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  • Analysis of HIV-1 fusion peptide inhibition by synthetic peptides from E1 protein of GB virus C.

Analysis of HIV-1 fusion peptide inhibition by synthetic peptides from E1 protein of GB virus C.

Journal of colloid and interface science (2011-05-14)
Maria Jesús Sánchez-Martín, Kalina Hristova, Montserrat Pujol, Maria J Gómara, Isabel Haro, M Asunción Alsina, M Antònia Busquets
ABSTRACT

The aim of this study was to identify proteins that could inhibit the activity of the peptide sequence representing the N-terminal of the surface protein gp41 of HIV, corresponding to the fusion peptide of the virus (HIV-1 FP). To do this we synthesized and studied 58 peptides corresponding to the envelope protein E1 of the hepatitis G virus (GBV-C). Five of the E1 synthetic peptides: NCCAPEDIGFCLEGGCLV (P7), APEDIGFCLEGGCLVALG (P8), FCLEGGCLVALGCTICTD (P10), QAGLAVRPGKSAAQLVGE (P18) and AQLVGELGSLYGPLSVSA (P22) were capable of inhibiting the leakage of vesicular contents caused by HIV-1 FP. A series of experiments were carried out to determine how these E1 peptides interact with HIV-1 FP. Our studies analyzed the interactions with and without the presence of lipid membranes. Isothermal titration calorimetry revealed that the binding of P7, P18 and P22 peptides to HIV-1 FP is strongly endothermic, and that binding is entropy-driven. Gibbs energy for the process indicates a spontaneous binding between E1 peptides and HIV-1 FP. Moreover, confocal microscopy of Giant Unilamellar Vesicles revealed that the disruption of the lipid bilayer by HIV-1 FP alone was inhibited by the presence of any of the five selected peptides. Our results highlight that these E1 synthetic peptides could be involved in preventing the entry of HIV-1 by binding to the HIV-1 FP. Therefore, the continued study into the interaction between GBV-C peptides and HIV-1 FP could lead to the development of new therapeutic agents for the treatment of AIDS.

MATERIALS
Product Number
Brand
Product Description

Avanti
18:0 (9,10dibromo) PC, 1,2-di-(9,10-dibromo)stearoyl-sn-glycero-3-phosphocholine, chloroform