Identification of the First Selective Activin Receptor-Like Kinase 1 Inhibitor, a Reversible Version of L-783277

被引:5
|
作者
Cho, Hanna [1 ]
Sengupta, Sandip [2 ]
Jeon, Sean S. H. [1 ]
Hur, Wooyoung [2 ]
Choi, Hwan Geun [2 ]
Seo, Hong-Seog [1 ,3 ]
Lee, Byung Joo [4 ,5 ]
Kim, Jeong Hun [4 ,5 ,6 ]
Chung, Minhwan [7 ]
Jeon, Noo Li [7 ]
Kim, Nam Doo [8 ]
Sim, Taebo [1 ,2 ]
机构
[1] Korea Univ, KIST Grad Sch Converging Sci & Technol, 145 Anam Ro, Seoul 02841, South Korea
[2] KIST, Chem Kinom Res Ctr, 5 Hwarangro 14 Gil, Seoul 02792, South Korea
[3] Korea Univ, Guro Hosp, Cardiovasc Ctr, 80 Guro Dong, Seoul 152703, South Korea
[4] Seoul Natl Univ Hosp, Clin Res Inst, Fight Angiogenesis Related Blindness Lab, 101 Daehak Ro, Seoul 03080, South Korea
[5] Seoul Natl Univ, Coll Med, Dept Biomed Sci, 103 Daehakro, Seoul 03080, South Korea
[6] Seoul Natl Univ, Coll Med, Dept Ophthalmol, 101 Daehak Ro, Seoul 03080, South Korea
[7] Seoul Natl Univ, Mech Engn, 1 Gwanak Ro, Seoul 08826, South Korea
[8] Daegu Gyeongbuk Med Innovat Fdn, 2387 Dalgubeol Daero, Daegu 42019, South Korea
基金
新加坡国家研究基金会;
关键词
BONE MORPHOGENETIC PROTEIN; RESORCYLIC ACID LACTONES; ABSOLUTE-CONFIGURATIONS; NEGATIVE REGULATION; ID PROTEINS; ALK1; ANALOGS; DIFFERENTIATION; ANGIOGENESIS; ACTIVATION;
D O I
10.1021/acs.jmedchem.6b01679
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
We synthesized 1 (San78-130), a reversible version of L-783277, as a selective and potent ALK1 inhibitor. Our study showed that 1 possesses great kinase selectivity against a panel of 342 kinases and more potent activity against ALK1 than L-783277. Among the six ALK isotypes (ALK1-6), ALK1 is most significantly inhibited by compound 1. Compound 1 suppresses the BMP9-induced Smad1/5 pathway by mainly inhibiting ALK1 in C2C12 cells. Our molecular dynamics simulations suggest that H-bonding interaction between the C-4' hydroxyl group of 1 and Arg334 of ALK1 substantially contributes to the ALK1 inhibition. To the best of our knowledge, 1 is the first selective ALK1 inhibitor. Furthermore, compound 1 promoted angiogenesis in both endothelial tube formation and microfluidic chip based 3D angiogenesis assays, suggesting that 1 could be a lead compound for therapeutic angiogenesis agents. Our study may provide an insight into designing selective and potent inhibitors against ALK1.
引用
收藏
页码:1495 / 1508
页数:14
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