化学
黑色素瘤
热休克蛋白90
细胞周期检查点
癌症研究
结构-活动关系
细胞培养
药理学
蛋白激酶B
细胞周期
细胞生长
细胞周期蛋白D1
伴侣(临床)
细胞周期进展
CDC20型
广谱
细胞
联合疗法
威罗菲尼
肿瘤细胞
细胞周期蛋白依赖激酶
下调和上调
作者
Qingsong Chen,Xiangyang Le,Qiwan Wen,Shuyang Cao,Yating Guo,Xiaoqi Weng,Lei Zhang,Junjie Wei,Menglan Zou,Liqing Hu,Qianbin Li,Suyou Liu,Zhuo Chen
标识
DOI:10.1021/acs.jmedchem.5c01444
摘要
Cell division cycle 20 homologue (Cdc20) is a cancer-promoting protein that is expressed at higher levels in tumor tissues than in neighboring tissues, and the degradation of Cdc20 is considered to be an effective strategy to inhibit tumor growth. Here, we designed Cdc20/Hsp90 dual-target inhibitors, hoping to synergistically exert antitumor effects. The preferred compound 2b exerted an extensive antitumor spectrum and lower toxicity, which closely bound to Cdc20 and Hsp90, respectively. Additionally, compound 2b exerted potent antitumor activity through reducing p53-mediated Cdc20, upregulating Bim, downregulating Cyclin B1 expression, and disturbing B-Raf and AKT pathways via destroying Hsp90 chaperone function. Furthermore, compound 2b inhibited parental melanoma growth, comparable to the marketed agent Vemurafenib and superior to the combination of Apcin and BIIB021 . Interestingly, compound 2b overcame Vemurafenib -induced resistant melanoma, superior to parental melanoma, indicating that compound 2b is a promising Cdc20/Hsp90 dual-target inhibitor for therapy of acquired resistance of malignant melanoma.
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