Interaction of short modified peptides deriving from glycoprotein gp36 of feline immunodeficiency virus with phospholipid membranes

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作者
Gerardino D’Errico
Giuseppe Vitiello
Anna Maria D’Ursi
Derek Marsh
机构
[1] Università di Napoli “Federico II”,Dipartimento di Chimica “Paolo Corradini”
[2] Università di Salerno,Dipartimento di Scienze Farmaceutiche
[3] Max-Planck-Institut für biophysikalische Chemie,Abt Spektroskopie
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关键词
Feline immunodeficiency virus; Membrane; Electron spin resonance; Spin-label;
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摘要
A tryptophan-rich octapeptide, C8 (Ac-Trp-Glu-Asp-Trp-Val-Gly-Trp-Ile-NH2), modelled on the membrane-proximal external region of the feline immunodeficiency virus (FIV) gp36 glycoprotein ectodomain, exhibits potent antiviral activity against FIV. A mechanism has been proposed by which the peptide, being positioned on the surface of the cell membrane, inhibits its fusion with the virus. In the present work, peptide–lipid interactions of C8 with dimyristoyl phosphatidylcholine liposomes are investigated using electron spin resonance spectroscopy of spin-labelled lipids. Three other peptides, obtained from modifications of C8, have also been investigated, in an attempt to clarify the essential molecular features of the interactions involving the tryptophan residues. The results show that C8 adsorbs strongly on the bilayer surface. Membrane binding requires not only the presence of the Trp residues in the sequence, but also their common orientation on one side of the peptide that is engendered by the WX2 WX2 W motif. Membrane interaction correlates closely with peptide antiviral activity, indicating that the membrane is essential in stabilizing the peptide conformation that will be able to inhibit viral infection.
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页码:873 / 882
页数:9
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