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细胞色素P450发育方面的综述。

A review of developmental aspects of cytochrome P450.

作者信息

Oesterheld J R

机构信息

Division of Child and Adolescent Psychiatry, University of South Dakota School of Medicine, Sioux Falls, USA.

出版信息

J Child Adolesc Psychopharmacol. 1998;8(3):161-74. doi: 10.1089/cap.1998.8.161.

DOI:10.1089/cap.1998.8.161
PMID:9853690
Abstract

This article surveys the development of human hepatic P450 cytochromes (CYPs) involved in xenobiotic metabolism from the fetus through the life span and explores possible clinical consequences of developmental issues. These hepatic P450 CYPs come "on line" at different times during fetal and infant development, and each one is discussed in that temporal sequence. CYP3A7. the major fetal hepatic cytochrome, is present during organogenesis, and it is involved in steroid metabolism. Variably expressed in some fetuses, CYP3A5 is also present at significant levels in about half of all children. In adults, CYP3A4 is the major functional member of the CYP3A subfamily. CYP1A1 is also present during organogenesis, and it metabolizes exogenous toxins, some of which are procarcinogens. CYP2E1 may be present in some second-trimester fetuses, and it may be involved in prenatal alcohol metabolism. After birth, hepatic CYP2D6 and CYP2C8/9 and CYP2C18/19 become active. Both CYP2D6 and CYP2C19 have genetic polymorphisms that can bring about differing capacities to metabolize exogenous drugs, including psychotropic drugs. CYP1A2 becomes active in the fourth to fifth postfetal months. It provides the best current examples of the importance of developmental changes in xenobiotic-metabolizing P450 CYPs through its metabolism of caffeine and theophylline in premature infants, neonates, and adolescents.

摘要

本文综述了从胎儿期到整个生命过程中参与异源物质代谢的人类肝脏细胞色素P450(CYPs)的发育情况,并探讨了发育问题可能产生的临床后果。这些肝脏P450 CYPs在胎儿和婴儿发育的不同时期“上线”,并按照时间顺序对每一种进行了讨论。CYP3A7是主要的胎儿肝脏细胞色素,在器官发生期存在,参与类固醇代谢。CYP3A5在一些胎儿中表达可变,在约一半的儿童中也有显著水平。在成年人中,CYP3A4是CYP3A亚家族的主要功能成员。CYP1A1在器官发生期也存在,它代谢外源性毒素,其中一些是前致癌物。CYP2E1可能存在于一些孕中期胎儿中,可能参与产前酒精代谢。出生后,肝脏CYP2D6、CYP2C8/9和CYP2C18/19开始活跃。CYP2D6和CYP2C幺九都有基因多态性,可导致对外源性药物(包括精神药物)代谢能力的差异。CYP1A2在出生后第四至第五个月开始活跃。通过其对早产儿、新生儿和青少年咖啡因和茶碱的代谢,它为异源物质代谢P450 CYPs发育变化的重要性提供了当前最好的例子。

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