Conformational Partitioning of the Fusion Peptide of HIV-1 gp41 and Its Structural Analogs in Bilayer Membranes

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Conformational Partitioning of the Fusion Peptide of HIV-1 gp41 and Its Structural Analogs in Bilayer Membranes

Michael W. Maddox and Marjorie L. Longo

Department of Chemical Engineering and Materials Science, University of California, Davis, California 95616 USA

Experiments have shown that the ability of the HIV-1 virus to infect cells can be greatly diminished by deactivation of theN-terminal (fusion) peptide of its glycoprotein gp41. Deactivationcan be achieved by the deletion of several amino acid residues,or replacement of a hydrophobic residue with a polar residue,to form mutant variants of the wild-type peptide. We report MonteCarlo simulation studies of a simplified peptide/membrane model,representing the interaction of an HIV-1 fusion peptide (FP) andfour closely related mutagens with a lipid bilayer. In agreementwith experimental results, we show that FP inserts deeply intothe bilayer at ~ 40° to the bilayer normal. We also show a previouslyunreported behavior of membrane peptides, namely their equilibriumpartitioning between several distinct conformations within thebilayer. We quantify this partitioning behavior and characterizeeach conformation in terms of its geometry, energy, and entropy.The diminished ability of FP mutagens to hemolyse and aggregatered blood cells due to their partitioning into unfavorable conformations,is also discussed. Our analysis supports a negative curvaturemechanism for red blood cell hemolysis by FP. We also suggestthat the small repulsive forces between surface-adsorbed peptidesin opposing membrane surfaces may blockaggregation.

Biophys J, December 2002, p. 3088-3096, Vol. 83, No. 6
© 2002 by the Biophysical Society 0006-3495/02/12/3088/09 $2.00

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