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Selective flexibility of side-chain residues improves VEGFR-2 docking score using autodock vina

机译:侧链残基的选择性灵活性可使用自动停靠装置提高VEGFR-2对接分数

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摘要

Selective side-chain residue flexibility is an option available on AutoDock Vina docking software. This approach is promising as it attempts to provide a more realistic ligand-protein interaction environment, without an unmanageable increase in computer processing time. However, studies validating this approach are still scarce. VEGFR-2 (vascular endothelial growth factor receptor 2), a known protein target for anti-angiogenic agents, was used in this study. Four residues present in the VEGFR-2 kinase site were selected and made flexible: Lys866, Glu885, Cys917 and Asp1044. The docking scores for all possible combinations of flexible residues were compared to the docking scores using a rigid conformation. The best overall docking scores were obtained using the Glu883 flexible conformation, with pearson and spearman rank correlation values of 0.568 and 0.543, respectively, and a 51% increase in computer processing time. Using different VEGFR-2 X-ray structures a similar trend was observed with Glu885 flexible conformation presenting the best scores. This study demonstrates that careful use of selective side-chain residue flexibility can improve AutoDock Vina docking score accuracy, without a significant increase in computer processing time. This methodology proved to be a valuable tool in drug design when using VEGFR-2 but will also probably be useful if applied to other protein targets.
机译:AutoDock Vina对接软件提供了一个可选的侧链残基灵活性选项。这种方法是有希望的,因为它试图提供更现实的配体-蛋白质相互作用环境,而不会增加计算机处理时间。但是,仍然缺乏验证这种方法的研究。在这项研究中,使用了VEGFR-2(血管内皮生长因子受体2),它是抗血管生成剂的已知蛋白靶标。选择存在于VEGFR-2激酶位点的四个残基并使其柔性:Lys866,Glu885,Cys917和Asp1044。使用刚性构象将柔性残基的所有可能组合的对接分数与对接分数进行比较。使用Glu883柔性构型可获得最佳的总体对接得分,皮尔逊和斯皮尔曼等级相关值分别为0.568和0.543,计算机处理时间增加51%。使用不同的VEGFR-2 X射线结构,观察到相似的趋势,其中Glu885柔性构象表现出最高分。这项研究表明,谨慎使用选择性侧链残基柔性可以提高AutoDock Vina对接得分的准确性,而不会显着增加计算机处理时间。使用VEGFR-2时,该方法被证明是药物设计中的宝贵工具,但如果将其应用于其他蛋白质靶标,也可能会很有用。

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