• Title of article

    Binding to δ and μ opioid receptors by deltorphin I/II analogues modified at the Phe3 and Asp4/Glu4 side chains: a report of 32 new analogues and a QSAR study Original Research Article

  • Author/Authors

    Stephen E. Schullery، نويسنده , , Tasneem Mohammedshah، نويسنده , , Hafida Makhlouf، نويسنده , , Eleanor L. Marks، نويسنده , , Benjamin S. Wilenkin، نويسنده , , Sharleen Escobar، نويسنده , , Carol Mousigian، نويسنده , , Deborah L. Heyl، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 1997
  • Pages
    14
  • From page
    2221
  • To page
    2234
  • Abstract
    The synthesis and binding affinities of 32 X3Gly4 dual-substitution analogues of the natural opioid heptapeptides deltorphin I and II are reported. A multiple regression QSAR analysis was performed using those results along with literature data for the X3Asp4 and Phe3X4 side chain analogues. Fitting to a three-term potential well model with hydrophobic and van der Waals attraction terms and a steric repulsion term indicates that the δ and μ receptor sites for binding the residue three side chain are similar, and that the binding interaction is primarily van der Waals and secondarily hydrophobic. Further analysis indicates that both sites are more constrained with respect to side chain length than width or thickness, and the μ site appears to be somewhat larger. A binding model consistent with these findings pictures the native third residues Phe ring laying on a step notched out of the receptor surface, pointing toward the back (riser) of the step, and sandwiched between the receptor and ligand. However, the binding sites for the residue four side chains are quite different on δ and μ receptors. Binding to the δ site appears to involve both electrostatic attraction (probably to a partial positive charge) and van der Waals attraction, but not necessarily hydrogen bonding, and more constraint with respect to side chain length than width or thickness. In contrast, there is no evidence for any kind of binding attraction between the side chain of residue four and the μ site, which acts more as steric repulsion site, as though the space that is a pocket on the δ receptor is filled in on the μ receptor. A regression model based only on steric repulsion by van der Waals bulk and/or the effective bulk of a hydration layer accounts for over 80% of the residue four related variation in μ affinity.
  • Keywords
    deltorphin , QSAR , Opioid , Binding , Peptide
  • Journal title
    Bioorganic and Medicinal Chemistry
  • Serial Year
    1997
  • Journal title
    Bioorganic and Medicinal Chemistry
  • Record number

    1301419