化学
技术
激酶
对偶(语法数字)
结构-活动关系
化学合成
生物化学
体外
天文
电离层
物理
文学类
艺术
作者
Guonan Cui,Rui Li,Duo An,Yonghua Xie,Chunyan Yu,Wuxin Zou,Yan Xia,Yan Zhang,Kaiwen Feng,Zijian Xu,Xueying Zheng,Tianshu Jing,Yang Yan,Yanxing Wang,Zhengyu Wang,Lijun Wang,Jianhui Huang,Zhiqing Zhang,Chengtao Li
标识
DOI:10.1021/acs.jmedchem.4c02288
摘要
Janus kinase 3 (JAK3) and tyrosine-protein kinase (TEC) play crucial roles in autoimmune diseases. Here, we report the optimization of JAK3/TEC dual covalent inhibitors through a series of rational design strategies. Through the fusion of a fluorine-substituted benzene ring to the piperidine, we achieved compound 8a with improved in vitro activity and selectivity and good drug-like properties. Compound 8a demonstrated excellent therapeutic efficacy in the experimental autoimmune encephalomyelitis (EAE) mouse model of multiple sclerosis orally, with no body weight loss, suggesting a preliminary indication of good safety. These findings support the potential of compound 8a as a promising candidate for the development of new therapies targeting JAK3 and TEC.
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