3/4催化的药物),以及(ii)出生后活性迅速增加,达到与青年/成熟成年人相当的水平,然后逐渐降低,最终在老年时下降更快(由CYP2E1催化的药物)。有必要进一步研究P450随年龄的变化,以帮助预防不良反应,并指导我们为个体患者更好地量身定制治疗方案。 (注:原文中“CYP2C19”后的“?”疑似有误,未影响整体翻译理解,故保留。)

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