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大肠杆菌染色体二聚体解离过程中重组、细胞分裂与染色体结构之间的相互作用

Interplay between recombination, cell division and chromosome structure during chromosome dimer resolution in Escherichia coli.

作者信息

Pérals K, Capiaux H, Vincourt J B, Louarn J M, Sherratt D J, Cornet F

机构信息

Laboratoire de Microbiologie et de Génétique Moléculaire du CNRS, 118 route de Narbonne, 31062 Toulouse Cedex, France.

出版信息

Mol Microbiol. 2001 Feb;39(4):904-13. doi: 10.1046/j.1365-2958.2001.02277.x.

Abstract

Chromosome dimers form in bacteria by recombination between circular chromosomes. Resolution of dimers is a highly integrated process involving recombination between dif sites catalysed by the XerCD recombinase, cell division and the integrity of the division septum-associated FtsK protein and the presence of dif inside a restricted region of the chromosome terminus, the dif activity zone (DAZ). We analyse here how these phenomena collaborate. We show that (i) both inter- and intrachromosomal recombination between dif sites are activated by their presence inside the DAZ; (ii) the DAZ-specific activation only occurs in conditions supporting the formation of chromosome dimers; (iii) overexpression of FtsK leads to a general increase in dif recombination irrespective of dif location; (iv) overexpression of FtsK does not improve the ability of dif sites inserted outside the DAZ to resolve chromosome dimers. Our results suggest that the formation of an active XerCD-FtsK-dif complex is restricted to when a dimer is present, the features of chromosome organization that determine the DAZ playing a central role in this control.

摘要

染色体二聚体在细菌中通过环状染色体之间的重组形成。二聚体的拆分是一个高度整合的过程,涉及由XerCD重组酶催化的dif位点之间的重组、细胞分裂以及与分裂隔膜相关的FtsK蛋白的完整性,并且染色体末端的一个受限区域(即dif活性区,DAZ)内存在dif位点。我们在此分析这些现象是如何协同作用的。我们发现:(i)dif位点之间的染色体间和染色体内重组均因它们存在于DAZ内而被激活;(ii)DAZ特异性激活仅在支持染色体二聚体形成的条件下发生;(iii)FtsK的过表达导致dif重组普遍增加,而与dif的位置无关;(iv)FtsK的过表达并不能提高插入DAZ之外的dif位点拆分染色体二聚体的能力。我们的结果表明,活性XerCD-FtsK-dif复合物的形成仅限于存在二聚体时,决定DAZ的染色体组织特征在这种调控中起核心作用。

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