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杆状革兰氏阴性菌分裂周期中细胞表面的合成

Synthesis of the cell surface during the division cycle of rod-shaped, gram-negative bacteria.

作者信息

Cooper S

机构信息

Department of Microbiology and Immunology, University of Michigan Medical School, Ann Arbor 48109-0620.

出版信息

Microbiol Rev. 1991 Dec;55(4):649-74. doi: 10.1128/mr.55.4.649-674.1991.

Abstract

When the growth of the gram-negative bacterial cell wall is considered in relation to the synthesis of the other components of the cell, a new understanding of the pattern of wall synthesis emerges. Rather than a switch in synthesis between the side wall and pole, there is a partitioning of synthesis such that the volume of the cell increases exponentially and thus perfectly encloses the exponentially increasing cytoplasm. This allows the density of the cell to remain constant during the division cycle. This model is explored at both the cellular and molecular levels to give a unified description of wall synthesis which has the following components: (i) there is no demonstrable turnover of peptidoglycan during cell growth, (ii) the side wall grows by diffuse intercalation, (iii) pole synthesis starts by some mechanism and is preferentially synthesized compared with side wall, and (iv) the combined side wall and pole syntheses enclose the newly synthesized cytoplasm at a constant cell density. The central role of the surface stress model in wall growth is distinguished from, and preferred to, models that propose cell-cycle-specific signals as triggers of changes in the rate of wall synthesis. The actual rate of wall synthesis during the division cycle is neither exponential nor linear, but is close to exponential when compared with protein synthesis during the division cycle.

摘要

当将革兰氏阴性细菌细胞壁的生长与细胞其他成分的合成联系起来考虑时,就会出现对细胞壁合成模式的新认识。并非是在侧壁和极之间切换合成,而是存在一种合成的分配方式,使得细胞体积呈指数增长,从而完美地包裹住呈指数增长的细胞质。这使得细胞密度在分裂周期中保持恒定。在细胞和分子水平上对该模型进行了探讨,以给出对细胞壁合成的统一描述,其具有以下组成部分:(i)在细胞生长过程中,肽聚糖没有可证明的周转;(ii)侧壁通过扩散插入生长;(iii)极合成通过某种机制开始,并且与侧壁相比优先合成;(iv)侧壁和极的合成相结合,以恒定的细胞密度包裹新合成的细胞质。表面应力模型在细胞壁生长中的核心作用与那些提出细胞周期特异性信号作为细胞壁合成速率变化触发因素的模型不同,且更受青睐。在分裂周期中细胞壁合成的实际速率既不是指数型的也不是线性的,但与分裂周期中的蛋白质合成相比,接近指数型。

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