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Considering Rotatability of Hydroxyl Groups for the Active Site Residues of MMP-13 in Retrospective Virtual Screening Campaigns

机译:在回顾性虚拟筛选活动中考虑MMP-13活性位点残基的羟基旋转性

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Considering different orientation of hydroxyl and thiol groups of receptor residues such as Thr, Tyr, Ser and Cys is an option available on Glide docking software. This is an attempt that can provide more realistic ligand-receptor interactions. Matrix metalloproteinase 13 (MMP-13) is a suggested target for several diseases including osteoarthritis and cancer. MMP-13 was selected as a receptor with reported flexibility in the active site residues. Four residues in the MMP-13 active site were selected and their hydroxyl groups were made flexible during docking: Tyr241, Thr242, Tyr243 and Thr244. The ability of retrospective virtual screenings using a rigid receptor for discriminating between actives and decoys were compared to those using receptor with different combination of flexible residues. Statistical analysis of the results and inspecting the binding pose of the ligands suggested that the hydroxyl orientation of Tyr241, Thr242, Tyr243 and Thr244 (in particular Thr242 and to a lesser extent Thr244) had impacts on the MMP-13 docking results.
机译:考虑到受体残基(例如Thr,Tyr,Ser和Cys)的羟基和硫醇基的不同取向,是Glide对接软件上的一个选项。这是可以提供更现实的配体-受体相互作用的尝试。基质金属蛋白酶13(MMP-13)是包括骨关节炎和癌症在内的几种疾病的建议靶标。选择MMP-13作为受体,在活性位点残基中具有灵活性。选择了MMP-13活性位点中的四个残基,使它们的羟基在对接过程中变为柔性的:Tyr241,Thr242,Tyr243和Thr244。将使用刚性受体区分活性物质和诱饵的回顾性虚拟筛选能力与使用具有柔性残基不同组合的受体进行回顾性虚拟筛选的能力进行了比较。结果的统计分析和检查配体的结合姿势表明,Tyr241,Thr242,Tyr243和Thr244(特别是Thr242,在较小程度上是Thr244)的羟基取向对MMP-13对接结果有影响。

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