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Emergence of a distinct HIV-specific IL-10-producing CD8 super(+) T-cell subset with immunomodulatory functions during chronic HIV-1 infection
Interleukin-10 (IL-10) plays a key role in regulating proinflammatory immune responses to infection but can interfere with pathogen clearance. Although IL-10 is upregulated throughout HIV-1 infection in multiple cell subsets, whether this is a viral immune evasion strategy or an appropriate response...
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Published in: | European journal of immunology 2013-11, Vol.43 (11), p.2875-2885 |
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container_issue | 11 |
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container_title | European journal of immunology |
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creator | Clutton, Genevieve Yang, Hongbing Hancock, Gemma Sande, Nellia Holloway, Cameron Angus, Brian Delft, Annette Barnes, Eleanor Borrow, Persephone Pellegrino, Pierre Williams, Ian McMichael, Andrew Dorrell, Lucy |
description | Interleukin-10 (IL-10) plays a key role in regulating proinflammatory immune responses to infection but can interfere with pathogen clearance. Although IL-10 is upregulated throughout HIV-1 infection in multiple cell subsets, whether this is a viral immune evasion strategy or an appropriate response to immune activation is unresolved. Analysis of IL-10 production at the single cell level in 51 chronically infected subjects (31 antiretroviral (ART) naive and 20 ART treated) showed that a subset of CD8 super(+) T cells with a CD25 super(neg) FoxP3 super(neg) phenotype contributes substantially to IL-10 production in response to HIV-1 gag stimulation. The frequencies of gag-specific IL-10- and IFN-[gamma]-producing T cells in ART-naive subjects were strongly correlated and the majority of these IL-10 super(+) CD8 super(+) T cells co-produced IFN-[gamma]; however, patients with a predominant IL-10 super(+)/IFN-[gamma] super(neg) profile showed better control of viraemia. Depletion of HIV-specific CD8 super(+) IL-10 super(+) cells from PBMCs led to upregulation of CD38 on CD14 super(+) monocytes together with increased IL-6 production, in response to gag stimulation. Increased CD38 expression was positively correlated with the frequency of the IL-10 super(+) population and was also induced by exposure of monocytes to HIV-1 in vitro. Production of IL-10 by HIV-specific CD8 super(+) T cells may represent an adaptive regulatory response to monocyte activation during chronic infection. |
doi_str_mv | 10.1002/eji.201343646 |
format | article |
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Although IL-10 is upregulated throughout HIV-1 infection in multiple cell subsets, whether this is a viral immune evasion strategy or an appropriate response to immune activation is unresolved. Analysis of IL-10 production at the single cell level in 51 chronically infected subjects (31 antiretroviral (ART) naive and 20 ART treated) showed that a subset of CD8 super(+) T cells with a CD25 super(neg) FoxP3 super(neg) phenotype contributes substantially to IL-10 production in response to HIV-1 gag stimulation. The frequencies of gag-specific IL-10- and IFN-[gamma]-producing T cells in ART-naive subjects were strongly correlated and the majority of these IL-10 super(+) CD8 super(+) T cells co-produced IFN-[gamma]; however, patients with a predominant IL-10 super(+)/IFN-[gamma] super(neg) profile showed better control of viraemia. Depletion of HIV-specific CD8 super(+) IL-10 super(+) cells from PBMCs led to upregulation of CD38 on CD14 super(+) monocytes together with increased IL-6 production, in response to gag stimulation. Increased CD38 expression was positively correlated with the frequency of the IL-10 super(+) population and was also induced by exposure of monocytes to HIV-1 in vitro. 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Depletion of HIV-specific CD8 super(+) IL-10 super(+) cells from PBMCs led to upregulation of CD38 on CD14 super(+) monocytes together with increased IL-6 production, in response to gag stimulation. Increased CD38 expression was positively correlated with the frequency of the IL-10 super(+) population and was also induced by exposure of monocytes to HIV-1 in vitro. 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Depletion of HIV-specific CD8 super(+) IL-10 super(+) cells from PBMCs led to upregulation of CD38 on CD14 super(+) monocytes together with increased IL-6 production, in response to gag stimulation. Increased CD38 expression was positively correlated with the frequency of the IL-10 super(+) population and was also induced by exposure of monocytes to HIV-1 in vitro. Production of IL-10 by HIV-specific CD8 super(+) T cells may represent an adaptive regulatory response to monocyte activation during chronic infection.</abstract><doi>10.1002/eji.201343646</doi></addata></record> |
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issn | 0014-2980 1521-4141 |
language | eng |
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source | Wiley-Blackwell Read & Publish Collection |
subjects | Human immunodeficiency virus 1 |
title | Emergence of a distinct HIV-specific IL-10-producing CD8 super(+) T-cell subset with immunomodulatory functions during chronic HIV-1 infection |
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