MHC class II‐independent CD25+ CD4+ CD8α β+ α β T cells attenuate CD4+ T cell‐induced transfer colitis

Krajina, Tamara; Leithäuser, Frank; Reimann, Jörg

doi:10.1002/eji.200324463

Cited by 23 publications

(26 citation statements)

References 44 publications

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“…Treg differentiation requires TCR interactions with MHC-II molecules (ref. 10 and references therein), as engagement of the TCR by agonist ligands during thymic differentiation strongly favors clonal deviation into the FoxP3+ lineage, either by inducing differentiation along the lineage (11) or because FoxP3+ cells are inherently more resistant to clonal deletion (12). Accordingly, the analysis of mice expressing a Nurr77-GFP reporter, whose expression correlates with the strength of cell activation via the TCR, showed that the reporter was generally expressed at a higher level in Treg than in Tconv cells (13).…”

Section: Imbalanced Signal Transduction In Regulatory T Cells Expressmentioning

confidence: 99%

Imbalanced signal transduction in regulatory T cells expressing the transcription factor FoxP3

Yan

Farache

Mingueneau

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

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FoxP3+ T regulatory (Treg) cells have a fundamental role in immunological tolerance, with transcriptional and functional phenotypes that demarcate them from conventional CD4+ T cells (Tconv). Differences between these two lineages in the signaling downstream of T-cell receptor-triggered activation have been reported, and there are different requirements for some signaling factors. Seeking a comprehensive view, we found that Treg cells have a broadly dampened activation of several pathways and signaling nodes upon TCR-mediated activation, with low phosphorylation of CD3ζ, SLP76, Erk1/2, AKT, or S6 and lower calcium flux. In contrast, STAT phosphorylation triggered by interferons, IL2 or IL6, showed variations between Treg and Tconv in magnitude or choice of preferential STAT activation but no general Treg signaling defect. Much, but not all, of the Treg/Tconv difference in TCR-triggered responses could be attributed to lower responsiveness of antigen-experienced cells with CD44hi or CD62Llo phenotypes, which form a greater proportion of the Treg pool. Candidate regulators were tested, but the Treg/Tconv differential could not be explained by overexpression in Treg cells of the signaling modulator CD5, the coinhibitors PD-1 and CTLA4, or the regulatory phosphatase DUSP4. However, transcriptome profiling in Dusp4-deficient mice showed that DUSP4 enhances the expression of a segment of the canonical Treg transcriptional signature, which partially overlaps with the TCR-dependent Treg gene set. Thus, Treg cells, likely because of their intrinsically higher reactivity to self, tune down TCR signals but seem comparatively more attuned to cytokines or other intercellular signals.

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Section: Imbalanced Signal Transduction In Regulatory T Cells Expressmentioning

confidence: 99%

Imbalanced signal transduction in regulatory T cells expressing the transcription factor FoxP3

Yan

Farache

Mingueneau

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

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“…Furthermore, the periphery of MHC II Ϫ/Ϫ mice contains CD8 ϩ CD25 ϩ T cells that exhibit contact-dependent suppressive activity analogous to that mediated by wild-type CD4 ϩ CD25 ϩ T cells (20). Other reports have indicated that a unique subset of CD4 ϩ CD8 ϩ CD25 ϩ T cells in MHC II Ϫ/Ϫ mice is enriched in FoxP3 mRNA and capable of suppressing T cellmediated inflammatory bowel disease (21). Curiously, while prevalent in MHC II Ϫ/Ϫ mice, CD8 ϩ CD25 ϩ T cells are quite rare in wild-type animals (20).…”

Section: Foxp3mentioning

confidence: 99%

Distinct Subsets of FoxP3+ Regulatory T Cells Participate in the Control of Immune Responses

Stephens

Andersson

Shevach

2007

The Journal of Immunology

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Expression of the transcription factor FoxP3 is the hallmark of regulatory T cells that play a crucial role in dampening immune responses. A comparison of the development and phenotype of FoxP3+ T cells in relation to the expression of conventional MHC molecules facilitated the identification of several distinct lineages of naive and effector/memory populations of Foxp3+ T cells. One subpopulation of effector/memory Foxp3+ T cells develops in the thymic medulla, whereas the second is thymic independent. Both lineages display a distinct activated phenotype, undergo extensive steady-state proliferation, home to sites of acute inflammation, and are unique in their capacity to mediate Ag-nonspecific suppression of T cell activation directly ex vivo. Effector FoxP3+ T cells may act as a sentinel of tolerance, providing a first line of defense against potentially harmful responses by rapidly suppressing immunity to peripheral self-Ags.

