Cytochrome P450 enzymes are responsible for phase I metabolism of the majority of drugs and xenobiotics. Identification of the substrates and inhibitors of these enzymes is important for the analysis of drug metabolism, prediction of drug-drug interactions and drug toxicity, and the design of drugs that modulate cytochrome P450 mediated metabolism. The substrates and inhibitors of these enzymes are structurally diverse. It is thus desirable to explore methods capable of predicting compounds of diverse structures without over-fitting. Support vector machine is an attractive method with these qualities, which has been employed for predicting the substrates and inhibitors of several cytochrome P450 isoenzymes as well as compounds of various other pharmacodynamic, pharmacokinetic, and toxicological properties. This article introduces the methodology, evaluates the performance, and discusses the underlying difficulties and future prospects of the application of support vector machines to in silico prediction of cytochrome P450 substrates and inhibitors.

译文

细胞色素P450酶负责大多数药物和异源生物的I期代谢。鉴定这些酶的底物和抑制剂对于分析药物代谢,预测药物-药物相互作用和药物毒性以及设计调节细胞色素P450介导的代谢的药物非常重要。这些酶的底物和抑制剂在结构上是多种多样的。因此,需要探索能够预测具有不同结构的化合物而不会过度拟合的方法。支持向量机是一种具有这些品质的有吸引力的方法,已用于预测几种细胞色素P450同工酶以及其他各种药效学,药代动力学和毒理学特性的化合物的底物和抑制剂。本文介绍了该方法,评估了性能,并讨论了支持向量机在细胞色素P450底物和抑制剂的计算机预测中的潜在困难和未来前景。

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