硫醚
化学
恶二唑
小分子
联苯
立体化学
乙醚
Jurkat细胞
体内
分子
IC50型
结构-活动关系
晶体结构
组合化学
体外
T细胞
免疫系统
生物化学
结晶学
生物技术
有机化学
生物
免疫学
作者
Jin Liu,Yao Cheng,L. Yuan,Ting Liu,Yong Ruan,Yichang Ren,Ling Li,Sheng Jiang,Yibei Xiao,Jianjun Chen
标识
DOI:10.1021/acs.jmedchem.3c01141
摘要
Current small-molecule PD-1/PD-L1 inhibitors are mainly based on the arylmethylamine/biphenyl core scaffold. Herein, we designed for the first time a series of non-arylmethylamine analogues (oxadiazole thioether derivatives) as small-molecule PD-1/PD-L1 inhibitors. Among them, compound LP23 exhibited the most potent PD-L1 inhibitory activity with an IC50 of 16.7 nM, 3.2-fold better than the lead BMS-202 (IC50 = 53.6 nM). The X-ray crystal structure of LP23 in complex with PD-L1 was solved at a resolution of 2.6 Å, which further confirmed the high binding affinity of LP23 to PD-L1. In the HepG2/Jurkat T cell co-culture model, LP23 effectively promoted HepG2 cell death by restoring the immune function of T cells. In addition, LP23 showed excellent in vivo antitumor efficacy (TGI = 88.6% at 30 mg/kg) and benign toxicity profiles in a B16-F10 tumor model by modulating PD-L1. In summary, LP23 represents the first non-arylmethylamine-based small-molecule PD-1/PD-L1 inhibitor worthy of further investigation.
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