Definition of a New HLA B*52-Restricted Rev CTL Epitope Targeted by an HIV-1-Infected Controller.
Boutaina El KenzKatja G SchmidtVictoria K Ogungbemi-AltSilke BergmannPhilipp SteiningerKlaus KornBernd SpriewaldEllen G HarrerKrystelle Nganou-MakamdopThomas HarrerPublished in: Viruses (2023)
The analysis of T-cell responses in HIV-1-infected controllers may contribute to a better understanding of the protective components of the immune system. Here, we analyzed the HIV-1-specific T-cell response in a 59-year-old HIV-1-infected controller, infected for at least seven years, who presented with low viral loads ranging from <20 copies/mL to 200 copies/mL and normal CD4 counts of >800 cells/µL. In γ-IFN-ELISpot assays using freshly isolated PBMCs, he displayed a very strong polyclonal T-cell response to eight epitopes in Gag, Nef and Rev; with the dominant responses directed against the HLA-B*57-epitope AISPRTLNAW and against a so-far-unknown epitope within Rev. Further analyses using peptide-stimulated T-cell lines in γ-IFN-ELISpot assays delineated the peptide RQRQIRSI (Rev-RI8) as a newly defined HLA-B*52-restricted epitope located within a functionally important region of Rev. Peptide-stimulation assays in 15 HLA-B*52-positive HIV-1-infected subjects, including the controller, demonstrated recognition of the Rev-RI8 epitope in 6/15 subjects. CD4 counts before the start of antiviral therapy were significantly higher in subjects with recognition of the Rev-RI8 epitope. Targeting of the Rev-RI8 epitope in Rev by CTL could contribute to the positive association of HLA-B*52 with a more favorable course of HIV-1-infection.
Keyphrases
- hiv infected
- antiretroviral therapy
- human immunodeficiency virus
- monoclonal antibody
- hiv positive
- hiv aids
- immune response
- induced apoptosis
- cancer therapy
- peripheral blood
- stem cells
- endoplasmic reticulum stress
- hepatitis c virus
- oxidative stress
- signaling pathway
- men who have sex with men
- cell proliferation
- cell cycle arrest