Structure-based design and synthesis of bicyclic fused-pyridines as MEK inhibitors.

Hejun Lu,Wangyang Tu,Hongbo Fei,Guoji Xu,Qiyue Hu,Lei Zhang,Bing Lin,Jijun Yuan,Junzhao Yin,Aishen Gong,Mimi Wan,Dan Wang,Xiaoyan Zhu,Jun Feng,Qian Wang,Piaoyang Sun

Bioorganic & Medicinal Chemistry Letters（2014）

Cited 6|Views9

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Abstract

The MAPK pathway is identified as one of the most important pathways involved in cell proliferation and differentiation. A key kinase in the pathway, the Mitogen-activated protein kinase kinase (MEK) is recognized as a promising target for antitumor drugs. Structure-based design and optimization of known MEK inhibitors resulted in identification of compound 10a as a potent non-ATP competitive MEK inhibitor in both in vitro and in vivo tests.

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Key words

MEK,Bicyclic,Fused-pyridine,Cancer,SBDD

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