Abstract

HIV-infected older individuals may have a diminished immune response because of exhaustion/immune aging of T-cells. Therefore, we have investigated HIV-specific CD4 and CD8 T-cell responses in 100 HIV-infected patients (HIV+) who have aged on long-term antiretroviral therapy (ART) and achieved controlled viremia (mostly undetectable viral load; 92 patients with <20 to <40 HIV RNA copies/mL and 8 <60 to <100) and improved CD4 T-cell counts. We show that the median frequencies of HIV-specific CD4+ and CD8+ IFN-γ T-cells were higher in HIV+ than uninfected individuals (HIV-), including increasing levels of IFN-γproduced by CD4+ T-cells and decreasing levels by CD8+ T-cells with increasing CD4 T-cell counts in HIV+. No correlation was found between T-cell responses and varying levels of undetectable viremia. HIV-specific TNF-α made by CD8+ T-cells was higher in HIV+ than HIV-, including decreasing levels with increasing CD4 T-cell counts in HIV+. Furthermore, the CD8+ T-cell mediators, CD107a and Granzyme-B, were higher in HIV+ than HIV-, and decreased with increasing CD4 T-cell counts in HIV+. Remarkably, HIV-specific CD8 T-cells produced decreasing levels of IFN-γwith increasing age of HIV+, including decreased levels of CD107a and Granzyme-B in older HIV+. However, HIV-specific CD8+ T-cells produced increasing levels of TNF-α with increasing age of the HIV+, suggesting continued inflammation. In conclusion, HIV+ with controlled viremia on long-term ART and with higher CD4 T-cell counts showed reduced HIV-specific CD8 T-cell responses as compared to those with lower CD4 T-cell counts, and older HIV+ exhibited decreasing levels of CD8 T-cell responses with increasing age.

Highlights

  • Despite the devastating effects of human immunodeficiency virus type 1 (HIV) infection on host immunity, infected adults mount a robust immune response against HIV antigens [1]

  • We found that the background levels of median frequencies of CD4+ T-cells expressing IFN-γ were higher in HIV+ (0.069%) than HIV- (0.051%) p = 0.0021 (Fig 2A), whereas the median frequencies of CD8+IFN-γ T-cells were lower in HIV+ (0.145%) compared with HIV(0.21%) (Fig 2B)

  • We have investigated HIV+ than uninfected individuals (HIV-)specific CD4 and CD8 T-cell responses in HIVinfected patients with controlled viremia and increasing CD4 T-cell counts and age of the HIV+ patients

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Summary

Introduction

Despite the devastating effects of human immunodeficiency virus type 1 (HIV) infection on host immunity, infected adults mount a robust immune response against HIV antigens [1]. In the era of expansion of antiretroviral drugs, many HIV-infected patients (HIV+) are successfully treated with long-term antiretroviral therapy (ART) resulting in controlled viremia (undetectable to very low viral load), improved CD4 T-cell counts, reduced incidence of opportunistic infections and increased life expectancy [6,7]. We show that the CD4+ and CD8+ T-cells from HIV+ older patients with controlled viremia (92% of the patients had

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