posted on 2015-03-12, 00:00authored byYuchi Ma, Guangqiang Sun, Danqi Chen, Xia Peng, Yue-Lei Chen, Yi Su, Yinchun Ji, Jin Liang, Xin Wang, Lin Chen, Jian Ding, Bing Xiong, Jing Ai, Meiyu Geng, Jingkang Shen
c-Met
has emerged as an attractive target for targeted cancer therapy
because of its abnormal activation in many cancer cells. To identify
high potent and selective c-Met inhibitors, we started with profiling
the potency and in vitro metabolic stability of a reported hit 7. By rational design, a novel sulfonylpyrazolo[4,3-b]pyridine 9 with improved DMPK properties
was discovered. Further elaboration of π–π stacking
interactions and solvent accessible polar moieties led to a series
of highly potent and selective type I c-Met inhibitors. On the basis
of in vitro and in vivo pharmacological and pharmacokinetics studies,
compound 46 was selected as a preclinical candidate for
further anticancer drug development.