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A quantitative structure–activity relationship study of anti-HIV activity of substituted HEPT using nonlinear models

机译:非线性模型对取代HEPT抗HIV活性的定量构效关系研究

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摘要

We performed studies on extended series of 79 HEPT ligands (1-[(2-hydroxyethoxy)methyl]-6-(phenylthio)thymine), inhibitors of HIV reverse-transcriptase with anti-HIV biological activity, using quantitative structure–activity relationship (QSAR) methods that imply analysis of correlations and representation of models. A suitable set of molecular descriptors was calculated, and the genetic algorithm was employed to select those descriptors which resulted in the best-fit models. The kernel partial least square and Levenberg–Marquardt artificial neural network were utilized to construct the nonlinear QSAR models. The proposed methods will be of great significance in this research, and would be expected to apply to other similar research fields.
机译:我们使用定量的结构-活性关系,对扩展的79种HEPT配体(1-[((2-羟基乙氧基)甲基] -6-(苯硫基)胸腺嘧啶)(具有抗HIV生物活性的HIV逆转录酶抑制剂)进行了研究( QSAR)方法暗示对模型的相关性和表示形式进行分析。计算了一组合适的分子描述子,并采用遗传算法选择了那些描述子,从而得到了最佳拟合模型。利用核的偏最小二乘和Levenberg-Marquardt人工神经网络来构建非线性QSAR模型。所提出的方法在这项研究中将具有重要意义,并有望应用于其他类似的研究领域。

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