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A Pilot Study of the Use of Mycophenolate Mofetil as a Component of Therapy for Multidrug-Resistant HIV-1 Infection
25
Citations
20
References
2001
Year
ImmunologySubtype BPharmacotherapyAntiviral DrugViral Structural ProteinPilot StudyDrug ResistanceMycophenolate MofetilHuman RetrovirusAntiviral Drug DevelopmentResistance Mutation (Virology)Antimicrobial ResistanceEnvelope GlycoproteinsVirologyHivPolyvalent VaccinePharmacologyNative Envelope GlycoproteinsVaccinationMultidrug-resistant Hiv-1 InfectionTreatment And PreventionAntiviral ResponseAntiviral TherapyVaccine DesignMedicineViral ImmunityDrug Discovery
Summary: We investigated immunogenic properties of native envelope glycoproteins derived from HIV-1 (subtype B). Our main objective was to assess whether the design of multivalent vaccines affects generation of neutralizing antibodies against primary viruses. Recombinant Semliki Forest virus (SFV) particles producing various HIV-1 envelope glycoproteins were used as vaccine vectors. The following multivalent vac cination approaches were compared: 1) immunization with a mixture of recombinant SFV expressing envelope glycoproteins derived from three HIV-1 primary isolates and two T-cell laboratory-adapted (TCLA) viruses; 2) immunization with a mixture of recombinant SFV expressing only the envelope glycoproteins derived from three HIV-1 primary isolates; 3) sequential immunizations with the recombinant SFV ex pressing the envelope glycoproteins derived from three HIV-1 primary isolates and two TCLA viruses, respectively. Two monovalent vaccine approaches using SFV expressing envelope glycoproteins derived from a single primary isolate or TCLA virus were also included in the study. The multivalent vaccination strategies based on SFV vaccine vectors did not induce more neutralizing antibodies than the previously tested TCLA envelope immunogens, which gave disappointing results against primary isolates.
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