Discovery of N-(3-(5-((3-acrylamido-4-(morpholine-4-carbonyl) phenyl)amino)-1-methyl-6-oxo-1,6-dihydropyridin-3-yl)-2-methylphenyl)-4-(tert-butyl)benzamide (CHMFL-BTK-01) as a highly selective irreversible Bruton's tyrosine kinase (BTK) inhibitor

被引:19
作者
Liang, Qianmao [1 ,2 ]
Chen, Yongfei [2 ,3 ]
Yu, Kailin [2 ,4 ]
Chen, Cheng [2 ,3 ]
Zhang, Shouxiang [5 ,6 ]
Wang, Aoli [2 ,4 ]
Wang, Wei [2 ,3 ]
Wu, Hong [2 ,4 ]
Liu, Xiaochuan [1 ,2 ]
Wang, Beilei [2 ,3 ]
Wang, Li [2 ,3 ]
Hu, Zhenquan [2 ,3 ]
Wang, Wenchao [2 ,3 ]
Ren, Tao [7 ]
Zhang, Shanchun [3 ,8 ]
Liu, Qingsong [2 ,3 ,4 ,7 ]
Yun, Cai-Hong [5 ,6 ]
Liu, Jing [2 ,3 ]
机构
[1] Univ Sci & Technol China, Dept Chem, Hefei 230036, Anhui, Peoples R China
[2] Chinese Acad Sci, High Field Magnet Lab, Mailbox 1110,350 Shushanhu Rd, Hefei 230031, Anhui, Peoples R China
[3] CHMFL HCMTC Target Therapy Joint Lab, 350 Shushanhu Rd, Hefei 230031, Anhui, Peoples R China
[4] Univ Sci & Technol China, Hefei 230036, Anhui, Peoples R China
[5] Peking Univ, Hlth Sci Ctr, Inst Syst Biomed, Dept Biophys,Beijing Key Lab Tumor Syst Biol, Beijing 100191, Peoples R China
[6] Peking Univ, Hlth Sci Ctr, Sch Basic Med Sci, Ctr Mol & Translat Med, Beijing 100191, Peoples R China
[7] Chinese Acad Sci, Inst Technol Innovat, Precis Targeted Therapy Discovery Ctr, Hefei Inst Phys Sci, Hefei 230088, Anhui, Peoples R China
[8] Hefei Cosource Med Technol Co LTD, 358 Ganquan Rd, Hefei 230031, Anhui, Peoples R China
来源
EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY | 2017年 / 131卷
基金
中国国家自然科学基金;
关键词
BTK; Irreversible inhibitor; Kinase inhibitor; Structure-activity relationship; B-cell lymphoma; X-LINKED AGAMMAGLOBULINEMIA; B-CELL; RHEUMATOID-ARTHRITIS; ACTIVATION; COVALENT; IBRUTINIB; POTENT; GENE; PROLIFERATION; EXPRESSION;
D O I
10.1016/j.ejmech.2017.03.001
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Currently there are several irreversible BTK inhibitors targeting Cys481 residue under preclinical or clinical development. However, most of these inhibitors also targeted other Idnases such as BMX, JAK3, and EGFR that bear the highly similar active cysteine residues. Through a structure-based drug design approach, we discovered a highly potent (IC50: 7 nM) irreversible BTK inhibitor compound 9 (CHMFL-BTK-01), which displayed a high selectivity profile in KINOMEscan (S score (35) = 0.00) among 468 kinases/mutants at the concentration of 1 mu M. Compound 9 completely abolished BMX, JAK3 and EGFR's activity. Both X-ray crystal structure and cysteine-serine mutation mediated rescue experiment confirmed 9's irreversible binding mode. 9 also potently inhibited BTK Y223 auto-phosphorylation (EC50: <30 nM), arrested cell cycle in G0/G1 phase and induced apoptosis in U2932 and Pfeiffer cells. We believe these features would make 9 a good pharmacological tool to study the BTK related pathology. (C) 2017 Elsevier Masson SAS. All rights reserved.
引用
收藏
页码:107 / 125
页数:19
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