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Staphylococcus aureus DivIB is a peptidoglycan-binding protein that is required for a morphological checkpoint in cell division

机译:金黄色葡萄球菌DivIB是一种肽聚糖结合蛋白,是细胞分裂形态学检查点所必需的

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摘要

Bacterial cell division is a fundamental process that requires the coordinated actions of a number of proteins which form a complex macromolecular machine known as the divisome. The membrane-spanning proteins DivIB and its orthologue FtsQ are crucial divisome components in Gram-positive and Gram-negative bacteria respectively. However, the role of almost all of the integral division proteins, including DivIB, still remains largely unknown. Here we show that the extracellular domain of DivIB is able to bind peptidoglycan and have mapped the binding to its β subdomain. Conditional mutational studies show that divIB is essential for Staphylococcus aureus growth, while phenotypic analyses following depletion of DivIB results in a block in the completion, but not initiation, of septum formation. Localisation studies suggest that DivIB only transiently localises to the division site and may mark previous sites of septation. We propose that DivIB is required for a molecular checkpoint during division to ensure the correct assembly of the divisome at midcell and to prevent hydrolytic growth of the cell in the absence of a completed septum.
机译:细菌细胞分裂是一个基本过程,需要许多蛋白质的协同作用,这些蛋白质形成称为“小分子”的复杂大分子机器。跨膜蛋白DivIB及其直向同源物FtsQ分别是革兰氏阳性细菌和革兰氏阴性细菌中至关重要的divisome成分。但是,包括DivIB在内的几乎所有整合分裂蛋白的作用仍然很大程度上未知。在这里,我们显示了DivIB的胞外域能够结合肽聚糖,并将结合映射到其β亚域。有条件的突变研究表明,divIB对于金黄色葡萄球菌的生长至关重要,而DivIB耗尽后的表型分析导致中隔形成的完成而不是启动。本地化研究表明,DivIB仅短暂地定位于分裂位点,并且可能标志着先前的分隔位点。我们建议,在分裂过程中,分子检查点需要DivIB,以确保在中层细胞中正确组装divisome,并在没有完整的隔膜的情况下防止细胞的水解生长。

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