Design and synthesis of highly selective Janus kinase 3 covalent inhibitors for the treatment of rheumatoid arthritis

Author:

Yao Hualiang1,Zhang Jie1,Zheng Qisheng2,Zeng Xianxia1,Huang Huaizheng1,Ling Zhen1,Tang Minghai3,Chen Zhiquan1,Wang Wenchu4,He Linhong1ORCID

Affiliation:

1. Guangxi Key Laboratory of Bioactive Molecules Research and Evaluation, Pharmaceutical College Guangxi Medical University Nanning China

2. School of Medicine Guangxi University Nanning China

3. State Key Laboratory of Biotherapy and Cancer Center, National Clinical Research Center for Geriatrics West China Hospital of Sichuan University Chengdu China

4. Center for Translational Medicine, School of Basic Medical Sciences Guangxi Medical University Nanning China

Abstract

AbstractSelective inhibition of Janus kinase 3 (JAK3) is a promising strategy for the treatment of autoimmune diseases. Based on the discovery of a hydrophobic pocket unutilized between the lead compound RB1 and the JAK3 protein, a series of covalent JAK3 inhibitors were prepared by introducing various aromatic fragments to RB1. Among them, J1b (JAK3 IC50 = 7.2 nM, other JAKs IC50 > 1000 nM) stood out because of its low toxicity (MTD > 2 g/kg) and superior anti‐inflammatory activity in Institute of Cancer Research mice. Moreover, the acceptable bioavailability (F% = 31.69%) ensured that J1b displayed excellent immune regulation in collagen‐induced arthritis mice, whose joints in the high‐dose group were almost recovered to a normal state. Given its clear kinase selectivity (Bmx IC50 = 539.9 nM, other Cys909 kinases IC50 > 1000 nM), J1b was nominated as a highly selective JAK3 covalent inhibitor, which could be used to safely treat arthritis and other autoimmune diseases.

Publisher

Wiley

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