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Late assembly of the Vibrio cholerae cell division machinery postpones septation to the last 10 of the cell cycle

机译:霍乱弧菌细胞分裂机制的后期组装将分离推迟到细胞周期的最后10%

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摘要

Bacterial cell division is a highly regulated process, which involves the formation of a complex apparatus, the divisome, by over a dozen proteins. In the few model bacteria in which the division process was detailed, divisome assembly occurs in two distinct steps: a few proteins, including the FtsZ tubulin-like protein, form a membrane associated contractile ring, the Z-ring, at ~30% of the cell cycle. The Z-ring serves as a scaffold for the recruitment of a second series of proteins, including integral membrane and periplasmic cell wall remodelling enzymes, at ~50% of the cell cycle. Actual septation occupies most of the remaining half of the cell cycle. In contrast, we present evidence suggesting that early pre-divisional Z-rings form between 40 and 50% of the cell cycle and mature into fully assembled divisome at about 80% of the cell cycle in Vibrio cholerae. Thus, actual septation is restricted to a very short amount of time. Our results further suggest that late assembly of the divisome probably helps maintain the asymmetric polar organisation of V. cholerae cells by limiting the accumulation of a cell pole marker, HubP, at the nascent cell poles.
机译:细菌细胞分裂是一个高度调控的过程,涉及由十几种蛋白质形成复杂的装置,即分裂体。在详细描述分裂过程的少数模型细菌中,分裂体的组装分两个不同的步骤进行:一些蛋白质(包括FtsZ微管蛋白样蛋白质)形成膜相关的收缩环,即Z环,占大约30%。细胞周期。 Z环充当支架,用于在细胞周期的〜50%时募集第二系列蛋白质,包括整合膜和周质细胞壁重塑酶。实际分隔占据了细胞周期剩余的大部分时间。相比之下,我们提供的证据表明,早期的除法Z形环在霍乱弧菌中约占细胞周期的40%至50%,并在约80%的细胞周期中成熟为完全组装的小体。因此,实际分隔只限于很短的时间。我们的研究结果进一步表明,通过限制新生体细胞极处细胞极标志物HubP的积累,divisome的后期组装可能有助于维持霍乱弧菌细胞的不对称极性组织。

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