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耻垢分枝杆菌 ParA 与细胞周期协调染色体分离,并与极性生长决定因子 DivIVA 相互作用。

ParA of Mycobacterium smegmatis co-ordinates chromosome segregation with the cell cycle and interacts with the polar growth determinant DivIVA.

机构信息

Faculty of Biotechnology, University of Wrocław, Wrocław, Poland.

出版信息

Mol Microbiol. 2013 Mar;87(5):998-1012. doi: 10.1111/mmi.12146. Epub 2013 Jan 28.

Abstract

Mycobacteria are among the clinically most important pathogens, but still not much is known about the mechanisms of their cell cycle control. Previous studies suggested that the genes encoding ParA and ParB (ATPase and DNA binding protein, respectively, required for active chromosome segregation) may be essential in Mycobacterium tuberculosis. Further research has demonstrated that a Mycobacterium smegmatis parB deletion mutant was viable but exhibited a chromosome segregation defect. Here, we address the question if ParA is required for the growth of M. smegmatis, and which cell cycle processes it affects. Our data show that parA may be deleted, but its deletion leads to growth inhibition and severe disturbances of chromosome segregation and septum positioning. Similar defects are also caused by ParA overproduction. EGFP-ParA localizes as pole-associated complexes connected with a patch of fluorescence accompanying two ParB complexes. Observed aberrations in the number and positioning of ParB complexes in the parA deletion mutant indicate that ParA is required for the proper localization of the ParB complexes. Furthermore, it is shown that ParA colocalizes and interacts with the polar growth determinant Wag31 (DivIVA homologue). Our results demonstrate that mycobacterial ParA mediates chromosome segregation and co-ordinates it with cell division and elongation.

摘要

分枝杆菌是临床最重要的病原体之一,但人们对其细胞周期控制机制仍知之甚少。先前的研究表明,编码 ParA 和 ParB(分别为活性染色体分离所需的 ATP 酶和 DNA 结合蛋白)的基因可能是结核分枝杆菌所必需的。进一步的研究表明,分枝杆菌 smegmatis parB 缺失突变体是有活力的,但表现出染色体分离缺陷。在这里,我们探讨了 ParA 是否是分枝杆菌生长所必需的,以及它影响哪些细胞周期过程。我们的数据表明,parA 可以缺失,但缺失会导致生长抑制和染色体分离以及隔膜定位的严重紊乱。ParA 的过表达也会导致类似的缺陷。EGFP-ParA 作为与伴随两个 ParB 复合物的荧光斑点相连的极相关复合物定位。在 parA 缺失突变体中观察到 ParB 复合物数量和定位的异常表明,ParA 是 ParB 复合物正确定位所必需的。此外,还表明 ParA 与极性生长决定因子 Wag31(DivIVA 同源物)共定位并相互作用。我们的结果表明,分枝杆菌 ParA 介导染色体分离,并与细胞分裂和伸长相协调。

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