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Cdc25 and Wee1: analogous opposites?

机译:Cdc25和Wee1:类似的对立?

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Movement through the cell cycle is controlled by the temporally and spatially ordered activation of cyclin-dependent kinases paired with their respective cyclin binding partners. Cell cycle events occur in a stepwise fashion and are monitored by molecular surveillance systems to ensure that each cell cycle process is appropriately completed before subsequent events are initiated. Cells prevent entry into mitosis while DNA replication is ongoing, or if DNA is damaged, via checkpoint mechanisms that inhibit the activators and activate the inhibitors of mitosis, Cdc25 and Wee1, respectively. Once DNA replication has been faithfully completed, Cdc2/Cyclin B is swiftly activated for a timely transition from interphase into mitosis. This sharp transition is propagated through both positive and negative feedback loops that impinge upon Cdc25 and Wee1 to ensure that Cdc2/Cyclin B is fully activated. Recent reports from a number of laboratories have revealed a remarkably complex network of kinases and phosphatases that coordinately control Cdc25 and Wee1, thereby precisely regulating the transition into mitosis. Although not all factors that inhibit Cdc25 have been shown to activate Wee1 and vice versa, a number of regulatory modules are clearly shared in common. Thus, studies on either the Cdc25 or Wee1-regulatory arm of the mitotic control pathway should continue to shed light on how both arms are coordinated to smoothly regulate mitotic entry.
机译:在细胞周期中的运动受细胞周期蛋白依赖性激酶及其各自细胞周期蛋白结合伴侣配对的时间和空间有序激活的控制。细胞周期事件以逐步的方式发生,并由分子监视系统进行监视,以确保在随后的事件开始之前适当地完成每个细胞周期过程。当DNA复制正在进行或DNA受到破坏时,细胞通过抑制点机制分别阻止Cdc25和Wee1激活剂并激活有丝分裂的抑制剂来防止进入有丝分裂。一旦忠实地完成了DNA复制,Cdc2 / Cyclin B就会迅速激活,以便及时地从相间过渡到有丝分裂。这种尖锐的跃迁通过正向和负向反馈环路传播,这些环路撞击到Cdc25和Wee1,以确保Cdc2 / Cyclin B被完全激活。来自许多实验室的最新报告显示,激酶和磷酸酶的网络非常复杂,可以协调控制Cdc25和Wee1,从而精确调节向有丝分裂的转化。尽管并非所有抑制Cdc25的因素均已显示可激活Wee1,反之亦然,但显然许多监管模块是共有的。因此,对有丝分裂控制途径的Cdc25或Wee1调节臂的研究应继续阐明如何协调两个臂以平稳调节有丝分裂进入。

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