首页> 美国卫生研究院文献>Journal of Bacteriology >MinDE-Dependent Pole-to-Pole Oscillation of Division Inhibitor MinC in Escherichia coli
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MinDE-Dependent Pole-to-Pole Oscillation of Division Inhibitor MinC in Escherichia coli

机译:MinDE依赖的分裂抑制剂MinC在大肠杆菌中的点对点振荡。

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摘要

By inhibiting FtsZ ring formation near the cell ends, the MinC protein plays a critical role in proper positioning of the division apparatus in Escherichia coli. MinC activity requires that of MinD, and the MinE peptide provides topological specificity by suppressing MinC-MinD-mediated division inhibition specifically at the middle of the cell. We recently presented evidence that MinE not only accumulates in an FtsZ-independent ring structure at the cell’s middle but also imposes a unique dynamic localization pattern upon MinD in which the latter accumulates alternately in either one of the cell halves in what appears to be a rapidly oscillating membrane association-dissociation cycle. Here we show that functional green fluorescent protein-MinC displays a very similar oscillatory behavior which is dependent on both MinD and MinE and independent of FtsZ. The results support a model in which MinD recruits MinC to its site of action and in which FtsZ ring assembly at each of the cell ends is blocked in an intermittent and alternate fashion.
机译:通过抑制细胞末端附近的FtsZ环形成,MinC蛋白在大肠杆菌中分裂装置的正确定位中起着关键作用。 MinC活性需要MinD的活性,而MinE肽通过特异性抑制MinC-MinD介导的分裂抑制在细胞中间提供拓扑特异性。我们最近提出的证据表明,MinE不仅在细胞中间以FtsZ独立的环结构积累,而且在MinD上施加了独特的动态定位模式,后者在每个细胞半部中交替出现,似乎是快速的。振动膜缔合-解离循环。在这里,我们显示功能性绿色荧光蛋白MinC表现出非常相似的振荡行为,这既取决于MinD和MinE,又取决于FtsZ。结果支持一个模型,其中MinD将MinC募集到其作用部位,并且其中每个单元末端的FtsZ环组件以间歇性和交替方式被阻止。

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