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尿路致病性大肠杆菌感染相关丝状体形成和分裂过程中 FtsZ 和 DamX 的组装动力学。

Assembly dynamics of FtsZ and DamX during infection-related filamentation and division in uropathogenic E. coli.

机构信息

Australian Institute for Microbiology and Infection, University of Technology Sydney, Sydney, 2007, NSW, Australia.

Department of Biochemistry and Biophysics, Stockholm University, Stockholm, 106 91, Sweden.

出版信息

Nat Commun. 2022 Jun 25;13(1):3648. doi: 10.1038/s41467-022-31378-1.

Abstract

During infection of bladder epithelial cells, uropathogenic Escherichia coli (UPEC) can stop dividing and grow into highly filamentous forms. Here, we find that some filaments of E. coli UTI89 released from infected cells grow very rapidly and by more than 100 μm before initiating division, whereas others do not survive, suggesting that infection-related filamentation (IRF) is a stress response that promotes bacterial dispersal. IRF is accompanied by unstable, dynamic repositioning of FtsZ division rings. In contrast, DamX, which is associated with normal cell division and is also essential for IRF, is distributed uniformly around the cell envelope during filamentation. When filaments initiate division to regenerate rod cells, DamX condenses into stable rings prior to division. The DamX rings maintain consistent thickness during constriction and remain at the septum until after membrane fusion. Deletion of damX affects vegetative cell division in UTI89 (but not in the model E. coli K-12), and, during infection, blocks filamentation and reduces bacterial cell integrity. IRF therefore involves DamX distribution throughout the membrane and prevention of FtsZ ring stabilization, leading to cell division arrest. DamX then reassembles into stable division rings for filament division, promoting dispersal and survival during infection.

摘要

在感染膀胱上皮细胞期间,尿路致病性大肠杆菌(UPEC)可以停止分裂并生长成高度丝状形式。在这里,我们发现从受感染细胞释放的一些 UTI89 大肠杆菌丝状体生长得非常迅速,在开始分裂之前超过 100μm,而其他丝状体则无法存活,这表明感染相关的丝状化(IRF)是一种促进细菌扩散的应激反应。IRF 伴随着 FtsZ 分裂环的不稳定、动态重定位。相比之下,与正常细胞分裂相关且对 IRF 也是必需的 DamX 在丝状化过程中均匀分布在细胞包膜周围。当丝状体开始分裂以再生杆状细胞时,DamX 在分裂前凝聚成稳定的环。DamX 环在收缩过程中保持一致的厚度,并在膜融合后仍保留在隔膜处。damX 的缺失会影响 UTI89 中的营养细胞分裂(但不会影响模型大肠杆菌 K-12),并且在感染期间,它会阻止丝状化并降低细菌细胞完整性。因此,IRF 涉及 DamX 在整个膜中的分布以及防止 FtsZ 环稳定化,从而导致细胞分裂停滞。然后,DamX 重新组装成稳定的分裂环,用于丝状体分裂,在感染期间促进分散和存活。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c971/9233674/6e6f59732703/41467_2022_31378_Fig1_HTML.jpg

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