PLK1
溴尿嘧啶
化学
Polo样激酶
BRD4
激酶
结构-活动关系
对偶(语法数字)
立体化学
生物化学
体外
细胞
细胞周期
组蛋白
艺术
文学类
基因
作者
Shuai Liu,Hailemichael O. Yosief,Lingling Dai,He Huang,Gagan Dhawan,Xiaofeng Zhang,Alex Muthengi,Justin M. Roberts,Dennis L. Buckley,Jennifer A. Perry,Lei Wu,James E. Bradner,Jun Qi,Wei Zhang
标识
DOI:10.1021/acs.jmedchem.8b00765
摘要
The simultaneous inhibition of polo-like kinase 1 (PLK1) and BRD4 bromodomain by a single molecule could lead to the development of an effective therapeutic strategy for a variety of diseases in which PLK1 and BRD4 are implicated. Compound 23 has been found to be a potent dual kinase–bromodomain inhibitor (BRD4-BD1 IC50 = 28 nM, PLK1 IC50 = 40 nM). Compound 6 was found to be the most selective PLK1 inhibitor over BRD4 in our series (BRD4-BD1 IC50 = 2579 nM, PLK1 IC50 = 9.9 nM). Molecular docking studies with 23 and BRD4-BD1/PLK1 as well as with 6 corroborate the biochemical assay results.
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