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QEX: target-specific druglikeness filter enhances ligand-based virtual screening

机译:QEX:靶标特异性药物相似性过滤器增强了基于配体的虚拟筛选

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摘要

Druglikeness is a useful concept for screening drug candidate compounds. We developed QEX, which is a new druglikeness index specific to individual targets. QEX is an improvement of the quantitative estimate of druglikeness (QED) method, which is a popular quantitative evaluation method of druglikeness proposed by Bickerton et al. QEX models the physicochemical properties of compounds that act on each target protein based on the concept of QED modeling physicochemical properties from information on US Food and Drug Administration-approved drugs. The result of the evaluation of PubChem assay data revealed that QEX showed better performance than the original QED did (the area under the curve value of the receiver operating characteristic curve improved by 0.069-0.236). We also present the c-Src inhibitor filtering results of the QEX constructed using Src family kinase inhibitors as a case study. QEX distinguished the inhibitors and non-inhibitors better than QED did. QEX works efficiently even when datasets of inactive compounds are unavailable. If both active and inactive compounds are present, QEX can be used as an initial filter to enhance the screening ability of conventional ligand-based virtual screenings.Electronic supplementary materialThe online version of this article (10.1007/s11030-018-9842-3) contains supplementary material, which is available to authorized users.
机译:药物相似性是筛选候选药物的有用概念。我们开发了QEX,这是一种针对个体目标的新药物相似性指数。 QEX是对药物相似性定量估计(QED)方法的改进,它是Bickerton等人提出的一种流行的药物相似性定量评价方法。 QEX基于QED的概念对可作用于每种靶蛋白的化合物的物理化学特性进行建模,该概念来自美国食品药品监督管理局批准的药物的物理化学特性建模。 PubChem分析数据的评估结果表明,QEX的性能比原始QED更好(接收器工作特性曲线的曲线值下方的面积提高了0.069-0.236)。我们还介绍了使用Src家族激酶抑制剂构建的QEX的c-Src抑制剂过滤结果作为案例研究。 QEX比QED更好地区分了抑制剂和非抑制剂。即使没有不活泼化合物的数据集,QEX也可以有效地工作。如果同时存在活性和非活性化合物,则QEX可用作初始过滤器以增强常规基于配体的虚拟筛选的筛选能力。电子补充材料本文的在线版本(10.1007 / s11030-018-9842-3)包含补充材料,授权用户可以使用。

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