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新型热休克蛋白90-细胞周期蛋白依赖性激酶37蛋白质-蛋白质相互作用抑制剂的发现:抗癌活性的筛选与优化

Discovery of new Hsp90-Cdc37 protein-protein interaction inhibitors: screening and optimization of anticancer activity.

作者信息

Dernovšek Jaka, Gradišek Nina, Zajec Živa, Urbančič Dunja, Cingl Jernej, Goričan Tjaša, Grdadolnik Simona Golič, Tomašič Tihomir

机构信息

Faculty of Pharmacy, University of Ljubljana Aškerčeva cesta 7 1000 Ljubljana Slovenia

Laboratory for Molecular Structural Dynamics, Theory Department, National Institute of Chemistry Hajdrihova 19 1001 Ljubljana Slovenia.

出版信息

RSC Adv. 2024 Sep 5;14(39):28347-28375. doi: 10.1039/d4ra05878j. eCollection 2024 Sep 4.

DOI:10.1039/d4ra05878j
PMID:39239280
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11375794/
Abstract

The interaction between heat shock protein 90 (Hsp90) and Hsp90 co-chaperone cell-division cycle 37 (Cdc37) is crucial for the folding and maturation of several oncogenic proteins, particularly protein kinases. This makes the inhibition of this protein-protein interaction (PPI) an interesting target for developing new anticancer compounds. However, due to the large interaction surface, developing PPI inhibitors is challenging. In this work, we describe the discovery of new Hsp90-Cdc37 PPI inhibitors using a ligand-based virtual screening approach. Initial hit compounds showed Hsp90 binding, resulting in anticancer activity in the MCF-7 breast cancer cell line. To optimize their antiproliferative effect, 35 analogs were prepared. Binding affinity for Hsp90 was determined for the most promising compounds, 8c ( = 70.8 μM) and 13g ( = 73.3 μM), both of which interfered with the binding of Cdc37 to Hsp90. This resulted in anticancer activity against Ewing sarcoma (SK-N-MC), breast cancer (MCF-7), and leukemia (THP-1) cell lines . Furthermore, compounds 8c and 13g demonstrated the ability to induce apoptosis in the Ewing sarcoma cell line and caused a decrease in the levels of several known Hsp90 client proteins in MCF-7 cells, all without inducing the heat shock response.

摘要

热休克蛋白90(Hsp90)与Hsp90共伴侣细胞分裂周期蛋白37(Cdc37)之间的相互作用对于几种致癌蛋白尤其是蛋白激酶的折叠和成熟至关重要。这使得抑制这种蛋白质-蛋白质相互作用(PPI)成为开发新型抗癌化合物的一个有吸引力的靶点。然而,由于相互作用表面较大,开发PPI抑制剂具有挑战性。在这项工作中,我们描述了使用基于配体的虚拟筛选方法发现新型Hsp90-Cdc37 PPI抑制剂的过程。最初的活性命中化合物显示出与Hsp90的结合,从而在MCF-7乳腺癌细胞系中产生抗癌活性。为了优化它们的抗增殖作用,制备了35种类似物。测定了最有前景的化合物8c( = 70.8 μM)和13g( = 73.3 μM)与Hsp90的结合亲和力,这两种化合物均干扰了Cdc37与Hsp90的结合。这导致了对尤因肉瘤(SK-N-MC)、乳腺癌(MCF-7)和白血病(THP-1)细胞系的抗癌活性。此外,化合物8c和13g表现出在尤因肉瘤细胞系中诱导凋亡的能力,并导致MCF-7细胞中几种已知Hsp90客户蛋白水平的降低,所有这些均未诱导热休克反应。

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