首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >PKN delays mitotic timing by inhibition of Cdc25C: Possible involvement of PKN in the regulation of cell division
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PKN delays mitotic timing by inhibition of Cdc25C: Possible involvement of PKN in the regulation of cell division

机译:PKN通过抑制Cdc25C延迟有丝分裂时间:PKN可能参与细胞分裂的调控

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摘要

The role of PKN, a fatty acid- and Rho small GTPase-activated protein kinase, in cell-cycle regulation was analyzed. Microinjec- tion of the active form of PKN into a Xenopus embryo caused cleavage arrest. whereas normal cell division proceeded in the control embryo microinjected with buffer or the inactive form of PKN. Exogenous addition of the active form of PKN delayed mitotic timing in Xenopus egg cycling extracts judging by morphology of sperm nuclei and Cdc2/cyclin B histone H1 kinase activity. The linase-negative form of PKN did not affect the timing, suggesting that delayed mitotic timing depends on the kinase activity of PKN. The dephosphorylation of Tyr-15 of Cdc2 was also delayed in correlation with Cdc2/cyclin B histone H1 kinase activation in extracts containing active PKN. The Cdc25C activity for the dephos- phorylation of Tyr-15 in Cdc2 was suppressed by pretreatment with the active form of PKN. Furthermore, PKN efficiently phos- phorylated Cdc25C in vitro, indicating that PKN directly inhibits Cdc25C activity by phosphorylation. These results suggest that PKN plays a significant role in the control of mitotic timing by inhibition 0f Cdc25C.
机译:分析了PKN(一种脂肪酸和Rho小GTPase激活的蛋白激酶)在细胞周期调控中的作用。将活性形式的PKN微注射入非洲爪蟾胚胎会导致卵裂停滞。而正常细胞分裂则是在对照胚胎中注入缓冲液或非活性形式的PKN后进行的。根据精子细胞核的形态和Cdc2 / cyclin B组蛋白H1激酶活性判断,外源添加PKN活性形式可延迟非洲爪蟾卵循环提取物中的有丝分裂时间。 PKN的负酶阴性形式不影响时间,提示有丝分裂时间的延迟取决于PKN的激酶活性。与含有活性PKN的提取物中的Cdc2 / cyclin B组蛋白H1激酶活化相关,Cdc2的Tyr-15的去磷酸化也被延迟。用活性形式的PKN预处理可抑制Cdc2C中Tyr-15脱磷酸的Cdc25C活性。此外,PKN在体外有效地磷酸化了Cdc25C,这表明PKN通过磷酸化直接抑制了Cdc25C的活性。这些结果表明PKN通过抑制0f Cdc25C在控制有丝分裂时机中起重要作用。

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