Discovery of novel exceptionally potent and orally active c-MET PROTACs for the treatment of tumors with MET alterations

细胞凋亡 药理学 医学 癌症研究 细胞生长 细胞 化学 生物化学
作者
Pengyun Li,Changkai Jia,Zhiya Fan,Xiaotong Hu,Wenjuan Zhang,Ke Liu,Shiyang Sun,Haoxin Guo,Ning Yang,Maoxiang Zhu,Xiaomei Zhuang,Junhai Xiao,Zhibing Zheng,Song Li
出处
期刊:Acta Pharmaceutica Sinica B [Elsevier BV]
卷期号:13 (6): 2715-2735 被引量:18
标识
DOI:10.1016/j.apsb.2023.01.014
摘要

Various c-mesenchymal-to-epithelial transition (c-MET) inhibitors are effective in the treatment of non-small cell lung cancer; however, the inevitable drug resistance remains a challenge, limiting their clinical efficacy. Therefore, novel strategies targeting c-MET are urgently required. Herein, through rational structure optimization, we obtained novel exceptionally potent and orally active c-MET proteolysis targeting chimeras (PROTACs) namely D10 and D15 based on thalidomide and tepotinib. D10 and D15 inhibited cell growth with low nanomolar IC50 values and achieved picomolar DC50 values and >99% of maximum degradation (Dmax) in EBC-1 and Hs746T cells. Mechanistically, D10 and D15 dramatically induced cell apoptosis, G1 cell cycle arrest and inhibited cell migration and invasion. Notably, intraperitoneal administration of D10 and D15 significantly inhibited tumor growth in the EBC-1 xenograft model and oral administration of D15 induced approximately complete tumor suppression in the Hs746T xenograft model with well-tolerated dose-schedules. Furthermore, D10 and D15 exerted significant anti-tumor effect in cells with c-METY1230H and c-METD1228N mutations, which are resistant to tepotinib in clinic. These findings demonstrated that D10 and D15 could serve as candidates for the treatment of tumors with MET alterations.
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