• Title of article

    Peptide NMHRYPNQ of the Cellular Prion Protein (PrPC) Inhibits Aggregation and Is a Potential Key for Understanding Prion–Prion Interactions

  • Author/Authors

    Dirk Rehders، نويسنده , , Birgit Claasen، نويسنده , , Lars Redecke، نويسنده , , Alexander Buschke، نويسنده , , Caroline Reibe، نويسنده , , Nico Jehmlich، نويسنده , , Martin von Bergen، نويسنده , , Christian Betzel، نويسنده , , Bernd Meyer، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2009
  • Pages
    10
  • From page
    198
  • To page
    207
  • Abstract
    Pathogenesis of transmissible spongiform encephalopathies is correlated with a conversion of the normal cellular form of the prion protein (PrPC) into the abnormal isoform (scrapie form of PrP). Contact of the normal PrP with its abnormal isoform, the scrapie form of PrP, induces the transformation. Knowledge of molecules that inhibit such contacts leads to an understanding of the mechanism of the aggregation, and these molecules may serve as leads for drugs against transmissible spongiform encephalopathies. Therefore, we screened a synthetic octapeptide library of the globular domain of the human PrPC for binding affinity to PrPC. Two fragments with binding affinity, 149YYRENMHR156 and 153NMHRYPNQ160, were identified with Kd values of 21 and 25 μM, respectively. A 10-fold excess of peptide 153NMHRYPNQ160 inhibits aggregation of the PrP by 99%. NMR and mass spectrometry showed that the binding region of the peptide 153NMHRYPNQ160 is located at helix 3 of the PrP.
  • Keywords
    surface plasmon resonance , BSE , NMR binding epitope , Aggregation
  • Journal title
    Journal of Molecular Biology
  • Serial Year
    2009
  • Journal title
    Journal of Molecular Biology
  • Record number

    1250271