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Identification of a novel Polo-like kinase 1 inhibitor that specifically blocks the functions of Polo-Box domain

机译:鉴定一种新型的Polo样激酶1抑制剂该抑制剂可特异性阻断Polo-Box结构域的功能

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摘要

Polo-like kinase 1 (Plk1) is a promising target for cancer therapy due to its essential role in cell division. In addition to a highly conserved kinase domain, Plk1 also contains a Polo-Box domain (PBD), which is essential for Plk1's subcellular localization and mitotic functions. We adopted a fluorescence polarization assay and identified a new Plk1 PBD inhibitor T521 from a small-molecule compound library. T521 specifically inhibits the PBD of Plk1, but not those of Plk2-3. T521 exhibits covalent binding to some lysine residues of Plk1 PBD, which causes significant changes in the secondary structure of Plk1 PBD. Using a cell-based assay, we showed that T521 impedes the interaction between Plk1 and Bub1, a mitotic checkpoint protein. Moreover, HeLa cells treated with T521 exhibited dramatic mitotic defects. Importantly, T521 suppresses the growth of A549 cells in xenograft nude mice. Taken together, we have identified a novel Plk1 inhibitor that specifically disrupts the functions of Plk1 PBD and shows anticancer activity.
机译:由于其在细胞分裂中的重要作用,Polo样激酶1(Plk1)是有希望的癌症治疗靶标。除了高度保守的激酶结构域之外,Plk1还包含一个Polo-Box域(PBD),这对Plk1的亚细胞定位和有丝分裂功能至关重要。我们采用了荧光偏振测定法,并从一个小分子化合物库中鉴定了一种新的Plk1 PBD抑制剂T521。 T521特异性抑制Plk1的PBD,但不抑制Plk2-3的PBD。 T521表现出与Plk1 PBD的某些赖氨酸残基共价结合,从而导致Plk1 PBD的二级结构发生重大变化。使用基于细胞的分析,我们表明T521阻止Plk1和Bub1(有丝分裂检查点蛋白)之间的相互作用。此外,用T521处理的HeLa细胞表现出明显的有丝分裂缺陷。重要的是,T521抑制异种移植裸鼠中A549细胞的生长。综上所述,我们已经确定了一种新型的Plk1抑制剂,该抑制剂可特异性破坏Plk1 PBD的功能并显示抗癌活性。

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