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Coarse-grained simulations of bacterial cell wall growth reveal that local coordination alone can be sufficient to maintain rod shape

机译:细菌细胞壁生长的粗粒度模拟显示,仅局部协调就足以维持棒状

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摘要

Bacteria are surrounded by a peptidoglycan (PG) cell wall that must be remodeled to allow cell growth. While many structural details and properties of PG and the individual enzymes involved are known, how the process is coordinated to maintain cell integrity and rod shape is not understood. We have developed a coarse-grained method to simulate how individual transglycosylases, transpeptidases, and endopeptidases could introduce new material into an existing unilayer PG network. We find that a simple model with no enzyme coordination fails to maintain cell wall integrity and rod shape. We then iteratively analyze failure modes and explore different mechanistic hypotheses about how each problem might be overcome by the macromolecules involved. In contrast to a current theory, which posits that long MreB filaments are needed to coordinate PG insertion sites, we find that local coordination of enzyme activities in individual complexes can be sufficient to maintain cell integrity and rod shape. We also present possible molecular explanations for the existence of monofunctional transpeptidases and glycosidases (glycoside hydrolases), trimeric peptide crosslinks, cell twisting during growth, and synthesis of new strands in pairs.
机译:细菌被肽聚糖(PG)细胞壁包围,必须对其进行改造才能使细胞生长。虽然已知PG的许多结构细节和性质以及所涉及的各个酶,但是如何协调该过程以维持细胞完整性和棒状仍是未知的。我们已经开发出一种粗粒度方法来模拟单个转糖基酶,转肽酶和内肽酶如何将新材料引入现有的单层PG网络中。我们发现没有酶配位的简单模型无法维持细胞壁完整性和棒状。然后,我们迭代分析故障模式,并探索有关所涉及的大分子如何解决每个问题的不同机制假设。与当前的理论相反,当前的理论认为需要较长的MreB细丝来协调PG的插入位点,我们发现单个复合物中酶活性的局部协调足以维持细胞的完整性和棒状。我们还为单功能转肽酶和糖苷酶(糖苷水解酶),三聚体肽交联,生长过程中的细胞扭曲以及成对合成新链的存在提供了可能的分子解释。

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