Comparison of stable human Treg and Th clones by transcriptional profiling

Stockis, Julie; Fink, Wolfram; François, Violaine; Connerotte, Thierry; Smet, Charles De; Knoops, Laurent; Bruggen, Pierre van der; Boon, Thierry; Coulie, Pierre G.; Lucas, Sophie

doi:10.1002/eji.200838807

Cited by 65 publications

(110 citation statements)

References 52 publications

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“…4 shows that stimulation of activated CD25 þ cells with L. infantum or P. falciparum extracts, in the absence of any support of external TGF-b, induces phosphorylation of SMAD 2/3 proteins. In contrast, the same parasitic extracts do not activate SMAD 2/3 phosphorylation in activated CD25 À cells which express TGF-b receptor but do not express membranebound latent TGF-b [29,30].…”

Section: Effect Of Parasitic Extracts On the Activation Of Membrane-bmentioning

confidence: 80%

“…TGF-b plays a key role in maintaining the balance between immunoprotection mediated by T cells and immunopathology either in experimental models of malaria and toxoplasma infection and in human diseases [5,29,30]. Macrophages and dendritic cells mostly account for TGF-b production following parasite uptake; nevertheless, the production of these cytokines by activated CD4 þ T cells following a direct stimulation with parasites or parasite products has also been reported [10,11,15].…”

Section: Discussionmentioning

confidence: 99%

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Effects of soluble extracts from Leishmania infantum promastigotes, Toxoplasma gondii tachyzoites on TGF-β mediated pathways in activated CD4+ T lymphocytes

Clemente

Severini

Castronovo

et al. 2014

Microbes and Infection

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Interference with transforming growth factor-b-mediated pathways helps several parasites to survive for long periods in immunocompetent hosts. Macrophages and dendritic cells infected by Toxoplasma, Leishmania and Plasmodium spp. produce large amounts of transforming growth factor-b and induce the differentiation of antigen-specific T-regulatory cells. Mechanisms not mediated by antigen-presentation could also account for the expansion of T-regulatory cells in parasitic diseases and they also might be mediated through transforming growth factor-breceptor activated pathways. We explored the properties of soluble extracts from Leishmania infantum promastigotes, Toxoplasma gondii tachyzoites, Trichinella spiralis muscle larvae to expand the pool of T-regulatory cells in a population of polyclonally activated T cells in the absence of accessory cells, and compared their effects to those induced by Plasmodium falciparum extracts. Similarly to P. falciparum, L. infantum extracts activate the latent soluble form of transforming growth factor-b and that bound to the membrane of activated T lymphocytes. The interaction of the active cytokine with transforming growth factor-b receptor induces Foxp3 expression by activated lymphocytes, favoring their conversion through the T-regulatory phenotype. Both Toxoplasma gondii and L. infantum extracts are able to induce transforming growth factor-b production by activated T cells in the absence of accessory cells.

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Section: Effect Of Parasitic Extracts On the Activation Of Membrane-bmentioning

confidence: 80%

Section: Discussionmentioning

confidence: 99%

Effects of soluble extracts from Leishmania infantum promastigotes, Toxoplasma gondii tachyzoites on TGF-β mediated pathways in activated CD4+ T lymphocytes

Clemente

Severini

Castronovo

et al. 2014

Microbes and Infection

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“…The converted DNA was then analyzed by real-time PCR for the methylated and the unmethylated forms of Foxp3 intron 1 as described previously (22). The results are expressed as percentages of unmethylated Foxp3 sequences, calculated as follows: % of demethylation = 2 ΔCt /(1 + 2 ΔCt ), wherein ΔCt = (Ct with methylated primers) 2 (Ct with unmethylated primers).…”

Section: Foxp3 Intron 1 Demethylation Analysis Of Cd4 + T Cell Clonesmentioning

confidence: 99%

Human Tumor Antigen-Specific Helper and Regulatory T Cells Share Common Epitope Specificity but Exhibit Distinct T Cell Repertoire

Fourcade¹,

Sun²,

Kudela³

et al. 2010

The Journal of Immunology

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CD4+ regulatory T cells (Tregs) accumulate at tumor sites and play a critical role in the suppression of immune responses against tumor cells. In this study, we show that two immunodominant epitopes derived from the tumor Ags (TAs) NY-ESO-1 and TRAG-3 stimulate both CD4+ Th cells and Tregs. TA-specific Tregs inhibit the proliferation of allogenic T cells, act in a cell-to-cell contact dependent fashion and require activation to suppress IL-2 secretion by T cells. TRAG-3 and NY-ESO-1–specific Tregs exhibit either a Th1-, a Th2-, or a Th0-type cytokine profile and dot not produce IL-10 or TGF-β. The Foxp3 levels vary from one Treg clone to another and are significantly lower than those of CD4+CD25high Tregs. In contrast to NY-ESO-1–specific Th cells, the NY-ESO-1–specific and TRAG-3–specific Treg clonotypes share a common TCR CDR3 Vβ usage with Foxp3+CD4+CD25high and CD4+CD25− T cells and were not detectable in PBLs of other melanoma patients and of healthy donors, suggesting that their recruitment occurs through the peripheral conversion of CD4+CD25− T cells upon chronic Ag exposure. Collectively, our findings demonstrate that the same epitopes spontaneously stimulate both Th cells and Tregs in patients with advanced melanoma. They also suggest that TA-specific Treg expansion may be better impaired by therapies aimed at depleting CD4+CD25high Tregs and preventing the peripheral conversion of CD4+CD25− T cells.

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“…Analyzing their transcriptional profiles, we demonstrated that activated human Tregs, but not other T cells, produced active TGF-ß1. 2 A possible contribution of soluble TGF-ß1 to immunosuppression by Tregs was in line with the fatal autoimmune phenotype of Tgfb1 -/-mice, but not with the contact dependency of immunosuppression by Tregs. But then we observed that TGF-ß1-signaling in T cells co-cultured with Tregs was also contactdependent, suggesting that active TGF-ß1 was produced close to the Treg surface.…”

mentioning

confidence: 81%

“…But then we observed that TGF-ß1-signaling in T cells co-cultured with Tregs was also contactdependent, suggesting that active TGF-ß1 was produced close to the Treg surface. 2 This prompted us to study the mechanisms of TGF-ß1 activation by Tregs. Indeed, most cells produce inactive forms of TGF-ß1 but very few activate the cytokine, via tightly regulated mechanisms that are cell-type specific.…”

mentioning

confidence: 99%