Fu Yuantao, Yuan Yinan, Tan Rongliang, Jiang Jinxin, Li Zhilong, Li Tong, Xie Guangjun, Xiao Yibei, Sun Haiying
Jiangsu Key Laboratory of Drug Design and Optimization, Department of Medicinal Chemistry, China Pharmaceutical University, Nanjing, 210009, China.
State Key Laboratory of Natural Medicines, China Pharmaceutical University, Nanjing, 210009, China.
ChemMedChem. 2025 Feb 16;20(4):e202400528. doi: 10.1002/cmdc.202400528. Epub 2024 Nov 25.
Based on a clinical staged small molecular hClpP activator ONC201, a class of novel hClpP agonists with a [1,8]naphthyridinone scaffold was designed, synthesized and evaluated in a series of biochemical and biological assays. Mechanism studies for the representative compound F20 indicated that it can potently bind to and activate hClpP, efficiently promote the degradation of hClpP substrates, robustly induce ATF4/CHOP regulated integrated stress responses, strongly inhibit cell growth and effectively induce apoptosis in a subset of cancer cell lines. F20 showed good PK profiles when dosed by intravenous injection and exhibited moderate oral bioavailability in mice.
基于临床分期的小分子hClpP激活剂ONC201,设计、合成了一类具有[1,8]萘啶酮骨架的新型hClpP激动剂,并在一系列生化和生物学试验中进行了评估。对代表性化合物F20的机制研究表明,它能有效结合并激活hClpP,有效促进hClpP底物的降解,强烈诱导ATF4/CHOP调节的综合应激反应,强烈抑制细胞生长,并有效诱导一部分癌细胞系的凋亡。F20静脉注射给药时显示出良好的药代动力学特征,在小鼠中表现出中等程度的口服生物利用度。
