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MreB and MurG as scaffolds for the cytoplasmic steps of peptidoglycan biosynthesis

机译:MreB和MurG作为肽聚糖生物合成细胞质步骤的支架

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摘要

Peptidoglycan is a major determinant of cell shape in bacteria, and its biosynthesis involves the concerted action of cytoplasmic, membrane-associated and periplasmic enzymes. Within the cytoplasm, Mur enzymes catalyse the first steps leading to peptidoglycan precursor biosynthesis, and have been suggested as being part of a multicomponent complex that could also involve the transglycosylase MurG and the cytoskeletal protein MreB. In order to initialize the characterization of a potential Mur interaction network, we purified MurD, MurE, MurF, MurG and MreB from Thermotoga maritima and characterized their interactions using membrane blotting and surface plasmon resonance. MurD, MurE and MurF all recognize MurG and MreB, but not each other, while the two latter proteins interact. In addition, we solved the crystal structures of MurD, MurE and MurF, which indicate that their C-termini display high conformational flexibilities. The differences in Mur conformations could be important parameters for the stability of an intracytoplasmic murein biosynthesis complex.
机译:肽聚糖是细菌细胞形状的主要决定因素,其生物合成涉及细胞质,膜相关和周质酶的协同作用。在细胞质内,Mur酶催化着导致肽聚糖前体生物合成的第一步,并被认为是多组分复合物的一部分,该复合物也可能涉及转糖基化酶MurG和细胞骨架蛋白MreB。为了初始化潜在的Mur相互作用网络的表征,我们从滨海嗜热菌中纯化了MurD,MurE,MurF,MurG和MreB,并使用膜印迹和表面等离振子共振表征了它们的相互作用。 MurD,MurE和MurF都识别MurG和MreB,但不能互相识别,而后两个蛋白相互作用。此外,我们解析了MurD,MurE和MurF的晶体结构,这表明它们的C末端显示了高构象柔性。 Mur构象的差异可能是胞质内壁叶黄素生物合成复合物稳定性的重要参数。

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