Structure Based Design of N-(3-((1H-Pyrazolo[3,4-b]pyridin-5-yl)ethynyl)benzenesulfonamides as Selective Leucine-Zipper and Sterile-α Motif Kinase (ZAK) Inhibitors

Yu Chang,Xiaoyun Lu,Marthandam Asokan Shibu,Yi Bo Dai,JinFeng Luo,Yan Zhang,Yingjun Li,Peng Zhao,Zhang Zhang,Yong Xu,Zheng Chao Tu,Qing Wen Zhang,Cai-Hong Yun,Chih Yang Huang,Ke Ding

Structure Based Design of N-(3-((1H-Pyrazolo[3,4-b]pyridin-5-yl)ethynyl)benzenesulfonamides as Selective Leucine-Zipper and Sterile-α Motif Kinase (ZAK) Inhibitors

2017

Yu Chang
Xiaoyun Lu
Marthandam Asokan Shibu
Yi Bo Dai
JinFeng Luo
Yan Zhang
Yingjun Li
Peng Zhao
Zhang Zhang
Yong Xu
Zheng Chao Tu
Qing Wen Zhang
Cai-Hong Yun
Chih Yang Huang
Ke Ding

A series of N-(3-((1H-pyrazolo[3,4-b]pyridin-5-yl)ethynyl)benzenesulfonamides were designed as the first class of highly selective ZAK inhibitors. The representative compound 3h strongly inhibits the kinase activity of ZAK with an IC50 of 3.3 nM and dose-dependently suppresses the activation of ZAK downstream signals in vitro and in vivo, while it is significantly less potent for the majority of 403 nonmutated kinases evaluated. Compound 3h also exhibits orally therapeutic effects on cardiac hypertrophy in a spontaneous hypertensive rat model.

Keywords:

Biochemistry
Spontaneous hypertensive rat
Leucine zipper
In vivo
IC50
Chemistry
In vitro
Kinase
Muscle hypertrophy
Stereochemistry
Molecular Docking Simulation
structure based
kinase activity

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