Sun Juan, Liu Han-Yu, Xu Ruo-Fei, Zhu Hai-Liang
School of Life Sciences, Shandong University of Technology, Zibo 255049, PR China; Elion Nature Biological Technology Co., Ltd, Nanjing 210046, PR China.
School of Life Sciences, Shandong University of Technology, Zibo 255049, PR China.
Bioorg Med Chem. 2017 Dec 15;25(24):6581-6588. doi: 10.1016/j.bmc.2017.10.035. Epub 2017 Oct 28.
Recent progress in the development of small molecular skeleton-derived polo-like kinase (PLK1) catalytic domain (K) inhibitors has led to the synthesis of multiple ligands with high binding affinity. However, few systematic analyses have been conducted to identify key PLK1-PBD domain and characterize their interactions with potent PLK1 inhibitors. Therefore, we designed a series of PLK1-PBD inhibitors with an in silico scaffold modification strategy. A docking simulation combined with a primary screen in vitro were performed to filter for the lead compound, which was then substituted, synthesized and evaluated by a variety of bioassays. The biological profile of 4v suggests that this compound may be developed as a potential anticancer agent.
小分子骨架衍生的 polo 样激酶(PLK1)催化结构域(K)抑制剂开发方面的最新进展已促成多种具有高结合亲和力的配体的合成。然而,很少有系统分析来鉴定关键的 PLK1-PBD 结构域并表征它们与强效 PLK1 抑制剂的相互作用。因此,我们采用计算机辅助支架修饰策略设计了一系列 PLK1-PBD 抑制剂。进行对接模拟并结合体外初步筛选以筛选先导化合物,然后对其进行取代、合成并通过多种生物测定进行评估。4v 的生物学特性表明该化合物可能被开发成为一种潜在的抗癌药物。
