• Title of article

    Membrane binding motif of the P-type cardiotoxin

  • Author/Authors

    Peter V. Dubovskii، نويسنده , , Daria V. Dementieva، نويسنده , , Eduard V. Bocharov، نويسنده , , Yuri N. Utkin، نويسنده , , Alexander S. Arseniev، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2001
  • Pages
    13
  • From page
    137
  • To page
    149
  • Abstract
    Carditoxins (CTXs) from cobra snake venoms, the basic 60–62 residue all-beta sheet polypeptides, are known to bind to and impair the function of cell membranes. To assess the membrane induced conformation and orientation of CTXs, the interaction of the P-type cardiotoxin II from Naja oxiana snake venom (CTII) with perdeuterated dodecylphosphocholine (DPC) was studied using 1H-NMR spectroscopy and diffusion measurements. Under conditions where the toxin formed a well-defined complex with DPC, the spatial structure of CTII with respect to the presence of tightly bound water molecules in loop II, was calculated using the torsion angle dynamics program DYANA. The structure was found to be similar, except for subtle changes in the tips of all three loops, to the previously described “major” form of CTII in aqueous solution illustrated by the “trans” configuration of the Val7-Pro8 peptide bond. No “minor” form with the “cis” configuration of the above bond was found in the micelle-bound state. The broadening of the CTII backbone proton signals by 5, 16-doxylstearate relaxation probes, together with modeling based on the spatial structure of CTII, indicated a periphery mode of binding of the toxin molecule to the micelle and revealed its micelle interacting domain. The latter includes a hydrophobic region of CTII within the extremities of loops I and III (residues 5–11, 46–50), the basement of loop II (residues 24–29,31–37) and the belt of polar residues encircling these loops (lysines 4,5,12,23,50, serines 11,46, histidine 31, arginine 36). It is suggested that this structural motif and the mode of binding can be realized during interaction of CTXs with lipid and biological membranes.
  • Keywords
    NMR , P-type cardiotoxin (cytotoxin) , dodecylphosphocholine micelle , doxylstearate relaxation probe , Spatial structure
  • Journal title
    Journal of Molecular Biology
  • Serial Year
    2001
  • Journal title
    Journal of Molecular Biology
  • Record number

    1240424