REVIEW OF DESIGN APPROACHES AND CLINICAL PROGRESS OF MDM2 INHIBITORS

Chiragkumar J. Gohil, M. Noolvi, C. Patel, D. Sen
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引用次数: 2

Abstract

Activation of the oncogenes and inhibition of the apoptotic function of the p53 protein is a gateway for the cancer genesis. Interaction of the MDM2 protein with p53 protein is responsible for the inhibition of the p53 function. Inhibiting the p53-MDM2 interaction by drug will lead to the p53 release in the cancer cells. And can restart the apoptosis in the cancer cell. Computational methods successfully used for the design and development of the new, potent MDM2 inhibitors. Researchers and pharma companies used rational approach like target-based drug design or ligand-based drug design to develop the novel MDM2 inhibitors. The number of MDM2 inhibitors, has been designed by the computer-aided drug design and in-silico studies. In clinical studies, MDM2 inhibitors are led by RG7112. RG7112 completed its phase-1 trials in 2016, and recently it is under phase-2 trials. Along with RG7112, the number of potent MDM2 inhibitors entered the clinical trials successfully. It indicates the successful development of this class (MDM2 inhibitors). MDM2 inhibitors were found very effective in various studies for the treatment of various kinds of cancers. They have good selectivity for the tumor cells over the normal cells. It induced the dose dependent cell cycle arrest only; in the normal cells. In studies, MDM2 inhibitors successfully detached the p53 protein from the MDM2 protein. And restart the cell-killing function of the p53 protein in the cancer cells. Hence, MDM2 inhibitors can selectively kill the cancer cells over the normal cells.
mdm2抑制剂的设计方法及临床进展综述
癌基因的激活和p53蛋白凋亡功能的抑制是癌症发生的门户。MDM2蛋白与p53蛋白的相互作用是抑制p53功能的原因。通过药物抑制p53- mdm2相互作用可导致p53在癌细胞内释放。并能重启癌细胞的凋亡。计算方法成功地用于设计和开发新的,有效的MDM2抑制剂。研究人员和制药公司采用基于靶标的药物设计或基于配体的药物设计等合理方法开发新型MDM2抑制剂。MDM2抑制剂的数量,已经通过计算机辅助药物设计和计算机研究进行了设计。在临床研究中,MDM2抑制剂以RG7112为先导。RG7112于2016年完成了第一阶段试验,最近正在进行第二阶段试验。与RG7112一起,许多强效MDM2抑制剂成功进入临床试验。这表明这类(MDM2抑制剂)的开发成功。在各种研究中发现MDM2抑制剂对治疗各种癌症非常有效。与正常细胞相比,它们对肿瘤细胞有很好的选择性。仅诱导剂量依赖性细胞周期阻滞;在正常细胞中。在研究中,MDM2抑制剂成功地将p53蛋白从MDM2蛋白中分离出来。重新启动癌细胞中p53蛋白的细胞杀伤功能。因此,MDM2抑制剂可以选择性地杀死癌细胞而不是正常细胞。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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