化学
PLK1
喹唑啉
Polo样激酶
体内
激酶
铅化合物
选择性
化学合成
立体化学
衍生工具(金融)
结构-活动关系
药理学
组合化学
体外
生物化学
细胞周期
医学
生物技术
生物
细胞
经济
金融经济学
催化作用
作者
Italo Beria,R Bossi,Maria Gabriella Brasca,Michele Caruso,Walter Ceccarelli,Gabriele Fachin,Marina Fasolini,Barbara Forte,Francesco Fiorentini,Enrico Pesenti,Daniele Pezzetta,Helena Posteri,Alessandra Scolaro,Stefania Re Depaolini,Barbara Valsasina
标识
DOI:10.1016/j.bmcl.2011.03.054
摘要
As part of our drug discovery effort, we identified and developed 4,5-dihydro-1H-pyrazolo[4,3-h]quinazoline derivatives as PLK1 inhibitors. We now report the optimization of this class that led to the identification of NMS-P937, a potent, selective and orally available PLK1 inhibitor. Also, in order to understand the source of PLK1 selectivity, we determined the crystal structure of PLK1 with NMS-P937. The compound was active in vivo in HCT116 xenograft model after oral administration and is presently in Phase I clinical trials evaluation.
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