一种用于Hsp90 C端抑制的支架融合方法:嵌合文库的合成与评估
A Scaffold Merging Approach to Hsp90 C-terminal Inhibition: Synthesis and Evaluation of a Chimeric Library.
作者信息
Davis Rachel E, Zhang Zheng, Blagg Brian S J
机构信息
Department of Medicinal Chemistry, The University of Kansas, 1251 Wescoe Hall Drive, 4070 Malott Hall, Lawrence, Kansas 66045, United States.
出版信息
Medchemcomm. 2017 Mar 1;8(3):593-598. doi: 10.1039/C6MD00377J. Epub 2017 Jan 17.
Abstract
Inhibition of the Hsp90 C-terminus is an attractive therapeutic paradigm for the treatment of cancer, however the developmental space of C-terminal inhibitors is limited. It was hypothesized that the combination of two previously identified scaffolds into a single structure could provide a platform for which to probe the three-dimensional space within the Hsp90 C-terminal binding pocket. The resulting chimeric compounds displayed anti-proliferative activity at low micromolar concentrations and manifested inhibitory activity in an Hsp90-dependent rematuration assay. Initial structure-activity relationships suggest that this new scaffold binds Hsp90 in a conformation different from that of the parent compounds, and consequently, provides a new opportunity to develop more efficacious inhibitors of the Hsp90 C-terminal binding pocket.
摘要
抑制热休克蛋白90(Hsp90)的C末端是一种颇具吸引力的癌症治疗模式,然而C末端抑制剂的研发空间有限。据推测,将两个先前确定的支架结构组合成单一结构可为探索Hsp90 C末端结合口袋内的三维空间提供一个平台。所得的嵌合化合物在低微摩尔浓度下显示出抗增殖活性,并在Hsp90依赖性复性试验中表现出抑制活性。初步的构效关系表明,这种新的支架结构以与母体化合物不同的构象结合Hsp90,因此为开发更有效的Hsp90 C末端结合口袋抑制剂提供了新机会。
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