随机森林
决策树
支持向量机
人工智能
机器学习
特征选择
计算机科学
数量结构-活动关系
化学信息学
试验装置
二元分类
适用范围
虚拟筛选
化学
计算生物学
数据挖掘
药物发现
生物信息学
分子描述符
生物信息学
生物
基因
生物化学
作者
Vasanthanathan Poongavanam,Olivier Taboureau,Chris Oostenbrink,Nico Vermeulen,Lars Olsen,Flemming Steen Jørgensen
标识
DOI:10.1124/dmd.108.023507
摘要
The cytochrome P450 (P450) superfamily plays an important role in the metabolism of drug compounds, and it is therefore highly desirable to have models that can predict whether a compound interacts with a specific isoform of the P450s. In this work, we provide in silico models for classification of CYP1A2 inhibitors and noninhibitors. Training and test sets consisted of approximately 400 and 7000 compounds, respectively. Various machine learning techniques, such as binary quantitative structure activity relationship, support vector machine (SVM), random forest, kappa nearest neighbor (kNN), and decision tree methods were used to develop in silico models, based on Volsurf and Molecular Operating Environment descriptors. The best models were obtained using the SVM, random forest, and kNN methods in combination with the BestFirst variable selection method, resulting in models with 73 to 76% of accuracy on the test set prediction (Matthews correlation coefficients of 0.51 and 0.52). Finally, a decision tree model based on Lipinski9s Rule-of-Five descriptors was also developed. This model predicts 67% of the compounds correctly and gives a simple and interesting insight into the issue of classification. All of the models developed in this work are fast and precise enough to be applicable for virtual screening of CYP1A2 inhibitors or noninhibitors or can be used as simple filters in the drug discovery process.
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