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Mei4p coordinates the onset of meiosis I by regulating cdc25+ in fission yeast

机译:Mei4p通过调节裂变酵母中的cdc25 +来协调减数分裂I的发作

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摘要

The kinase Cdc2p is a central regulator of entry into and progression through nuclear division during mitosis and meiosis in eukaryotes. Cdc2p is activated at the onset of mitosis by dephosphorylation on tyrosine-15, the phosphorylation status of which is determined mainly by the kinase Wee1p and the phosphatase Cdc25p. In fission yeast, the forkhead-type transcription factor Mei4p is required for expression of many genes during meiosis, with mei4 mutant cells arresting before meiosis I. The mechanism of cell cycle arrest in mei4 cells has remained unknown, however. We now show that cdc25+ is an important target of Mei4p in control of entry into meiosis I. Forced dephosphorylation of Cdc2p on tyrosine-15 thus induced meiosis I in mei4 mutant cells without a delay, although no spores were formed. We propose that Mei4p acts as a rate-limiting regulator of meiosis I by activating cdc25+ transcription in coordination with other meiotic events.
机译:Cdc2p激酶是真核生物有丝分裂和减数分裂过程中核分裂进入和通过核分裂的中央调节剂。 Cdc2p在有丝分裂开始时通过酪氨酸15上的去磷酸化被激活,酪氨酸15的磷酸化状态主要由激酶Wee1p和磷酸酶Cdc25p决定。在裂变酵母中,在减数分裂过程中许多基因的表达都需要叉头型转录因子Mei4p,在减数分裂I之前mei4突变细胞会被阻滞。然而,在mei4细胞中细胞周期阻滞的机制仍然未知。现在我们显示,cdc25 +是控制进入减数分裂I的Mei4p的重要靶点。在酪氨酸15上强制Cdc2p的去磷酸化可在mei4突变细胞中立即诱导减数分裂I,尽管没有孢子形成。我们建议Mei4p通过激活cdc25 +转录与其他减数分裂事件的协调作用,作为减数分裂I的限速调节剂。

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