Your search keyword '"HIV Fusion Inhibitors/pharmacology"' showing total 2 results

1. Baseline Susceptibility of Primary HIV-2 to Entry Inhibitors

Author

Cheila Rocha, Fernando Maltez, Umbelina Caixas, Pedro Borrego, Manuela Doroana, Patrícia Cavaco-Silva, Rita Calado, Inês Bártolo, Francisco Antunes, Helena Barroso, José Maria Marcelino, and Nuno Taveira

Subjects

Male, Cyclohexanes/pharmacology, Enfuvirtide, HIV Fusion Inhibitors/pharmacology, HCC INF, Human immunodeficiency virus (HIV), HIV Infections, Cyclohexanes/therapeutic use, medicine.disease_cause, Maraviroc, HIV Envelope Protein gp41/therapeutic use, chemistry.chemical_compound, HIV Fusion Inhibitors, inhibitors, Medicine, Pharmacology (medical), Triazoles/pharmacology, HIV Fusion Inhibitors/therapeutic use, Antiviral therapy, virus diseases, HIV Envelope Protein gp41/pharmacology, HIV Envelope Protein gp41, HIV-2/drug effects, Infectious Diseases, HIV-1/drug effects, Publishing, CCR5 Receptor Antagonists, Female, Triazoles/therapeutic use, medicine.drug, medicine.medical_specialty, Amides/therapeutic use, Anti-HIV Agents, HIV Infections/drug therapy, MEDLINE, Microbial Sensitivity Tests, Inhibitory Concentration 50, Cyclohexanes, HSJ MED, Anti-HIV Agents/pharmacology, Humans, Inhibitory concentration 50, Baseline (configuration management), Amides/pharmacology, Pharmacology, Peptide Fragments/therapeutic use, Quaternary Ammonium Compounds/therapeutic use, Peptide Fragments/pharmacology, Quaternary Ammonium Compounds/pharmacology, business.industry, Triazoles, Amides, Virology, Peptide Fragments, Quaternary Ammonium Compounds, chemistry, Anti-HIV Agents/therapeutic use, Family medicine, HIV-2, HIV-1, HIV Infections/virology, business

Abstract

Background The baseline susceptibility of primary HIV-2 to maraviroc (MVC) and other entry inhibitors is currently unknown. Methods The susceptibility of 19 HIV-2 isolates obtained from asymptomatic and AIDS patients and seven HIV-1 clinical isolates to the fusion inhibitors enfuvirtide (ENF) and T-1249, and to the coreceptor antagonists AMD3100, TAK-779 and MVC, was measured using a TZM-bl cell-based assay. The 50% inhibitory concentration (IC50), 90% inhibitory concentration (IC90) and dose–response curve slopes were determined for each drug. Results ENF and T-1249 were significantly less active on HIV-2 than on HIV-1 (211- and 2-fold, respectively). AMD3100 and TAK-779 inhibited HIV-2 and HIV-1 CXCR4 tropic (X4) and CCR5 tropic (R5) variants with similar IC50 and IC90 values. MVC, however, inhibited the replication of R5 HIV-2 variants with significantly higher IC90 values (42.7 versus 9.7 nM; P+ T-cells. Conclusions T-1249 is a potent inhibitor of HIV-2 replication indicating that new fusion inhibitors might be useful to treat HIV-2 infection. Coreceptor antagonists TAK-779 and AMD3100 are also potent inhibitors of HIV-2 replication. The reduced sensitivity of R5 variants to MVC, especially in severely immunodeficient patients, indicates that the treatment of HIV-2-infected patients with MVC might require higher dosages than those used in HIV-1 patients, and should be adjusted to the disease stage.

Published

2011

2. Semisynthetic analogues of PSC-RANTES, a potent anti-HIV protein

Author

Robin E. Offord, Oliver Hartley, Hubert François Gaertner, Gabriel Kuenzi, and Paolo Botti

Subjects

Spectrometry, Mass, Electrospray Ionization, Stereochemistry, HIV Fusion Inhibitors/pharmacology, Thiazolidine, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Hydrazide, Chemical synthesis, chemistry.chemical_compound, HIV Fusion Inhibitors, Microbicide, medicine, Peptide bond, Humans, Chromatography High Pressure Liquid, ddc:610, ddc:576, Chemokine CCL5, Chromatography, High Pressure Liquid, Pharmacology, Chemistry, Organic Chemistry, Combinatorial chemistry, Semisynthesis, Entry inhibitor, Hela Cells, Chemokine CCL5/chemistry/pharmacology, Spectrometry Mass Electrospray Ionization, Linker, Biotechnology, medicine.drug, HeLa Cells

Abstract

New HIV prevention methods are needed, and among those currently being explored are "microbicides", substances applied topically to prevent HIV acquisition during sexual intercourse. The chemokine analogue PSC-RANTES (N(alpha)(n-nonanoyl)-des-Ser(1)-[ L-thioprolyl(2), L-cyclohexylglycyl(3)]-RANTES(4-68)) is a highly potent HIV entry inhibitor which has shown promising efficacy in its initial evaluation as a candidate microbicide. However, a way must be found to produce the molecule by cheaper means than total chemical synthesis. Since the only noncoded structures are located at the N-terminus, a possible solution would be to produce a protein fragment representing all but the N-terminal region using low-cost recombinant production methods and then to attach, site specifically, a short synthetic fragment containing the noncoded N-terminal structures. Here, we describe the evaluation of a range of different conjugation chemistries in order to identify those with potential for development as economical routes to production of a PSC-RANTES analogue with antiviral activity as close as possible to that of the parent protein. The strategies tested involved linkage through oxime, hydrazone/hydrazide, and Psi[CH2-NH] bonds, as well as through a peptide bond obtained either by a thiazolidine rearrangement or by direct alpha-amino acylation of a protein fragment in which 4 of the 5 lysine residues of the native sequence were replaced by arginine (the fifth lysine is essential for activity). Where conjugation involved replacement of one or more residues with a linker moiety, the point in the main chain at which the linker was introduced was varied. The resulting panel of 22 PSC-RANTES analogues was evaluated for anti-HIV activity in an entry inhibition assay. The [Arg (25,45,56,57)] PSC-RANTES analogue has comparable potency to PSC-RANTES, and one of the oxime linked analogues, 4L-57, has potency only 5-fold lower, with scope for improvement. Both represent promising leads for development as microbicide compounds that could be produced at low cost via semisynthesis.

Published

2008