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通过细菌形态发生蛋白 MreB 和 MreD 定位细胞壁合成复合物。

Positioning cell wall synthetic complexes by the bacterial morphogenetic proteins MreB and MreD.

机构信息

Department of Chemistry and Biochemistry, and Molecular Biology Institute, University of California, Los Angeles, CA 90095-1569, USA.

出版信息

Mol Microbiol. 2010 May;76(3):616-33. doi: 10.1111/j.1365-2958.2010.07108.x. Epub 2010 Mar 10.

DOI:10.1111/j.1365-2958.2010.07108.x
PMID:20233306
Abstract

In Caulobacter crescentus, intact cables of the actin homologue, MreB, are required for the proper spatial positioning of MurG which catalyses the final step in peptidoglycan precursor synthesis. Similarly, in the periplasm, MreC controls the spatial orientation of the penicillin binding proteins and a lytic transglycosylase. We have now found that MreB cables are required for the organization of several other cytosolic murein biosynthetic enzymes such as MraY, MurB, MurC, MurE and MurF. We also show these proteins adopt a subcellular pattern of localization comparable to MurG, suggesting the existence of cytoskeletal-dependent interactions. Through extensive two-hybrid analyses, we have now generated a comprehensive interaction map of components of the bacterial morphogenetic complex. In the cytosol, this complex contains both murein biosynthetic enzymes and morphogenetic proteins, including RodA, RodZ and MreD. We show that the integral membrane protein, MreD, is essential for lateral peptidoglycan synthesis, interacts with the precursor synthesizing enzymes MurG and MraY, and additionally, determines MreB localization. Our results suggest that the interdependent localization of MreB and MreD functions to spatially organize a complex of peptidoglycan precursor synthesis proteins, which is required for propagation of a uniform cell shape and catalytically efficient peptidoglycan synthesis.

摘要

在新月柄杆菌中,肌动蛋白同源物 MreB 的完整电缆对于催化肽聚糖前体合成最后一步的 MurG 的正确空间定位是必需的。同样,在周质中,MreC 控制青霉素结合蛋白和溶菌转糖基酶的空间定向。我们现在发现 MreB 电缆对于其他几种细胞质 murein 生物合成酶的组织是必需的,例如 MraY、MurB、MurC、MurE 和 MurF。我们还表明这些蛋白质采用类似于 MurG 的亚细胞定位模式,表明存在细胞骨架依赖性相互作用。通过广泛的双杂交分析,我们现在生成了细菌形态发生复合物成分的综合相互作用图谱。在细胞质中,该复合物包含 murein 生物合成酶和形态发生蛋白,包括 RodA、RodZ 和 MreD。我们表明,完整膜蛋白 MreD 对于侧肽聚糖合成是必需的,与前体合成酶 MurG 和 MraY 相互作用,此外,还决定了 MreB 的定位。我们的结果表明,MreB 和 MreD 功能的相互依赖的定位有助于空间组织肽聚糖前体合成蛋白的复合物,这对于传播均匀的细胞形状和催化有效的肽聚糖合成是必需的。

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