Discovery of ganoderic acid A (GAA) PROTACs as MDM2 protein degraders for the treatment of breast cancer

被引:9
作者
Li, Yan [1 ]
Li, Guangyu [1 ]
Zuo, Chenwei [1 ]
Wang, Xiaolin [1 ]
Han, Fang [1 ]
Jia, Yi [1 ]
Shang, Hai [1 ]
Tian, Yu [1 ]
机构
[1] Chinese Acad Med Sci & Peking Union Med Coll, Inst Med Plant Dev, State Key Lab Qual Ensurance & Sustainable Use Dao, Beijing 100193, Peoples R China
来源
EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY | 2024年 / 270卷
关键词
Ganoderic acid A; PROTAC; MDM2; Breast cancer; TNBC; NEGATIVE REGULATOR; IN-VIVO; P21; APOPTOSIS; PATHWAY; GROWTH; P21(WAF1/CIP1); INHIBITOR; ARREST; CELLS;
D O I
10.1016/j.ejmech.2024.116367
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Breast cancer is one of the most common female malignant tumors, with triple-negative breast cancer (TNBC) being the most specific, highly invasive, metastatic and associated with a poor prognosis. Our previous study showed that the natural product ganoderic acid A (GAA) has a certain affinity for MDM2. In this study, two series of novel GAA PROTACs C1-C10 - C10 and V1-V10 - V10 were designed and synthesized for the treatment of breast cancer. The antitumor activity of these compounds was evaluated against four human tumor cell lines (MCF-7, MDA-MB231, SJSA-1, and HepG2). Among them, V9 and V10 showed stronger anti-proliferative effects against breast cancer cells, and V10 showed the best selectivity in MDA-MB-231 cells (TNBC), which was 5-fold higher than that of the lead compound GAA. Preliminary structure-activity analysis revealed that V-series GAA PROTACs had better effects than C-series, and the introduction of 2O-4O PEG linkers could significantly improve the antitumor activity. Molecular docking, surface plasmon resonance (SPR), cellular thermal shift assay (CETSA), and Western blot researches showed that both V9 and V10 could bind with MDM2, and degrade the protein through the ubiquitin-proteasome system. Molecular dynamics simulation (MD) revealed that V10 is a bifunctional molecule that can bind to von Hippel-Lindau (VHL) at one end and target MDM2 at the other. In addition, V10 promoted the upregulation of p21 in p53-mutant MDA-MB-231 cells, and induced apoptosis via down-regulation of the bcl2/bax ratio and the expression of cyclin B1. Finally, in vivo experiments showed that, V10 also exhibited good tumor inhibitory activity in xenografted TNBC zebrafish models, with an inhibition rate of 27.2% at 50 mu g/mL. In conclusion, our results suggested that V10 has anti-tumor effects on p53-mutant breast cancer in vitro and in vivo, , and may be used as a novel lead compound for the future development of TNBC.
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页数:20
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