A role for CD4 super(+)CD25 super(+) T cells in regulation of the immune response during human tuberculosis
Active tuberculosis (TB) is associated with prolonged suppression of Mycobacterium tuberculosis (MTB)-specific immune responses, but mechanisms involved are understood incompletely. We investigated a potential role for CD4 super(+)CD25 super(+) regulatory T cells in depressed anti-MTB immunity by ev...
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| Veröffentlicht in: | Clinical and experimental immunology 2006-04, Vol.144 (1), p.25-34 |
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| creator | Ribeiro-Rodrigues, R Resende Co, T Rojas, R Toossi, Z Dietze, R Boom, W H Maciel, E Hirsch, C S |
| description | Active tuberculosis (TB) is associated with prolonged suppression of Mycobacterium tuberculosis (MTB)-specific immune responses, but mechanisms involved are understood incompletely. We investigated a potential role for CD4 super(+)CD25 super(+) regulatory T cells in depressed anti-MTB immunity by evaluating serially CD4 cell phenotype and interferon (IFN)- gamma production by mononuclear cells from patients with TB. At diagnosis, frequencies of CD4 super(+)CD25 super(+) T cells were increased in blood from TB patients compared to healthy purified protein derivative (PPD)-positive controls (with a history of prior TB exposure), and remained elevated at completion of therapy (6 months). By contrast, expression of another activation marker, CD69, by CD4 T cells was increased at diagnosis, but declined rapidly to control levels with treatment. Among CD4 super(+)CD25 super(+) T cells from TB patients at diagnosis those expressing high levels of CD25, probably representing regulatory T cells, were increased 2.9-fold when compared to control subjects, while MTB-stimulated IFN- gamma levels in whole blood supernatants were depressed. A role for CD4 super(+)CD25 super(+) T cells in depressed IFN- gamma production during TB was substantiated in depletion experiments, where CD25 super(+)-depleted CD4 T cells produced increased amounts of IFN- gamma upon MTB stimulation compared to unseparated T cells. At follow-up, IFN- gamma production improved most significantly in blood from TB patients with high baseline frequencies of CD4 super(+)CD25 super(+) T cells (more than threefold higher than controls for both total and CD25 super(hi+) CD4 T cells), who also had a significant drop in frequencies of both total and 'regulatory' CD4 super(+)CD25 super(+) T cells in response to treatment. Expansion of CD4 super(+)CD25 super(+) regulatory T cells during active TB may play a role in depressed T cell IFN- gamma production. |
| doi_str_mv | 10.1111/j.1365-2249.2006.03027.x |
| format | Article |
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We investigated a potential role for CD4 super(+)CD25 super(+) regulatory T cells in depressed anti-MTB immunity by evaluating serially CD4 cell phenotype and interferon (IFN)- gamma production by mononuclear cells from patients with TB. At diagnosis, frequencies of CD4 super(+)CD25 super(+) T cells were increased in blood from TB patients compared to healthy purified protein derivative (PPD)-positive controls (with a history of prior TB exposure), and remained elevated at completion of therapy (6 months). By contrast, expression of another activation marker, CD69, by CD4 T cells was increased at diagnosis, but declined rapidly to control levels with treatment. Among CD4 super(+)CD25 super(+) T cells from TB patients at diagnosis those expressing high levels of CD25, probably representing regulatory T cells, were increased 2.9-fold when compared to control subjects, while MTB-stimulated IFN- gamma levels in whole blood supernatants were depressed. A role for CD4 super(+)CD25 super(+) T cells in depressed IFN- gamma production during TB was substantiated in depletion experiments, where CD25 super(+)-depleted CD4 T cells produced increased amounts of IFN- gamma upon MTB stimulation compared to unseparated T cells. At follow-up, IFN- gamma production improved most significantly in blood from TB patients with high baseline frequencies of CD4 super(+)CD25 super(+) T cells (more than threefold higher than controls for both total and CD25 super(hi+) CD4 T cells), who also had a significant drop in frequencies of both total and 'regulatory' CD4 super(+)CD25 super(+) T cells in response to treatment. 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A role for CD4 super(+)CD25 super(+) T cells in depressed IFN- gamma production during TB was substantiated in depletion experiments, where CD25 super(+)-depleted CD4 T cells produced increased amounts of IFN- gamma upon MTB stimulation compared to unseparated T cells. At follow-up, IFN- gamma production improved most significantly in blood from TB patients with high baseline frequencies of CD4 super(+)CD25 super(+) T cells (more than threefold higher than controls for both total and CD25 super(hi+) CD4 T cells), who also had a significant drop in frequencies of both total and 'regulatory' CD4 super(+)CD25 super(+) T cells in response to treatment. 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A role for CD4 super(+)CD25 super(+) T cells in depressed IFN- gamma production during TB was substantiated in depletion experiments, where CD25 super(+)-depleted CD4 T cells produced increased amounts of IFN- gamma upon MTB stimulation compared to unseparated T cells. At follow-up, IFN- gamma production improved most significantly in blood from TB patients with high baseline frequencies of CD4 super(+)CD25 super(+) T cells (more than threefold higher than controls for both total and CD25 super(hi+) CD4 T cells), who also had a significant drop in frequencies of both total and 'regulatory' CD4 super(+)CD25 super(+) T cells in response to treatment. Expansion of CD4 super(+)CD25 super(+) regulatory T cells during active TB may play a role in depressed T cell IFN- gamma production.</abstract><doi>10.1111/j.1365-2249.2006.03027.x</doi></addata></record> |
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| source | Oxford University Press Journals All Titles (1996-Current); EZB-FREE-00999 freely available EZB journals; PubMed Central; Alma/SFX Local Collection |
| subjects | Mycobacterium tuberculosis |
| title | A role for CD4 super(+)CD25 super(+) T cells in regulation of the immune response during human tuberculosis |
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