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发育相关药物性肝损伤在新生儿和儿童中的研究进展。

A developmental approach to drug-induced liver injury in newborns and children.

机构信息

Istituto di Anatomia Patologica, Ospedale San Giovanni di Dio, Via Ospedale n. 60, 09124 Cagliari, Sardinia, Italy.

出版信息

Curr Med Chem. 2012;19(27):4581-94. doi: 10.2174/092986712803306385.

Abstract

The liver represents the major site of drug metabolism in humans. The developmental changes that occur in the liver's metabolic activity during fetal life and in the perinatal period are at the basis of the varied sensitivity of human newborns to many drugs. The decreased capacity of the fetal and newborn liver to metabolize, detoxify, and excrete drugs--total cytochrome P450 content in the fetal liver being 30% to 60% of adult values--may explain the prolonged actions of many drugs in the newborn, as well as less their potential toxicity. On the other hand, the low levels of phase I (activation) enzymes, producing more polar reactive and often toxic metabolites, could explain the lower incidence of adverse effects of some drugs reported in newborns. Moreover, the greater capacity of newborns to synthesize glutathione is at the basis of their ability in inactivating many toxic metabolites. Here we review the acute and chronic liver toxicity due to the most widely used drugs in the neonate. We will discuss in detail the biochemical profile of the fetal and neonatal liver, and the toxic metabolites formed during the metabolism of the most widely used drugs in the neonate. The histological picture of liver disease related to the therapeutic use of drugs will be discussed, with particular emphasis on the mode of cell death involved in hepatitis induced by different drugs most frequently utilized in the neonatal intensive care units.

摘要

肝脏是人体药物代谢的主要部位。胎儿期和围产期肝脏代谢活性的发育变化是人类新生儿对许多药物敏感性不同的基础。胎儿和新生儿肝脏代谢、解毒和排泄药物的能力下降——胎儿肝脏中的总细胞色素 P450 含量为成人的 30%至 60%——这可能解释了许多药物在新生儿中的作用时间延长,而潜在毒性较小。另一方面,I 期(激活)酶水平较低,产生更多极性反应性且往往有毒的代谢物,这可以解释新生儿报告的某些药物不良反应发生率较低的原因。此外,新生儿合成谷胱甘肽的能力更强,这是其能够使许多有毒代谢物失活的基础。在这里,我们回顾了由于新生儿中最广泛使用的药物而导致的急性和慢性肝毒性。我们将详细讨论胎儿和新生儿肝脏的生化特征,以及新生儿中最广泛使用的药物代谢过程中形成的有毒代谢物。我们将讨论与药物治疗相关的肝病的组织学图片,特别强调新生儿重症监护病房中最常使用的不同药物引起的肝炎所涉及的细胞死亡方式。

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