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为细胞核膜破裂准备细胞:有丝分裂进入过程中磷酸化的时空控制。

Preparing a cell for nuclear envelope breakdown: Spatio-temporal control of phosphorylation during mitotic entry.

作者信息

Alvarez-Fernández Mónica, Malumbres Marcos

机构信息

Cell Division and Cancer Group, Spanish National Cancer Research Centre (CNIO), Madrid, Spain.

出版信息

Bioessays. 2014 Aug;36(8):757-65. doi: 10.1002/bies.201400040. Epub 2014 May 30.

Abstract

Chromosome segregation requires the ordered separation of the newly replicated chromosomes between the two daughter cells. In most cells, this requires nuclear envelope (NE) disassembly during mitotic entry and its reformation at mitotic exit. Nuclear envelope breakdown (NEB) results in the mixture of two cellular compartments. This process is controlled through phosphorylation of multiple targets by cyclin-dependent kinase 1 (Cdk1)-cyclin B complexes as well as other mitotic enzymes. Experimental evidence also suggests that nucleo-cytoplasmic transport of critical cell cycle regulators such as Cdk1-cyclin B complexes or Greatwall, a kinase responsible for the inactivation of PP2A phosphatases, plays a major role in maintaining the boost of mitotic phosphorylation thus preventing the potential mitotic collapse derived from NEB. These data suggest the relevance of nucleo-cytoplasmic transport not only to communicate cytoplasmic and nuclear compartments during interphase, but also to prepare cells for the mixture of these two compartments during mitosis.

摘要

染色体分离需要将新复制的染色体在两个子细胞之间有序分离。在大多数细胞中,这需要在有丝分裂开始时核膜(NE)解体,并在有丝分裂结束时重新形成。核膜破裂(NEB)导致两个细胞区室混合。这个过程通过细胞周期蛋白依赖性激酶1(Cdk1)-细胞周期蛋白B复合物以及其他有丝分裂酶对多个靶点的磷酸化来控制。实验证据还表明,关键细胞周期调节因子如Cdk1-细胞周期蛋白B复合物或负责使PP2A磷酸酶失活的激酶Greatwall的核质运输,在维持有丝分裂磷酸化增强从而防止NEB导致的潜在有丝分裂崩溃中起主要作用。这些数据表明核质运输不仅与间期细胞质和细胞核区室之间的通讯有关,而且与细胞在有丝分裂期间为这两个区室的混合做准备有关。

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