Composition and function of T cell subpopulations are slow to change despite effective antiretroviral treatment of HIV disease.

Composition and function of T cell subpopulations are slow to change despite effective antiretroviral treatment of HIV disease.

The ability to reconstitute a normal immune system with antiretroviral therapy in the setting of HIV infection remains uncertain. This study aimed to characterize quantitative and qualitative aspects of various T cell subpopulations that do not improve despite effective ART. CD4∶CD8 ratio was evalua...

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Main Authors: Brinda Emu, Walter J Moretto, Rebecca Hoh, Melissa Krone, Jeffrey N Martin, Douglas F Nixon, Steven G Deeks, Joseph M McCune
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3897457?pdf=render
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spelling doaj-5be25b4023fd48e089b4316c51a28abe2020-11-25T01:46:39ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0191e8561310.1371/journal.pone.0085613Composition and function of T cell subpopulations are slow to change despite effective antiretroviral treatment of HIV disease.Brinda EmuWalter J MorettoRebecca HohMelissa KroneJeffrey N MartinDouglas F NixonSteven G DeeksJoseph M McCuneThe ability to reconstitute a normal immune system with antiretroviral therapy in the setting of HIV infection remains uncertain. This study aimed to characterize quantitative and qualitative aspects of various T cell subpopulations that do not improve despite effective ART. CD4∶CD8 ratio was evaluated in HIV-infected subjects with viral loads >10,000 copies/µl ("non-controllers", n = 42), those with undetectable viral loads on ART ("ART-suppressed", n = 53), and HIV-uninfected subjects (n = 22). In addition, T cell phenotype and function were examined in 25 non-controllers, 18 ART-suppressed, and 7 HIV-uninfected subjects. CD4∶CD8 ratio in non-controllers, ART-suppressed, and HIV-uninfected subjects was 0.25, 0.48, and 1.95 respectively (P<0.0001 for all comparisons). The increased ratio in ART-suppressed compared to non-controllers was driven by an increase of CD4+ T cells, with no change in the expanded CD8+ T cell population. Expansion of differentiated (CD28-CD27-CD45RA+/-CCR7-) T cell subpopulations persisted despite ART and minimal changes were noted in naïve T cell frequencies over time. Increased number of CD8+CD28- T cells and increased CD8+ CMV-specific T cell responses were associated with a decreased CD4∶CD8 ratio. Measures of T cell function demonstrated persistence of high frequencies of CD8+ T cells producing IFN-γ. Lastly, though all CD8+ subpopulations demonstrated significantly lower Ki67 expression in ART-suppressed subjects, CD4+ T cell subpopulations did not consistently show this decrease, thus demonstrating different proliferative responses in the setting of T cell depletion. In summary, this study demonstrated that CD4∶CD8 ratios remained significantly decreased and naïve T cell numbers were slow to increase despite long-term viral suppression on ART. In addition, there is a evidence of differential regulation of the CD4+ and CD8+ T cell subpopulations, suggesting independent homeostatic regulation of the two compartments.http://europepmc.org/articles/PMC3897457?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Brinda Emu
Walter J Moretto
Rebecca Hoh
Melissa Krone
Jeffrey N Martin
Douglas F Nixon
Steven G Deeks
Joseph M McCune
spellingShingle Brinda Emu
Walter J Moretto
Rebecca Hoh
Melissa Krone
Jeffrey N Martin
Douglas F Nixon
Steven G Deeks
Joseph M McCune
Composition and function of T cell subpopulations are slow to change despite effective antiretroviral treatment of HIV disease.
PLoS ONE
author_facet Brinda Emu
Walter J Moretto
Rebecca Hoh
Melissa Krone
Jeffrey N Martin
Douglas F Nixon
Steven G Deeks
Joseph M McCune
author_sort Brinda Emu
title Composition and function of T cell subpopulations are slow to change despite effective antiretroviral treatment of HIV disease.
title_short Composition and function of T cell subpopulations are slow to change despite effective antiretroviral treatment of HIV disease.
title_full Composition and function of T cell subpopulations are slow to change despite effective antiretroviral treatment of HIV disease.
title_fullStr Composition and function of T cell subpopulations are slow to change despite effective antiretroviral treatment of HIV disease.
title_full_unstemmed Composition and function of T cell subpopulations are slow to change despite effective antiretroviral treatment of HIV disease.
title_sort composition and function of t cell subpopulations are slow to change despite effective antiretroviral treatment of hiv disease.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description The ability to reconstitute a normal immune system with antiretroviral therapy in the setting of HIV infection remains uncertain. This study aimed to characterize quantitative and qualitative aspects of various T cell subpopulations that do not improve despite effective ART. CD4∶CD8 ratio was evaluated in HIV-infected subjects with viral loads >10,000 copies/µl ("non-controllers", n = 42), those with undetectable viral loads on ART ("ART-suppressed", n = 53), and HIV-uninfected subjects (n = 22). In addition, T cell phenotype and function were examined in 25 non-controllers, 18 ART-suppressed, and 7 HIV-uninfected subjects. CD4∶CD8 ratio in non-controllers, ART-suppressed, and HIV-uninfected subjects was 0.25, 0.48, and 1.95 respectively (P<0.0001 for all comparisons). The increased ratio in ART-suppressed compared to non-controllers was driven by an increase of CD4+ T cells, with no change in the expanded CD8+ T cell population. Expansion of differentiated (CD28-CD27-CD45RA+/-CCR7-) T cell subpopulations persisted despite ART and minimal changes were noted in naïve T cell frequencies over time. Increased number of CD8+CD28- T cells and increased CD8+ CMV-specific T cell responses were associated with a decreased CD4∶CD8 ratio. Measures of T cell function demonstrated persistence of high frequencies of CD8+ T cells producing IFN-γ. Lastly, though all CD8+ subpopulations demonstrated significantly lower Ki67 expression in ART-suppressed subjects, CD4+ T cell subpopulations did not consistently show this decrease, thus demonstrating different proliferative responses in the setting of T cell depletion. In summary, this study demonstrated that CD4∶CD8 ratios remained significantly decreased and naïve T cell numbers were slow to increase despite long-term viral suppression on ART. In addition, there is a evidence of differential regulation of the CD4+ and CD8+ T cell subpopulations, suggesting independent homeostatic regulation of the two compartments.
url http://europepmc.org/articles/PMC3897457?pdf=render
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