显性阴性polo样激酶1诱导的有丝分裂灾难与cdc25C的功能无关。

J P Cogswell, C E Brown, J E Bisi, S D Neill
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引用次数: 0

摘要

polo样激酶1 (PLK1)已被证明在有丝分裂中起关键作用,是癌症治疗干预的一个可能靶点。至少在非洲爪蟾中,PLK1通过磷酸化和激活cdc25C磷酸酶来启动有丝分裂级联。此外,PLK1功能的丧失已被证明在HeLa宫颈癌细胞系中诱导有丝分裂灾难,但在正常的Hs68成纤维细胞中没有。我们想了解HeLa细胞中的选择性有丝分裂突变是否可以扩展到其他肿瘤类型,如果是这样,它是否可以归因于肿瘤特异性的cdc25C活化对PLK1依赖性的丧失。当PLK1功能通过腺病毒传递的显性阴性基因被阻断时,我们在大多数肿瘤细胞系中观察到肿瘤选择性凋亡。在一些细胞系中,显性阴性PLK1诱导了类似于HeLa细胞的有丝分裂灾难(K. E. Mundt et al, Biochem)。生物物理学:普通。科学通报,23(3):377-385,1997)。正常的人乳腺上皮细胞,虽然在有丝分裂中被阻止,但似乎逃脱了中心体成熟的丧失和肿瘤系有丝分裂的灾难。在人乳腺上皮细胞和肿瘤细胞系中,无论是否发生有丝分裂突变,cdc25C的有丝分裂磷酸化和cdk1的激活都被显性阴性PLK1阻断。这些数据有力地证明,有丝分裂灾难不是由于缺乏对PLK1激活cdc25C的依赖性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Dominant-negative polo-like kinase 1 induces mitotic catastrophe independent of cdc25C function.

Polo-like kinase 1 (PLK1), which has been shown to have a critical role in mitosis, is one possible target for cancer therapeutic intervention. PLK1, at least in Xenopus, starts the mitotic cascade by phosphorylating and activating cdc25C phosphatase. Also, loss of PLK1 function has been shown to induce mitotic catastrophe in a HeLa cervical carcinoma cell line but not in normal Hs68 fibroblasts. We wanted to understand whether the selective mitotic catastrophe in HeLa cells could be extended to other tumor types, and, if so, whether it could be attributable to a tumor-specific loss of dependence on PLK1 for cdc25C activation. When PLK1 function was blocked through adenovirus delivery of a dominant-negative gene, we observed tumor-selective apoptosis in most tumor cell lines. In some lines, dominant-negative PLK1 induced a mitotic catastrophe similar to that published in HeLa cells (K. E. Mundt et al., Biochem. Biophys Res. Commun., 239: 377-385, 1997). Normal human mammary epithelial cells, although arrested in mitosis, appeared to escape the loss of centrosome maturation and mitotic catastrophe seen in tumor lines. Mitotic phosphorylation of cdc25C and activation of cdk1 was blocked by dominant-negative PLK1 in human mammary epithelial cells as well as in the tumor lines regardless of whether they underwent mitotic catastrophe. These data strongly argue that the mitotic catastrophe is not attributable to a lack of dependence for PLK1 in activating cdc25C.

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