| Literature DB >> 28438890 |
Qing Yao1, Andrew I Jewett1, Yi-Wei Chang1, Catherine M Oikonomou1, Morgan Beeby1, Cristina V Iancu1, Ariane Briegel1, Debnath Ghosal1, Grant J Jensen2,3.
Abstract
FtsZ, the bacterial homologue of eukaryotic tubulin, plays a central role in cell division in nearly all bacteria and many archaea. It forms filaments under the cytoplasmic membrane at the division site where, together with other proteins it recruits, it drives peptidoglycan synthesis and constricts the cell. Despite extensive study, the arrangement of FtsZ filaments and their role in division continue to be debated. Here, we apply electron cryotomography to image the native structure of intact dividing cells and show that constriction in a variety of Gram-negative bacterial cells, including Proteus mirabilis and Caulobacter crescentus, initiates asymmetrically, accompanied by asymmetric peptidoglycan incorporation and short FtsZ-like filament formation. These results show that a complete ring of FtsZ is not required for constriction and lead us to propose a model for FtsZ-driven division in which short dynamic FtsZ filaments can drive initial peptidoglycan synthesis and envelope constriction at the onset of cytokinesis, later increasing in length and number to encircle the division plane and complete constriction.Entities:
Keywords: zzm321990Caulobacter crescentuszzm321990; FtsZ; asymmetric division; bacterial cell division; electron cryotomography
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Year: 2017 PMID: 28438890 PMCID: PMC5452018 DOI: 10.15252/embj.201696235
Source DB: PubMed Journal: EMBO J ISSN: 0261-4189 Impact factor: 11.598