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Functional cdc25C Dual-Specificity Phosphatase Is Required for S-Phase Entry in Human Cells

机译:S相需要功能性cdc25C双特异性磷酸酶 进入人体细胞

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摘要

In view of the common regulatory mechanism that induces transcription of the mitotic phosphatase cdc25C and cyclin A at the beginning of S-phase, we investigated whether cdc25C was required for S-phase transit. Here, we show that in both nontransformed human fibroblasts and HeLa cells, cdc25C protein levels significantly increased concomitant with S-phase onset and cyclin A synthesis. Activity measurements on immunoprecipitates from synchronized HeLa cells revealed a sharp rise in cdc25C-associated phosphatase activity that coincided with S-phase. Microinjection of various antisense-cdc25C molecules led to inhibition of DNA synthesis in both HeLa cells and human fibroblasts. Furthermore, transfection of small interfering RNA directed against cdc25C specifically depleted cdc25C in HeLa cells without affecting cdc25A or cdc25B levels. Cdc25C RNA interference was also accompanied by S-phase inhibition. In cells depleted of cdc25C by antisense or siRNA, normal cell cycle progression could be re-established through microinjection of wild-type cdc25C protein but not inactive C377S mutant protein. Taken together, these results show that cdc25C not only plays a role at the G2/M transition but also in the modulation of DNA replication where its function is distinct from that of cdc25A.
机译:鉴于在S期开始时诱导有丝分裂磷酸酶cdc25C和细胞周期蛋白A转录的常见调控机制,我们研究了S期转运是否需要cdc25C。在这里,我们显示在未转化的人类成纤维细胞和HeLa细胞中,cdc25C蛋白水平与S期发作和细胞周期蛋白A合成显着增加。对同步化的HeLa细胞的免疫沉淀物的活性测量表明,与S期一致的cdc25C相关磷酸酶活性急剧上升。显微注射各种反义-cdc25C分子可抑制HeLa细胞和人类成纤维细胞中DNA的合成。此外,针对cdc25C的小干扰RNA的转染可在HeLa细胞中特异性消耗cdc25C,而不会影响cdc25A或cdc25B的水平。 Cdc25C RNA干扰还伴有S期抑制。在通过反义或siRNA耗尽了cdc25C的细胞中,可以通过显微注射野生型cdc25C蛋白而不是灭活的C377S突变蛋白来重新建立正常的细胞周期进程。综上所述,这些结果表明,cdc25C不仅在G2 / M过渡中起作用,而且还在DNA复制的调节中起作用,其功能不同于cdc25A。

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