Literature DB >> 23520975

Structural organization of FtsB, a transmembrane protein of the bacterial divisome.

Loren M LaPointe1, Keenan C Taylor, Sabareesh Subramaniam, Ambalika Khadria, Ivan Rayment, Alessandro Senes.   

Abstract

We report the first structural analysis of an integral membrane protein of the bacterial divisome. FtsB is a single-pass membrane protein with a periplasmic coiled coil. Its heterologous association with its partner FtsL represents an essential event for the recruitment of the late components to the division site. Using a combination of mutagenesis, computational modeling, and X-ray crystallography, we determined that FtsB self-associates, and we investigated its structural organization. We found that the transmembrane domain of FtsB homo-oligomerizes through an evolutionarily conserved interaction interface where a polar residue (Gln 16) plays a critical role through the formation of an interhelical hydrogen bond. The crystal structure of the periplasmic domain, solved as a fusion with Gp7, shows that 30 juxta-membrane amino acids of FtsB form a canonical coiled coil. The presence of conserved Gly residue in the linker region suggests that flexibility between the transmembrane and coiled coil domains is functionally important. We hypothesize that the transmembrane helices of FtsB form a stable dimeric core for its association with FtsL into a higher-order oligomer and that FtsL is required to stabilize the periplasmic domain of FtsB, leading to the formation of a complex that is competent for binding to FtsQ, and to their consequent recruitment to the divisome. The study provides an experimentally validated structural model and identifies point mutations that disrupt association, thereby establishing important groundwork for the functional characterization of FtsB in vivo.

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Year:  2013        PMID: 23520975      PMCID: PMC3702382          DOI: 10.1021/bi400222r

Source DB:  PubMed          Journal:  Biochemistry        ISSN: 0006-2960            Impact factor:   3.162


  77 in total

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3.  Evidence from artificial septal targeting and site-directed mutagenesis that residues in the extracytoplasmic β domain of DivIB mediate its interaction with the divisomal transpeptidase PBP 2B.

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Review 4.  Bacterial cell division: assembly, maintenance and disassembly of the Z ring.

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Journal:  Nat Rev Microbiol       Date:  2009-09       Impact factor: 60.633

5.  Multiple interaction domains in FtsL, a protein component of the widely conserved bacterial FtsLBQ cell division complex.

Authors:  Mark D Gonzalez; Esra A Akbay; Dana Boyd; Jon Beckwith
Journal:  J Bacteriol       Date:  2010-04-02       Impact factor: 3.490

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  17 in total

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2.  Fine-mapping the contact sites of the Escherichia coli cell division proteins FtsB and FtsL on the FtsQ protein.

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3.  The FtsLB subcomplex of the bacterial divisome is a tetramer with an uninterrupted FtsL helix linking the transmembrane and periplasmic regions.

Authors:  Samson G F Condon; Deena-Al Mahbuba; Claire R Armstrong; Gladys Diaz-Vazquez; Samuel J Craven; Loren M LaPointe; Ambalika S Khadria; Rahul Chadda; John A Crooks; Nambirajan Rangarajan; Douglas B Weibel; Aaron A Hoskins; Janice L Robertson; Qiang Cui; Alessandro Senes
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Review 4.  Fluorophores, environments, and quantification techniques in the analysis of transmembrane helix interaction using FRET.

Authors:  Ambalika S Khadria; Alessandro Senes
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5.  The Soluble Periplasmic Domains of Escherichia coli Cell Division Proteins FtsQ/FtsB/FtsL Form a Trimeric Complex with Submicromolar Affinity.

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Journal:  Biochemistry       Date:  2013-10-18       Impact factor: 3.162

10.  Lipid Binding Controls Dimerization of the Coat Protein p24 Transmembrane Helix.

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