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Large-scale structure-activity relationship study of hepatitis C virus NS5B polymerase inhibition using SMILES-based descriptors

机译:基于SMILES的描述符对丙型肝炎病毒NS5B聚合酶抑制的大规模构效关系研究

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摘要

Hepatitis C virus (HCV) is composed of structural and non-structural proteins involved in viral transcription and propagation. In particular, NS5B is an RNA-dependent RNA polymerase for viral transcription and genome replication and is a target for designing anti-viral agents. In this study, classification and quantitative structure-activity relationship (QSAR) models of HCV NS5B inhibitors were constructed using the Correlation and Logic software. Molecular descriptors for a set of 970 HCV NS5B inhibitors were encoded using the simplified molecular input line entry system notation, and predictive models were built via the Monte Carlo method. The QSAR models provided acceptable correlation coefficients of and in the ranges of 0.6038-0.7344 and 0.6171-0.7294, respectively, while the classification models displayed sensitivity, specificity, and accuracy in ranges of 88.24-98.84, 83.87-93.94, and 86.50-94.41 %, respectively. Furthermore, molecular fragments as substructures involved in increased and decreased inhibitory activities were explored. The results provide information on QSAR and classification models for high-throughput screening and mechanistic insights into the inhibitory activity of HCV NS5B polymerase.
机译:丙型肝炎病毒(HCV)由参与病毒转录和繁殖的结构蛋白和非结构蛋白组成。特别地,NS5B是用于病毒转录和基因组复制的RNA依赖性RNA聚合酶,并且是设计抗病毒剂的目标。在这项研究中,使用Correlation and Logic软件构建了HCV NS5B抑制剂的分类和定量构效关系(QSAR)模型。使用简化的分子输入线输入系统符号编码一组970 HCV NS5B抑制剂的分子描述符,并通过蒙特卡洛方法建立预测模型。 QSAR模型提供的可接受相关系数分别在0.6038-0.7344和0.6171-0.7294范围内,而分类模型在88.24-98.84、83.87-93.94和86.50-94.41%的范围内显示出灵敏度,特异性和准确性。 , 分别。此外,探索了作为增加和减少抑制活性的亚结构的分子片段。结果为高通量筛选提供了有关QSAR和分类模型的信息,并提供了对HCV NS5B聚合酶抑制活性的机理了解。

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