• Title of article

    Integrin inhibitors from snake venom: Exploring the relationship between the structure and activity of RGD-peptides

  • Author/Authors

    Wermelinger، نويسنده , , Luciana S. and Geraldo، نويسنده , , Reinaldo B and Frattani، نويسنده , , Flavia S. and Rodrigues، نويسنده , , Carlos R. and Juliano، نويسنده , , Maria A. de Castro، نويسنده , , Helena C. and Zingali، نويسنده , , Russolina B. Zingali، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2009
  • Pages
    8
  • From page
    25
  • To page
    32
  • Abstract
    αIIbβ3 is an integrin that is involved in platelet adhesion and aggregation. This receptor may be inhibited by cysteine-rich peptides known as disintegrins. We isolated two disintegrins from Bothrops jararaca venom called jarastatin and jararacin. We evaluated the structural characteristics and the effects on human platelet aggregation of these disintegrins. Inhibitory profiles were compared to six distinct peptides synthesized based on their RGD hairpin loop primary sequences. Both jarastatin and jararacin inhibited ADP and thrombin induction. Conversely, none of the cyclic peptides showed high-quality activity in assays induced by ADP or thrombin. We constructed homology models for all of these molecules, and theoretically evaluated their interaction with the αIIbβ3 crystal structure using a molecular modeling approach. These results support the observations that the cyclic peptides had little effects, and also reinforce the observation that residues outside the disintegrin RGD sequence are required for interactions with receptor.
  • Keywords
    Aggregation , disintegrin , platelet , Inhibitor , RGD-peptide , Integrin , Jararacin , Jarastatin , molecular modeling , Receptor
  • Journal title
    Archives of Biochemistry and Biophysics
  • Serial Year
    2009
  • Journal title
    Archives of Biochemistry and Biophysics
  • Record number

    1603201