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Influence of FtsZ GTPase activity and concentration on nanoscale Z-ring structure in vivo revealed by three-dimensional superresolution imaging

机译:三维超分辨率成像揭示FtsZ GTPase活性和浓度对体内纳米Z环结构的影响

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摘要

FtsZ is an essential bacterial cytoskeletal protein that assembles into a ring-like structure (Z-ring) at midcell to carry out cytokinesis. In vitro, FtsZ exhibits polymorphism in polymerizing into different forms of filaments based on its GTPase activity, concentration, and buffer condition. In vivo, the Z-ring appeared to be punctate and heterogeneously organized, although continuous, homogenous Z-ring structures have also been observed. Understanding how the Z-ring is organized in vivo is important because it provides a structural basis for the functional role of the Z-ring in cytokinesis. Here, we assess the effects of both GTPase activity and FtsZ concentration on the organization of the Z-ring in vivo using three-dimensional (3D) superresolution microscopy. We found that the Z-ring became more homogenous when assembled in the presence of a GTPase-deficient mutant, and upon overexpression of either wt or mutant FtsZ. These results suggest that the in vivo organization of the Z-ring is largely dependent on the intrinsic polymerization properties of FtsZ, which are significantly influenced by the GTPase activity and concentration of FtsZ. Our work provides a unifying theme to reconcile previous observations of different Z-ring structures, and supports a model in which the wt Z-ring comprises loosely associated, heterogeneously distributed FtsZ clusters.
机译:FtsZ是必不可少的细菌细胞骨架蛋白,在中层细胞组装成环状结构(Z环)以进行胞质分裂。在体外,基于其GTPase活性,浓度和缓冲条件,FtsZ在聚合成不同形式的长丝时表现出多态性。在体内,尽管还观察到了连续的,均匀的Z形环结构,但Z形环似乎是点状和异质组织的。了解Z环在体内的组织方式非常重要,因为它为Z环在胞质分裂中的功能作用提供了结构基础。在这里,我们使用三维(3D)超分辨率显微镜评估GTPase活性和FtsZ浓度对体内Z环组织的影响。我们发现,在存在GTPase缺陷型突变体的情况下,以及在wt或突变体FtsZ过表达时,Z环变得更加均质。这些结果表明,Z环的体内组织在很大程度上取决于FtsZ的固有聚合特性,该特性受GTPase活性和FtsZ浓度的显着影响。我们的工作提供了统一的主题,以调和先前对不同Z形环结构的观察结果,并支持其中wt Z形环包括松散关联的,异构分布的FtsZ簇的模型。

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