CD4
            <sup>+</sup>
            Regulatory T Cells Control T
            <sub>H</sub>
            17 Responses in a Stat3-Dependent Manner

Chaudhry, Ashutosh; Rudra, Dipayan; Treuting, Piper M.; Samstein, Robert M.; Liang, Yuqiong; Kas, Arnold; Rudensky, Alexander Y.

doi:10.1126/science.1172702

Cited by 873 publications

(733 citation statements)

References 28 publications

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“…However, it is not clear whether such Treg cells have intrinsically different suppressive function or whether they share common suppressive properties and the specificity is exerted mainly through local environmental adaptation. The latter hypothesis is supported by the observations that Treg cells isolated from these studies largely show intact suppressive activity in vitro (9)(10)(11)(12). We sought to approach this question by addressing whether transcriptionally diverse Treg cell subsets exist in humans, and whether the diversity accounts for potential differences in their in vitro functionality.…”

Section: Discussionmentioning

confidence: 92%

“…Several key studies have revealed a biased breakdown of tolerance when Treg cells are genetically mutated for particular genes. Specifically, Tregspecific deletion of T-bet, IFN regulatory factor 4, Stat3, and Bcl6 resulted in the impairment of specific regulation of Th1, Th2, Th17, and T follicular helper cells, respectively (9)(10)(11)(12). The finding that the key transcription factors for Th cell differentiation are also required for Treg cells to suppress these Teff cells suggests that the Treg population comprises multiple functional subsets, some of which may have a designated Th cell target.…”

Section: R Egulatory T (Treg) Cells Play a Key Role In Maintainingmentioning

confidence: 95%

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Diverse Gene Expression in Human Regulatory T Cell Subsets Uncovers Connection between Regulatory T Cell Genes and Suppressive Function

Hua

Davis

Hill

et al. 2015

The Journal of Immunology

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Regulatory T (Treg) cells have a critical role in the control of immunity, and their diverse subpopulations may allow adaptation to different types of immune responses. In this study, we analyzed human Treg cell subpopulations in the peripheral blood by performing genome-wide expression profiling of 40 Treg cell subsets from healthy donors. We found that the human peripheral blood Treg cell population is comprised of five major genomic subgroups, represented by 16 tractable subsets with a particular cell surface phenotype. These subsets possess a range of suppressive function and cytokine secretion and can exert a genomic footprint on target effector T (Teff) cells. Correlation analysis of variability in gene expression in the subsets identified several cell surface molecules associated with Treg suppressive function, and pharmacological interrogation revealed a set of genes having causative effect. The five genomic subgroups of Treg cells imposed a preserved pattern of gene expression on Teff cells, with a varying degree of genes being suppressed or induced. Notably, there was a cluster of genes induced by Treg cells that bolstered an autoinhibitory effect in Teff cells, and this induction appears to be governed by a different set of genes than ones involved in counteracting Teff activation. Our work shows an example of exploiting the diversity within human Treg cell subpopulations to dissect Treg cell biology.

show abstract

Section: Discussionmentioning

confidence: 92%

Section: R Egulatory T (Treg) Cells Play a Key Role In Maintainingmentioning

confidence: 95%

Diverse Gene Expression in Human Regulatory T Cell Subsets Uncovers Connection between Regulatory T Cell Genes and Suppressive Function

Hua

Davis

Hill

et al. 2015

The Journal of Immunology

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“…However, all animals have naturally occurring Treg (nTreg) cells that confer basal suppression of effector cell functions; the depletion of nTreg cells results in the induction of autoimmune and/or inflammatory diseases, which are associated with enhanced autoreactive cellular immune responses (61). Therefore, it is common that total Treg cell depletion in mice results in stronger cellular immune responses than do those in Treg cell-competent mice, and this could be observed with any kind of infection (62,63). A strategy to deplete virus-induced Treg cells alone, without affecting the numbers and functions of nTreg cells, would be necessary to precisely determine the role of induced Treg cells in vivo, which has never been demonstrated.…”

Section: Discussionmentioning

confidence: 99%

Premature Terminal Exhaustion of Friend Virus-Specific Effector CD8+ T Cells by Rapid Induction of Multiple Inhibitory Receptors

