| Literature DB >> 28043720 |
Yifei Yang1, Yuan Zhang1, LingYun Yang2, Leilei Zhao2, Lianghui Si2, Huibin Zhang2, Qingsong Liu3, Jinpei Zhou4.
Abstract
Receptor tyrosine kinase c-Met acts as an alternative angiogenic pathway in the process and contents of cancers. A series of imidazopyridine derivatives were designed and synthesized according to the established docking studies as possible c-Met inhibitors. Most of these imidazopyridine derivatives displayed nanomolar potency against c-Met in both biochemical enzymatic screens and cellular pharmacology studies. Especially, compound 7g exhibited the most inhibitory activity against c-Met with IC50 of 53.4nM and 253nM in enzymatic and cellular level, respectively. Following that, the compound 7g was docked into the protein of c-Met and the structure-activity relationship was analyzed in detail. These findings indicated that the novel imidazopyridine derivative compound 7g was a potential c-Met inhibitor deserving further investigation for cancer treatment.Entities:
Keywords: Cancer; Imidazopyridine derivatives; Molecular docking; c-Met kinase inhibitors
Mesh:
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Year: 2016 PMID: 28043720 DOI: 10.1016/j.bioorg.2016.12.002
Source DB: PubMed Journal: Bioorg Chem ISSN: 0045-2068 Impact factor: 5.275