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营养不良儿童的药物代谢与药代动力学

Drug metabolism and pharmacokinetics in malnourished children.

作者信息

Krishnaswamy K

机构信息

Food & Drug Toxicology, Research Centre, National Institute of Nutrition, Hyderabad, India.

出版信息

Clin Pharmacokinet. 1989;17 Suppl 1:68-88. doi: 10.2165/00003088-198900171-00006.

Abstract

Malnutrition is a complex condition in which many deficiencies occur simultaneously. Protein-energy malnutrition is a major public health and clinical problem in paediatric practice that accounts for high child mortality and morbidity. It includes many different clinical syndromes with protean manifestations. The malnourished often have several concomitant diseases; drugs are therefore as widely used as in the well-nourished. The pathophysiological profile in malnutrition can alter pharmacokinetic processes, drug responses and toxicity. This review summarizes the available knowledge on nutrient-drug interactions in malnourished children. Although there is much evidence in the literature that diet and nutritional status are 2 important environmental variables determining the pharmacotoxicological properties of chemicals, there are few data on humans. Recently, intense effort has been initially directed at studying drug kinetics in grade III malnutrition, namely kwashiorkor and marasmus. Studies on drugs and nutrients indicate delayed or decreased absorption, reduced protein binding of several drugs, fluctuations in volume of distribution, altered hepatic oxidative drug biotransformations and conjugations, reduced elimination of conjugates and reduced elimination of renally excreted drugs. The estimated steady-state levels of a few drugs suggest accumulation. Bioavailability problems with certain drugs are due to divergent effects of pharmacokinetic processes. Clinical risk of toxicity appears to be higher in malnourished children. Rehabilitation studies suggest that a number of these pharmacological abnormalities can be reversed. The majority of studies have concentrated on single-dose pharmacokinetics in severely malnourished children. A number of abnormalities seen in drug disposition during the acute phase of malnutrition need to be confirmed for other grades of malnutrition. For practical purposes, it is important to consider steady-state levels and data in mild and moderate forms of growth-retarded children; drug-induced nutritional deficiencies can occur more easily in these populations. Although some of the drugs described in this review have been in use for many years, knowledge on drug response and toxicity is still only approximate. There is at present enough evidence to support monitoring plasma drug concentrations in malnourished children, particularly for those drugs which have dose-dependent kinetics and narrow margins of safety. The metabolism and disposition of xenobiotics seem to vary widely in children with protein-energy malnutrition. Therapeutic inadequacies and toxicities need careful evaluation in malnourished children.

摘要

营养不良是一种复杂的状况,其中多种营养素缺乏会同时出现。蛋白质 - 能量营养不良是儿科实践中的一个主要公共卫生和临床问题,导致儿童高死亡率和高发病率。它包括许多具有多样表现的不同临床综合征。营养不良的儿童常常伴有多种疾病;因此,药物的使用与营养良好的儿童一样广泛。营养不良中的病理生理特征可改变药代动力学过程、药物反应及毒性。本综述总结了关于营养不良儿童中营养 - 药物相互作用的现有知识。尽管文献中有很多证据表明饮食和营养状况是决定化学物质药物毒理学特性的两个重要环境变量,但关于人类的数据却很少。最近,人们最初投入大量精力研究重度营养不良(即夸希奥科病和消瘦症)中的药物动力学。对药物和营养素的研究表明,吸收延迟或减少、几种药物的蛋白质结合减少、分布容积波动、肝脏氧化药物生物转化和结合改变、结合物消除减少以及经肾脏排泄药物的消除减少。少数药物的估计稳态水平表明有蓄积现象。某些药物的生物利用度问题是由于药代动力学过程的不同影响所致。营养不良儿童的临床中毒风险似乎更高。康复研究表明,许多这些药理学异常情况是可以逆转的。大多数研究集中在重度营养不良儿童的单剂量药代动力学上。营养不良急性期药物处置中出现的许多异常情况需要在其他程度的营养不良中得到证实。出于实际目的,考虑轻度和中度生长发育迟缓儿童的稳态水平和数据很重要;药物引起的营养缺乏在这些人群中更容易发生。尽管本综述中描述的一些药物已经使用多年,但关于药物反应和毒性的知识仍然只是大致的。目前有足够的证据支持监测营养不良儿童的血浆药物浓度,特别是对于那些具有剂量依赖性动力学和安全范围狭窄的药物。蛋白质 - 能量营养不良儿童中外源物质的代谢和处置似乎差异很大。在营养不良儿童中,治疗不足和毒性需要仔细评估。

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