• Title of article

    Interstitial Contacts in an RNA-Dependent RNA Polymerase Lattice

  • Author/Authors

    Andres B. Tellez، نويسنده , , Jing Wang، نويسنده , , Elizabeth J. Tanner، نويسنده , , Jeannie F. Spagnolo، نويسنده , , Scott Crowder and Karla Kirkegaard، نويسنده , , Esther Bullitt، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2011
  • Pages
    14
  • From page
    737
  • To page
    750
  • Abstract
    Catalytic activities can be facilitated by ordered enzymatic arrays that co-localize and orient enzymes and their substrates. The purified RNA-dependent RNA polymerase from poliovirus self-assembles to form two-dimensional lattices, possibly facilitating the assembly of viral RNA replication complexes on the cytoplasmic face of intracellular membranes. Creation of a two-dimensional lattice requires at least two different molecular contacts between polymerase molecules. One set of polymerase contacts, between the “thumb” domain of one polymerase and the back of the “palm” domain of another, has been previously defined. To identify the second interface needed for lattice formation and to test its function in viral RNA synthesis, we used a hybrid approach of electron microscopic and biochemical evaluation of both wild-type and mutant viral polymerases to evaluate computationally generated models of this second interface. A unique solution satisfied all constraints and predicted a two-dimensional structure formed from antiparallel arrays of polymerase fibers that use contacts from the flexible amino-terminal region of the protein. Enzymes that contained mutations in this newly defined interface did not form lattices and altered the structure of wild-type lattices. When reconstructed into virus, mutations that disrupt lattice assembly exhibited growth defects, synthetic lethality or both, supporting the function of the oligomeric lattice in infected cells. Understanding the structure of polymerase lattices within the multimeric RNA-dependent RNA polymerase complex should facilitate antiviral drug design and provide a precedent for other positive-strand RNA viruses.
  • Keywords
    protein oligomerization , site-directed mutagenesis , Electron microscopy , macromolecular assembly , molecular modeling
  • Journal title
    Journal of Molecular Biology
  • Serial Year
    2011
  • Journal title
    Journal of Molecular Biology
  • Record number

    1254094