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FtsZ环在min和分区突变体中的聚集:Min系统和类核在调节FtsZ环定位中的作用。

FtsZ ring clusters in min and partition mutants: role of both the Min system and the nucleoid in regulating FtsZ ring localization.

作者信息

Yu X C, Margolin W

机构信息

Department of Microbiology and Molecular Genetics, University of Texas Medical School, 6431 Fannin, Houston, TX 77030, USA.

出版信息

Mol Microbiol. 1999 Apr;32(2):315-26. doi: 10.1046/j.1365-2958.1999.01351.x.

Abstract

To understand further the role of the nucleoid and the min system in selection of the cell division site, we examined FtsZ localization in Escherichia coli cells lacking MinCDE and in parC mutants defective in chromosome segregation. More than one FtsZ ring was sometimes found in the gaps between nucleoids in min mutant filaments. These multiple FtsZ rings were more apparent in longer cells; double or triple rings were often found in the nucleoid-free gaps in ftsI min and ftsA min double mutant filaments. Introducing a parC mutation into the ftsA min double mutant allowed the nucleoid-free gaps to become significantly longer. These gaps often contained dramatic clusters of FtsZ rings. In contrast, filaments of the ftsA parC double mutant, which contained active MinCDE, assembled only one or two rings in most of the large nucleoid-free gaps. These results suggest that all positions along the cell length are competent for FtsZ ring assembly, not just sites at mid-cell or at the poles. Consistent with previous results, unsegregated nucleoids also correlated with a lack of FtsZ localization. A model is proposed in which both the inhibitory effect of the nucleoid and the regulation by MinCDE ensure that cells divide precisely at the midpoint.

摘要

为了进一步了解类核和min系统在细胞分裂位点选择中的作用,我们检测了缺乏MinCDE的大肠杆菌细胞以及染色体分离存在缺陷的parC突变体中FtsZ的定位情况。在min突变体细丝类核之间的间隙中,有时会发现不止一个FtsZ环。这些多个FtsZ环在较长的细胞中更为明显;在ftsI min和ftsA min双突变体细丝的无类核间隙中经常发现双环或三环。在ftsA min双突变体中引入parC突变会使无类核间隙显著变长。这些间隙中常常含有大量的FtsZ环簇。相比之下,含有活性MinCDE的ftsA parC双突变体细丝,在大多数大的无类核间隙中仅组装一两个环。这些结果表明,细胞长度上的所有位置都适合FtsZ环组装,而不仅仅是细胞中部或两极的位点。与之前的结果一致,未分离的类核也与FtsZ定位缺失相关。我们提出了一个模型,其中类核的抑制作用和MinCDE的调节作用共同确保细胞精确地在中点处分裂。

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