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首页> 外文期刊>International Journal of Pharmaceutics >Developmental expression of drug metabolizing enzymes: impact on disposition in neonates and young children.
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Developmental expression of drug metabolizing enzymes: impact on disposition in neonates and young children.

机译:药物代谢酶的发育性表达:对新生儿和幼儿处置的影响。

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Profound changes in drug metabolizing enzyme expression occurs during development that impacts drug efficacy and the risk of adverse events in the neonate and young child. A review of our current knowledge suggests individual hepatic drug metabolizing enzymes can be categorized into one of three classes based on developmental trajectories. The time frame for the perinatal changes observed for both Class 1 and Class 3 enzymes varies considerably between different enzymes. However, for a given enzyme, significant interindividual variation is observed in the timing of the perinatal changes, creating windows of hypervariability. Genetic variation clearly impacts drug disposition in children. However, developmental factors can dominate pharmacogenetic factors. Thus, a major challenge in applying pharmacogenomics to improve pediatric drug safety is determining at what age functional genetic variants identified in adults become a major determinant of expression in children. Developmental and genetic data on drug metabolizing enzyme ontogeny, as well as age-dependent changes in other physiological factors impacting drug disposition, can be integrated into physiologically-based pharmacokinetic models. Such models have proven useful in predicting the range of expected metabolic capacities at a given age.
机译:药物代谢酶表达发生深刻变化,在发育过程中会影响药物的有效性以及新生儿和幼儿发生不良事件的风险。对我们当前知识的回顾表明,根据发展轨迹,可以将单个肝药物代谢酶分为三类之一。对于1类和3类酶而言,围产期变化的时间框架在不同酶之间差异很大。但是,对于给定的酶,在围产期变化的时间中观察到显着的个体间差异,从而形成了高变异性窗口。遗传变异显然会影响儿童的药物处置。但是,发育因素可以主导药理遗传因素。因此,应用药物基因组学来改善儿科药物安全性的主要挑战是确定在几岁时在成人中鉴定的功能性遗传变异成为儿童表达的主要决定因素。关于药物代谢酶个体发育的发育和遗传数据,以及影响药物处置的其他生理因素的年龄依赖性变化,都可以整合到基于生理的药代动力学模型中。事实证明,此类模型可用于预测给定年龄下预期的代谢能力范围。

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