期刊
CELL CHEMICAL BIOLOGY
卷 28, 期 10, 页码 1446-+出版社
CELL PRESS
DOI: 10.1016/j.chembiol.2021.03.016
关键词
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资金
- National Natural Science Foundation of China, China [82073766, 81872737, 81773639, 81930100]
- Foundation Research Project of Jiangsu Province, China [BK20201331]
- National Science & Technology Major Project Key New Drug Creation and Manufacturing Program,China [2018ZX09711002]
- Double First Class Innovation Team of China Phar-maceutical University, China [CPU2018GY02]
- Open Project of State KeyLaboratory of Natural Medicines, China Pharmaceutical University, China [SKLNMZZCX202003]
- Jiangsu Qing Lan Project, China
- Young Elite Scientists Sponsorship Program by CAST, China [YESS20180146]
The study identified DDO-6600 as a covalent modifier of Hsp90, which inhibits tumor cell proliferation, induces apoptosis, and reduces cell motility.
Heat shock protein (Hsp90), a critical molecular chaperone that regulates the maturation of a large number of oncogenic client proteins, plays an essential role in the growth of neoplastic cells. Herein, DDO-6600 is identified to covalent modification of Cys598 on Hsp90 from in silico study and is verified by a series of biological assays. We demonstrated that DDO-6600 covalently bound to Cys598 on the Hsp90 C terminus and exhibited antiproliferative activities against multiple tumor cells without inhibiting ATPase activity. Further studies showed that DDO-6600 disrupted the interaction between Hsp90 and Cdc37, which induced the degradation of kinase client proteins in multiple tumor cell lines, promoted apoptosis, and inhibited cell motility. Our findings offer mechanic insights into the covalent modification of Hsp90 and provide an alternative strategy for the development of Hsp90 covalent regulators or chemical probes to explore the therapeutical potential of Hsp90.
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