Design, synthesis, and SAR study of highly potent, selective, irreversible covalent JAK3 inhibitors

被引:0
|
作者
Linhong He
Mingfeng Shao
Taijin Wang
Tingxuan Lan
Chufeng Zhang
Lijuan Chen
机构
[1] Sichuan University and Collaborative Innovation Center,Cancer Center, West China Hospital
[2] Guangxi Medical University,Department of Pharmacology, School of Pharmacy
来源
Molecular Diversity | 2018年 / 22卷
关键词
JAK3; Covalent inhibitor; Selectivity; Structure–activity relationship (SAR); Docking;
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中图分类号
学科分类号
摘要
Here, we report the design and synthesis of pyrimidinyl heterocyclic compounds containing terminal electrophiles as irreversible covalent JAK3 inhibitors that exploit a unique cysteine (Cys909) residue in JAK3. Investigation of the structure–activity relationship utilizing kinase assays resulted in the identification of potent and selective JAK3 inhibitors such as T1, T8, T15, T22, and T29. Among them, T29 was verified as a promising JAK3 irreversible inhibitor that possessed the best bioactivity and selectivity against JAKs and kinases containing a cysteine in the residue analogous to Cys909 in JAK3, suggesting that covalent modification of this Cys residue allowed the identification of a highly selective JAK3 inhibitor. Moreover, T29 also displayed a significant anti-inflammatory effect in ICR mice through the inhibition of increased paw thickness, which is worth further optimization to increase its potency and medicinal properties.
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页码:343 / 358
页数:15
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