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复杂阐述:理解减数分裂黏连蛋白动力学

Complex elaboration: making sense of meiotic cohesin dynamics.

作者信息

Rankin Susannah

机构信息

Program in Cell Cycle and Cancer Biology, Oklahoma Medical Research Foundation, OK, USA.

出版信息

FEBS J. 2015 Jul;282(13):2426-43. doi: 10.1111/febs.13301. Epub 2015 May 9.

DOI:10.1111/febs.13301
PMID:25895170
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4490075/
Abstract

In mitotically dividing cells, the cohesin complex tethers sister chromatids, the products of DNA replication, together from the time they are generated during S phase until anaphase. Cohesion between sister chromatids ensures accurate chromosome segregation, and promotes normal gene regulation and certain kinds of DNA repair. In somatic cells, the core cohesin complex is composed of four subunits: Smc1, Smc3, Rad21 and an SA subunit. During meiotic cell divisions meiosis-specific isoforms of several of the cohesin subunits are also expressed and incorporated into distinct meiotic cohesin complexes. The relative contributions of these meiosis-specific forms of cohesin to chromosome dynamics during meiotic progression have not been fully worked out. However, the localization of these proteins during chromosome pairing and synapsis, and their unique loss-of-function phenotypes, suggest non-overlapping roles in controlling meiotic chromosome behavior. Many of the proteins that regulate cohesin function during mitosis also appear to regulate cohesin during meiosis. Here we review how cohesin contributes to meiotic chromosome dynamics, and explore similarities and differences between cohesin regulation during the mitotic cell cycle and meiotic progression. A deeper understanding of the regulation and function of cohesin in meiosis will provide important new insights into how the cohesin complex is able to promote distinct kinds of chromosome interactions under diverse conditions.

摘要

在进行有丝分裂的细胞中,黏连蛋白复合体将姐妹染色单体(DNA复制的产物)从它们在S期产生之时起就拴在一起,直至后期。姐妹染色单体之间的黏连确保了染色体的准确分离,并促进正常的基因调控和某些类型的DNA修复。在体细胞中,核心黏连蛋白复合体由四个亚基组成:Smc1、Smc3、Rad21和一个SA亚基。在减数分裂细胞分裂过程中,几种黏连蛋白亚基的减数分裂特异性异构体也会表达并整合到不同的减数分裂黏连蛋白复合体中。这些减数分裂特异性形式的黏连蛋白在减数分裂进程中对染色体动态变化的相对贡献尚未完全明确。然而,这些蛋白质在染色体配对和联会过程中的定位,以及它们独特的功能丧失表型,表明它们在控制减数分裂染色体行为中发挥着不重叠的作用。许多在有丝分裂过程中调节黏连蛋白功能的蛋白质在减数分裂过程中似乎也发挥着调节作用。在这里,我们综述了黏连蛋白如何促进减数分裂染色体动态变化,并探讨了有丝分裂细胞周期和减数分裂进程中黏连蛋白调节的异同。对减数分裂中黏连蛋白的调节和功能有更深入的了解,将为黏连蛋白复合体如何在不同条件下促进不同类型的染色体相互作用提供重要的新见解。

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本文引用的文献

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Connecting by breaking and repairing: mechanisms of DNA strand exchange in meiotic recombination.通过断裂与修复实现连接:减数分裂重组中DNA链交换的机制
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Meiosis-specific cohesin component, Stag3 is essential for maintaining centromere chromatid cohesion, and required for DNA repair and synapsis between homologous chromosomes.减数分裂特异性黏连蛋白组分Stag3对于维持着丝粒染色单体黏连至关重要,并且是DNA修复以及同源染色体之间联会所必需的。
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