| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 1398875 | European Journal of Medicinal Chemistry | 2014 | 16 Pages |
•E1P8cyc peptide inhibits the interaction of HIV-1 FP with lipid monolayers and bilayers.•E1P8cyc peptide inhibits the fusogenic capacity of HIV-1 FP.•E1P8cyc peptide induce conformational changes in the secondary structure of HIV-1 FP.
The development of peptide fusion inhibitors based on short synthetic peptides represents a promising option in the fight against HIV-1 infection, especially in individuals infected with multiresistant HIV-1 strains. GBV-C has the beneficial effect of retarding the progression of AIDS in people who are co-infected with both the GBV-C and HIV viruses. In previous works, the E1(22–39) GBV-C sequence (E1P8lin) was found to be capable of inhibiting the interaction of HIV-1 FP with bilayers and its cyclic analogue (E1P8cyc) showed a higher anti-HIV-1 activity. In the present work, in an attempt to gain a better understanding of the interaction of E1P8 peptides with HIV-1 FP, we analyzed direct interactions between peptides at the molecular level. Our results support that E1P8cyc might be more potent at blocking HIV-1 entry than E1P8lin as a consequence of the structure induced in the complex formed with HIV-1 FP, which is able to modify the conformation adopted by this functional domain of the HIV-1 gp41 protein in target cell membranes.
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