Quantitative Structure-Activity Relationships and Molecular Docking Studies of P56 LCK Inhibitors

Kavitha Bharatham; Keun Woo Lee; Nagakumar Bharatham

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Quantitative Structure-Activity Relationships and Molecular Docking Studies of P56 LCK Inhibitors

机译：P56 LCK抑制剂的定量构效关系和分子对接研究

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Three-dimensional quantitative structure-activity relationship (3D-QSAR) models were developed for 67 molecules of 2-amino-benzothiazole-6-anilide derivatives against lymphocyte-specific protein tyrosine kinase (P56 LCK). The molecular field analysis (MFA) and receptor surface analysis (RSA) were employed for QSAR studies and the predictive ability of the model was validated by 15 test set molecules. Structure-based investigations using molecular docking simulation were performed with the crystal structure of P56 LCK. Good correlation between predicted fitness scores versus observed activities was demonstrated. The results suggested that the nature of substitutions at the 2-amino and 6-anilide positions were crucial in enhancing the activity, thereby providing new guidelines for the design of novel P56 LCK inhibitors.

机译：建立了针对67个分子的2-氨基-苯并噻唑-6-苯胺衍生物针对淋巴细胞特异性蛋白酪氨酸激酶（P56 LCK）的三维定量构效关系（3D-QSAR）模型。使用分子场分析（MFA）和受体表面分析（RSA）进行QSAR研究，并通过15个测试集分子验证了该模型的预测能力。使用分子对接模拟对P56 LCK的晶体结构进行基于结构的研究。证明了预测的健身评分与观察到的活动之间的良好相关性。结果表明2-氨基和6-苯胺位置上的取代性质对于增强活性至关重要，从而为新型P56 LCK抑制剂的设计提供了新的指导原则。

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《Bulletin of the Korean Chemical Society 》 |2006年第2期| 共页
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Kavitha Bharatham; Keun Woo Lee; Nagakumar Bharatham;
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机译：P56 LCK抑制剂的定量构效关系和分子对接研究
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Quantitative Structure-Activity Relationships and Molecular Docking Studies of P56 LCK Inhibitors

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