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“…18 eGFP-tg B6 mice express eGFP under the chicken ␤-actin promoter control. 17 eGFP is heterogeneously expressed from the transgene in the CD4 ϩ T-cell population of transgenic mice but remains stable within the adoptive host.…”

Section: Isolation and Adoptive Transfer Of Gfp ϩ Cd4mentioning

confidence: 99%

“…Twelve l of RNA isolated from microdissected tissue or 1 l of RNA prepared from cell suspensions, respectively, were annealed to 1 pmol of hexamer (random) primer, denatured at 80°C and reverse-transcribed as described. 18 Real-Time PCR mRNA expression was determined by real-time reverse transcriptase (RT)-PCR and relative quantification using the reference gene HPRT or CD3, respectively. Primers for HPRT and Foxp3 were as published elsewhere.…”

Section: Rna Isolation and Reverse Transcriptionmentioning

confidence: 99%

“…18 The tissue was digested with 0.5 mg/ml of collagenase type VIII and 5 U/ml DNase at 37°C for 90 minutes in RPMI 1640/5% v/v fetal calf serum. Lamina propria lymphoid cells were collected at the 40%/70% interface of a Percoll gradient for analysis by flow cytometry or fluorescence-activated cell sorting.…”

Section: Preparation Of Colonic Lamina Propria Cells Flow Cytometry mentioning

confidence: 99%

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Foxp3-Expressing CD103+ Regulatory T Cells Accumulate in Dendritic Cell Aggregates of the Colonic Mucosa in Murine Transfer Colitis

Leithäuser

Meinhardt-Krajina

Fink

et al. 2006

The American Journal of Pathology

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Little is known of the anatomical compartmentalization of colitogenic or regulatory T-cell responses in the murine transfer colitis model. Therefore, we analyzed the putative function of large intestinal dendritic cell (DC) aggregates, to which donor CD4 ؉ T cells selectively home before colitis becomes manifest. The co-stimulatory molecules MHC-II, CD40, CD80, and CD86 were expressed in DC aggregates. IL-23 was primarily absent from DC aggregates at all stages of disease but was expressed at high levels in the severely inflamed lamina propria. Interferon-␥ was up-regulated in the lamina propria during early and advanced disease, whereas in DC aggregates it was detectable to a significant degree only in fully developed colitis. In contrast, Foxp3, a marker of regulatory T cells, was expressed in DC aggregates on T-cell transfer, coinciding with the appearance of CD103 ؉ CD25 ؊ T cells in these clusters. Foxp3 was enriched in the CD103 ؉ T-cell fraction isolated from the lamina propria of diseased mice. T-cell grafts depleted of CD103 ؉ T cells generated similar numbers of colonic CD103؉ T cells as unfractionated T cells. We conclude that DC aggregates are structures involved in the expansion and/or differentiation of CD103 ؉ CD25 ؊ CD4

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MHC class II‐independent CD25⁺ CD4⁺ CD8α β⁺ α β T cells attenuate CD4⁺ T cell‐induced transfer colitis

Cited by 23 publications

References 44 publications

Imbalanced signal transduction in regulatory T cells expressing the transcription factor FoxP3

Imbalanced signal transduction in regulatory T cells expressing the transcription factor FoxP3

Distinct Subsets of FoxP3+ Regulatory T Cells Participate in the Control of Immune Responses

Foxp3-Expressing CD103+ Regulatory T Cells Accumulate in Dendritic Cell Aggregates of the Colonic Mucosa in Murine Transfer Colitis

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