Literature DB >> 22753055

Synthetic motility and cell shape defects associated with deletions of flotillin/reggie paralogs in Bacillus subtilis and interplay of these proteins with NfeD proteins.

Felix Dempwolff1, Heiko M Möller, Peter L Graumann.   

Abstract

Flotillin/reggie proteins are membrane-associated proteins present in all kinds of cells and belong to the family of proteins carrying the SPFH (stomatin, prohibitin, flotillin, and HflK/HflC) domain. In addition to this domain of unknown function, flotillin proteins are characterized by the flotillin domain, which is rich in heptad repeats. Bacterial flotillin orthologs have recently been shown to be part of lipid rafts, like their eukaryotic counterparts, and to be involved in signaling events. Double deletions of floT and the gene encoding the second flotillin-like protein in Bacillus subtilis, floA, show strong synthetic defects in cell morphology, motility, and transformation efficiency. The lack of FloT resulted in a marked defect in motility. Using total internal reflection fluorescence (TIRF) microscopy, we show that both proteins localize in characteristic focal structures within the cell membrane, which move in a highly dynamic and random manner but localize independently of each other. Thus, flotillin paralogs act in a spatially distinct manner. Flotillin domains in both FloA and FloT are essential for focal assemblies and for the proper function of flotillins. Both flotillin genes are situated next to genes encoding NfeD proteins. FloT dramatically affects the localization of NfeD2: FloT apparently recruits NfeD2 into the focal assemblies, documenting a close interaction between flotillins and NfeDs in bacteria. In contrast, the localization of NfeD1b is not affected by FloA, FloT, or NfeD2. FloA does not show a spatial connection with the upstream-encoded NfeD1b (YqeZ). Our work establishes that bacterial flotillin-like proteins have overlapping functions in a variety of membrane-associated processes and that flotillin domain-mediated assembly and NfeD proteins play important roles in setting up the flotillin raft-like structures in vivo.

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Year:  2012        PMID: 22753055      PMCID: PMC3415494          DOI: 10.1128/JB.00910-12

Source DB:  PubMed          Journal:  J Bacteriol        ISSN: 0021-9193            Impact factor:   3.490


  28 in total

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Review 5.  Dissecting the molecular function of reggie/flotillin proteins.

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Review 7.  Scaffolding microdomains and beyond: the function of reggie/flotillin proteins.

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Journal:  Cell Mol Life Sci       Date:  2005-10       Impact factor: 9.261

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Review 9.  Lipid domains in bacterial membranes.

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  24 in total

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Review 2.  Functional Membrane Microdomains Organize Signaling Networks in Bacteria.

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Journal:  J Membr Biol       Date:  2016-08-26       Impact factor: 1.843

Review 3.  Imaging Bacterial Cell Wall Biosynthesis.

Authors:  Atanas D Radkov; Yen-Pang Hsu; Garrett Booher; Michael S VanNieuwenhze
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Review 5.  Exploring functional membrane microdomains in bacteria: an overview.

Authors:  Daniel Lopez; Gudrun Koch
Journal:  Curr Opin Microbiol       Date:  2017-02-23       Impact factor: 7.934

6.  Attenuating Staphylococcus aureus Virulence by Targeting Flotillin Protein Scaffold Activity.

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7.  Exploring the existence of lipid rafts in bacteria.

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8.  In vivo characterization of the scaffold activity of flotillin on the membrane kinase KinC of Bacillus subtilis.

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9.  The deletion of bacterial dynamin and flotillin genes results in pleiotrophic effects on cell division, cell growth and in cell shape maintenance.

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