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Literature DB >> 26268537

MinC/MinD copolymers are not required for Min function.

Kyung-Tae Park¹, Shishen Du¹, Joe Lutkenhaus¹.

Abstract

In Escherichia coli, precise placement of the cytokinetic Z ring at midcell requires the concerted action of the three Min proteins. MinD activates MinC, an inhibitor of FtsZ, at least in part, by recruiting it to the membrane and targeting it to the Z ring, while MinE stimulates the MinD ATPase inducing an oscillation that directs MinC/MinD activity away from midcell. Recently, MinC and MinD were shown to form copolymers of alternating dimers of MinC and MinD, and it was suggested that these copolymers are the active form of MinC/MinD. Here, we use MinD mutants defective in binding MinC to generate heterodimers with wild-type MinD that are unable to form MinC/MinD copolymers. Similarly, MinC mutants defective in binding to MinD were used to generate heterodimers with wild-type MinC that are unable to form copolymers. Such heterodimers are active and in the case of MinC were shown to mediate spatial regulation of the Z ring demonstrating that MinC/MinD copolymer formation is not required. Our results are consistent with a model in which a membrane anchored MinC/MinD complex is targeted to the Z ring through the conserved carboxy tail of FtsZ leading to breakage of FtsZ filaments.

Entities: Chemical Gene Mutation Species

Mesh：

Substances：

Year: 2015 PMID： 26268537 PMCID： PMC4715711 DOI： 10.1111/mmi.13164

Source DB: PubMed Journal: Mol Microbiol ISSN： 0950-382X Impact factor: 3.501

63 in total

1. Pattern formation in Escherichia coli: a model for the pole-to-pole oscillations of Min proteins and the localization of the division site.

Authors: H Meinhardt; P A de Boer
Journal: Proc Natl Acad Sci U S A Date: 2001-12-04 Impact factor: 11.205

2. Targeting of (D)MinC/MinD and (D)MinC/DicB complexes to septal rings in Escherichia coli suggests a multistep mechanism for MinC-mediated destruction of nascent FtsZ rings.

Authors: Jay E Johnson; Laura L Lackner; Piet A J de Boer
Journal: J Bacteriol Date: 2002-06 Impact factor: 3.490

3. Bacterial mitosis: partitioning protein ParA oscillates in spiral-shaped structures and positions plasmids at mid-cell.

Authors: Gitte Ebersbach; Kenn Gerdes
Journal: Mol Microbiol Date: 2004-04 Impact factor: 3.501

4. Positioning of the MinE binding site on the MinD surface suggests a plausible mechanism for activation of the Escherichia coli MinD ATPase during division site selection.

Authors: Luyan Ma; Glenn F King; Lawrence Rothfield
Journal: Mol Microbiol Date: 2004-10 Impact factor: 3.501

5. A division inhibitor and a topological specificity factor coded for by the minicell locus determine proper placement of the division septum in E. coli.

Authors: P A de Boer; R E Crossley; L I Rothfield
Journal: Cell Date: 1989-02-24 Impact factor: 41.582

6. FtsZ ring structure associated with division in Escherichia coli.

Authors: E F Bi; J Lutkenhaus
Journal: Nature Date: 1991-11-14 Impact factor: 49.962

7. Conserved glycines in the C terminus of MinC proteins are implicated in their functionality as cell division inhibitors.

Authors: S Ramirez-Arcos; V Greco; H Douglas; D Tessier; D Fan; J Szeto; J Wang; J R Dillon
Journal: J Bacteriol Date: 2004-05 Impact factor: 3.490

8. Division site selection in Escherichia coli involves dynamic redistribution of Min proteins within coiled structures that extend between the two cell poles.

Authors: Yu-Ling Shih; Trung Le; Lawrence Rothfield
Journal: Proc Natl Acad Sci U S A Date: 2003-05-23 Impact factor: 11.205

9. ZipA is required for targeting of DMinC/DicB, but not DMinC/MinD, complexes to septal ring assemblies in Escherichia coli.

Authors: Jay E Johnson; Laura L Lackner; Cynthia A Hale; Piet A J de Boer
Journal: J Bacteriol Date: 2004-04 Impact factor: 3.490

10. Coordination of cell division and chromosome segregation by a nucleoid occlusion protein in Bacillus subtilis.

Authors: Ling Juan Wu; Jeff Errington
Journal: Cell Date: 2004-06-25 Impact factor: 41.582

7 in total

1. MinC N- and C-Domain Interactions Modulate FtsZ Assembly, Division Site Selection, and MinD-Dependent Oscillation in Escherichia coli.

Authors: Christopher J LaBreck; Joseph Conti; Marissa G Viola; Jodi L Camberg
Journal: J Bacteriol Date: 2019-01-28 Impact factor: 3.490

MinC/MinD copolymers are not required for Min function.

1. Pattern formation in Escherichia coli: a model for the pole-to-pole oscillations of Min proteins and the localization of the division site.

2. Targeting of (D)MinC/MinD and (D)MinC/DicB complexes to septal rings in Escherichia coli suggests a multistep mechanism for MinC-mediated destruction of nascent FtsZ rings.

3. Bacterial mitosis: partitioning protein ParA oscillates in spiral-shaped structures and positions plasmids at mid-cell.

4. Positioning of the MinE binding site on the MinD surface suggests a plausible mechanism for activation of the Escherichia coli MinD ATPase during division site selection.

5. A division inhibitor and a topological specificity factor coded for by the minicell locus determine proper placement of the division septum in E. coli.

6. FtsZ ring structure associated with division in Escherichia coli.

7. Conserved glycines in the C terminus of MinC proteins are implicated in their functionality as cell division inhibitors.

8. Division site selection in Escherichia coli involves dynamic redistribution of Min proteins within coiled structures that extend between the two cell poles.

9. ZipA is required for targeting of DMinC/DicB, but not DMinC/MinD, complexes to septal ring assemblies in Escherichia coli.

10. Coordination of cell division and chromosome segregation by a nucleoid occlusion protein in Bacillus subtilis.

1. MinC N- and C-Domain Interactions Modulate FtsZ Assembly, Division Site Selection, and MinD-Dependent Oscillation in Escherichia coli.

2. MinC and FtsZ mutant analysis provides insight into MinC/MinD-mediated Z ring disassembly.

3. The cell division protein MinD from Pseudomonas aeruginosa dominates the assembly of the MinC-MinD copolymers.

4. Characterization of C-terminal structure of MinC and its implication in evolution of bacterial cell division.

5. Cryo-EM structure of the MinCD copolymeric filament from Pseudomonas aeruginosa at 3.1 Å resolution.

Review 6. The E. coli MinCDE system in the regulation of protein patterns and gradients.

Review 7. Structural Insights into Protein-Protein Interactions Involved in Bacterial Cell Wall Biogenesis.