• Title of article

    Crystal Structure of the Resuscitation-Promoting Factor ΔDUFRpfB from M. tuberculosis

  • Author/Authors

    Alessia Ruggiero، نويسنده , , Barbara Tizzano، نويسنده , , Emilia Pedone، نويسنده , , Carlo Pedone، نويسنده , , Matthias Wilmanns، نويسنده , , Rita Berisio، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2009
  • Pages
    10
  • From page
    153
  • To page
    162
  • Abstract
    Mycobacterium tuberculosis is able to establish a non-replicating state and survive in an intracellular habitat for years. Resuscitation of dormant M. tuberculosis bacteria is promoted by resuscitation-promoting factors (Rpfs), which are secreted from slowly replicating bacteria close to dormant bacteria. Here we report the crystal structure of a truncated form of RpfB (residues 194–362), the sole indispensable Rpf of the five Rpfs encoded in this bacterium genome. The structure, denoted as ΔDUFRpfB, exhibits a comma-like shape formed by a lysozyme-like globular catalytic domain and an elongated G5 domain, which is widespread among cell surface binding proteins. The G5 domain, whose structure was previously uncharacterised, presents some peculiar features. The basic structural motif of this domain, which represents the tail of the comma-like structure, is a novel super-secondary-structure element, made of two β-sheets interconnected by a pseudo-triple helix. This intricate organisation leads to the exposure of several backbone hydrogen-bond donors/acceptors. Mutagenesis analyses and solution studies indicate that this protein construct as well as the full-length form are elongated monomeric proteins. Although ΔDUFRpfB does not self-associate, the exposure of structural elements (backbone H-bond donors/acceptors and hydrophobic side chains) that are usually buried in globular proteins is typically associated with adhesive properties. This suggests that the RpfB G5 domain has a cell-wall adhesive function, which allows the catalytic domain to be properly oriented for the cleavage reaction. Interestingly, sequence comparisons indicate that these structural features are also shared by G5 domains involved in biofilm formation.
  • Keywords
    peptidoglycan , Cell wall , Latency , crystal structure , Tuberculosis
  • Journal title
    Journal of Molecular Biology
  • Serial Year
    2009
  • Journal title
    Journal of Molecular Biology
  • Record number

    1257831