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多染色体霍乱弧菌中的细胞分裂许可。

Cell division licensing in the multi-chromosomal Vibrio cholerae bacterium.

机构信息

Institute for Integrative Biology of the Cell (I2BC), Université Paris-Saclay, CEA, CNRS, Université Paris Sud, 1 avenue de la Terrasse, 91198 Gif sur Yvette, France.

出版信息

Nat Microbiol. 2016 Jun 27;1(9):16094. doi: 10.1038/nmicrobiol.2016.94.

Abstract

Cell division must be coordinated with chromosome replication and segregation to ensure the faithful transmission of genetic information during proliferation. In most bacteria, assembly of the division apparatus, the divisome, starts with the polymerization of a tubulin homologue, FtsZ, into a ring-like structure at mid-cell, the Z-ring(1). It typically occurs at half of the cell cycle when most of the replication and segregation cycle of the unique chromosome they generally harbour is achieved(2). The chromosome itself participates in the regulation of cell division, at least in part because it serves as a scaffold to position FtsZ polymerization antagonists(3). However, about 10% of bacteria have more than one chromosome(4), which raises questions about the way they license cell division(3). For instance, the genome of Vibrio cholerae, the agent of cholera, is divided between a 3 Mbp replicon that originates from the chromosome of its mono-chromosomal ancestor, Chr1, and a 1 Mbp plasmid-derived replicon, Chr2 (ref. 5). Here, we show that Chr2 harbours binding motifs for an inhibitor of Z-ring formation, which helps accurately position the V. cholerae divisome at mid-cell and postpones its assembly to the very end of the cell cycle.

摘要

细胞分裂必须与染色体复制和分离相协调,以确保在增殖过程中遗传信息的忠实传递。在大多数细菌中,分裂装置的组装,即分裂体,始于微管同源物 FtsZ 的聚合,在细胞中部形成一个类似环的结构,即 Z 环(1)。当它们通常携带的独特染色体的大部分复制和分离周期完成一半时,它通常发生在细胞周期的一半时(2)。染色体本身参与细胞分裂的调节,至少部分原因是它作为 FtsZ 聚合拮抗剂的支架(3)。然而,大约 10%的细菌有不止一个染色体(4),这就提出了它们如何许可细胞分裂的问题(3)。例如,霍乱弧菌的基因组,霍乱的病原体,分为起源于其单染色体祖先 Chr1 的 3 Mbp 复制子和 1 Mbp 质粒衍生的复制子 Chr2(参考 5)。在这里,我们表明 Chr2 含有 Z 环形成抑制剂的结合基序,这有助于准确地将霍乱弧菌的分裂体定位在细胞中部,并将其组装推迟到细胞周期的最后。

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