BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Liver, Anticancer prodrugs, Lipitor, rs6983267, FGF21, Coagulation, Diabetes mellitus)
Bookmark Forward

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

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

The Journal of biological chemistry 2018 Feb 02


filter terms:
  • amino acids (1)
  • cell cycle (2)
  • cell membrane (1)
  • escherichia coli (4)
  • FtsB (2)
  • ftsb protein, e coli (1)
  • FtsL (4)
  • ftsl protein, e coli (1)
  • FtsQ (1)
  • hydrogen bonds (1)
  • models molecular (1)
  • multiprotein complexes (2)
  • peptidoglycan (1)
  • periplasm (1)
  • protein e coli (2)
  • signal (1)
  • subunits (2)
  • tetramer (2)
    • Sizes of these terms reflect their relevance to your search.

    In Escherichia coli, FtsLB plays a central role in the initiation of cell division, possibly transducing a signal that will eventually lead to the activation of peptidoglycan remodeling at the forming septum. The molecular mechanisms by which FtsLB operates in the divisome, however, are not understood. Here, we present a structural analysis of the FtsLB complex, performed with biophysical, computational, and in vivo methods, that establishes the organization of the transmembrane region and proximal coiled coil of the complex. FRET analysis in vitro is consistent with formation of a tetramer composed of two FtsL and two FtsB subunits. We predicted subunit contacts through co-evolutionary analysis and used them to compute a structural model of the complex. The transmembrane region of FtsLB is stabilized by hydrophobic packing and by a complex network of hydrogen bonds. The coiled coil domain probably terminates near the critical constriction control domain, which might correspond to a structural transition. The presence of strongly polar amino acids within the core of the tetrameric coiled coil suggests that the coil may split into two independent FtsQ-binding domains. The helix of FtsB is interrupted between the transmembrane and coiled coil regions by a flexible Gly-rich linker. Conversely, the data suggest that FtsL forms an uninterrupted helix across the two regions and that the integrity of this helix is indispensable for the function of the complex. The FtsL helix is thus a candidate for acting as a potential mechanical connection to communicate conformational changes between periplasmic, membrane, and cytoplasmic regions. © 2018 by The American Society for Biochemistry and Molecular Biology, Inc.

    Citation

    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. The FtsLB subcomplex of the bacterial divisome is a tetramer with an uninterrupted FtsL helix linking the transmembrane and periplasmic regions. The Journal of biological chemistry. 2018 Feb 02;293(5):1623-1641

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 29233891

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.