Discovery of 5-Azaquinoxaline Derivatives as Potent and Orally Bioavailable Allosteric SHP2 Inhibitors

Mohamed S. A. Elsayed,James F. Blake,Mark L. Boys, Eric Brown, Bruno D. Chapsal, Mark J. Chicarelli,Adam W. Cook,Jay B. Fell,John P. Fischer, Lauren Hanson, Christine Lemieux,Matthew C. Martinson, Joseph McCown, Oren T. McNulty, Macedonio J. Mejia,Nickolas A. Neitzel, Jennifer N. Otten, Martha E. Rodriguez, Daniel Wilcox, Christina E. Wong, Yeyun Zhou,Ronald J. Hinklin

ACS MEDICINAL CHEMISTRY LETTERS（2023）

引用 0|浏览2

暂无评分

摘要

SHP2 has emerged as an important target for oncology small-molecule drug discovery. As a nonreceptor tyrosine phosphatase within the MAPK pathway, it has been shown to control cell growth, differentiation, and oncogenic transformation. We used structure-based design to find a novel class of potent and orally bioavailable SHP2 inhibitors. Our efforts led to the discovery of the 5-azaquinoxaline as a new core for developing this class of compounds. Optimization of the potency and properties of this scaffold generated compound 30, that exhibited potent in vitro SHP2 inhibition and showed excellent in vivo efficacy and pharmacokinetic profile.

查看译文

关键词

SHP2,Phosphatase inhibitor,Structure-baseddesign,MAPK,In vivo

AI 理解论文

溯源树

样例

生成溯源树，研究论文发展脉络

Chat Paper

正在生成论文摘要