Takamura¹,

Tsuji-Kawahara²,

Yagita

et al. 2010

The Journal of Immunology

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During chronic viral infection, persistent exposure to viral Ags leads to the overexpression of multiple inhibitory cell-surface receptors that cause CD8+ T cell exhaustion. The severity of exhaustion correlates directly with the level of infection and the number and intensity of inhibitory receptors expressed, and it correlates inversely with the ability to respond to the blockade of inhibitory pathways. Friend virus (FV) is a murine retrovirus complex that induces acute high-level viremia, followed by persistent infection and leukemia development, when inoculated into immunocompetent adult mice. In this article, we provide conclusive evidence that FV infection results in the generation of virus-specific effector CD8+ T cells that are terminally exhausted. Acute FV-induced disease is characterized by a rapid increase in the number of virus-infected erythroblasts, leading to massive splenomegaly. Most of the expanded erythroblasts strongly express programmed death ligand-1 and MHC class I, thereby creating a highly tolerogenic environment. Consequently, FV-specific effector CD8+ T cells uniformly express multiple inhibitory receptors, such as programmed cell death 1 (PD-1), T cell Ig domain and mucin domain 3 (Tim-3), lymphocyte activation gene-3, and CTLA-4, rapidly become nonresponsive to restimulation and are no longer reinvigorated by combined in vivo blockade of PD-1 and Tim-3 during the memory phase. However, combined blockade of PD-1 and Tim-3 during the priming/differentiation phase rescued FV-specific CD8+ T cells from becoming terminally exhausted, resulting in improved CD8+ T cell functionality and virus control. These results highlight FV’s unique ability to evade virus-specific CD8+ T cell responses and the importance of an early prophylactic approach for preventing terminal exhaustion of CD8+ T cells.

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“…13,14 In addition, Treg-specific deletion of the transcription factors IRF4 (interferon regulatory factor 4) or STAT3 (signal transducer and activator of transcription 3) resulted in an impaired regulation of Th2-and Th17-dominated immune responses, respectively. 15,16 Recently, a population of germinal center-resident Tregs, termed follicular regulatory T cells, was identified. 17,18 These follicular regulatory T cells suppress germinal center B and T cells and depend, similar to their follicular T helper cell counterparts, on the expression of the transcription factor Bcl6 for their development.…”

Section: Introductionmentioning

confidence: 99%

Foxp3+ T cells expressing RORγt represent a stable regulatory T-cell effector lineage with enhanced suppressive capacity during intestinal inflammation

et al. 2016

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CD4 ⁺ Regulatory T Cells Control T _H 17 Responses in a Stat3-Dependent Manner

Cited by 873 publications

References 28 publications

Diverse Gene Expression in Human Regulatory T Cell Subsets Uncovers Connection between Regulatory T Cell Genes and Suppressive Function

Diverse Gene Expression in Human Regulatory T Cell Subsets Uncovers Connection between Regulatory T Cell Genes and Suppressive Function

Premature Terminal Exhaustion of Friend Virus-Specific Effector CD8+ T Cells by Rapid Induction of Multiple Inhibitory Receptors

Foxp3+ T cells expressing RORγt represent a stable regulatory T-cell effector lineage with enhanced suppressive capacity during intestinal inflammation

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CD4 + Regulatory T Cells Control T H 17 Responses in a Stat3-Dependent Manner

Cited by 873 publications

References 28 publications

Diverse Gene Expression in Human Regulatory T Cell Subsets Uncovers Connection between Regulatory T Cell Genes and Suppressive Function

Diverse Gene Expression in Human Regulatory T Cell Subsets Uncovers Connection between Regulatory T Cell Genes and Suppressive Function

Premature Terminal Exhaustion of Friend Virus-Specific Effector CD8+ T Cells by Rapid Induction of Multiple Inhibitory Receptors

Foxp3+ T cells expressing RORγt represent a stable regulatory T-cell effector lineage with enhanced suppressive capacity during intestinal inflammation

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Product

Resources

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CD4 ⁺ Regulatory T Cells Control T _H 17 Responses in a Stat3-Dependent Manner