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首页> 外文期刊>Journal of molecular graphics & modelling >Prediction of dual agents as an activator of mutant p53 and inhibitor of Hsp90 by docking, molecular dynamic simulation and virtual screening
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Prediction of dual agents as an activator of mutant p53 and inhibitor of Hsp90 by docking, molecular dynamic simulation and virtual screening

机译:通过对接,分子动力学模拟和虚拟筛选预测作为突变体p53激活剂和Hsp90抑制剂的双重试剂

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Heat shock protein90s (Hsp90s) play a crucial role in the development of cancer, and their inhibitors are a main target for tumor suppression. P53 also is a tumor suppressor, but in cancer cells, mutations in the p53 gene lead to the inactivation and accumulation of protein. For instance, the ninth p53 cancer mutation, Y220C, destabilizes the p53 core domain. Small molecules have been assumed to bind to Y220C DNA-binding domain and reactivate cellular mutant p53 functions. In this study, one of the mutant p53 activators is suggested as an Hsp90 inhibitor according to a pyrazole scaffold. To confirm a new ligand as a dual agent, molecular docking and molecular dynamic simulations were performed on both proteins (p53 and Hsp90). Molecular dynamic simulations were also conducted to evaluate the obtained results on the other two pyrazole structures, one known as Hsp90 inhibitor and the other as the reported mutant p53 activator. The findings indicate that the new ligand was stable in the active site of both proteins. Finally, a virtual screening was performed on ZINC database, and a set of new dual agents was proposed according to the new ligand scaffold. (C) 2015 Published by Elsevier Inc.
机译:热激蛋白90s(Hsp90s)在癌症的发展中起着至关重要的作用,其抑制剂是抑制肿瘤的主要靶标。 P53也是一种肿瘤抑制因子,但在癌细胞中,p53基因的突变会导致蛋白质失活和积累。例如,第九个p53癌症突变Y220C使p53核心结构域不稳定。假定小分子与Y220C DNA结合域结合并重新激活细胞突变体p53功能。在这项研究中,根据吡唑支架,突变型p53激活剂之一被认为是Hsp90抑制剂。为了确认新的配体作为双重作用剂,对两种蛋白质(p53和Hsp90)都进行了分子对接和分子动力学模拟。还进行了分子动力学模拟,以评估在其他两种吡唑结构上获得的结果,一种称为Hsp90抑制剂,另一种称为已报道的突变p53激活剂。这些发现表明,新的配体在两种蛋白质的活性位点都是稳定的。最后,在ZINC数据库上进行了虚拟筛选,并根据新的配体支架提出了一组新的双重作用剂。 (C)2015年由Elsevier Inc.出版

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