Stability and function of regulatory T cells expressing the transcription factor T-bet

Levine, Andrew G.; Medoza, Alejandra; Hemmers, Saskia; Moltedo, Bruno; Niec, Rachel; Schizas, Michail; Hoyos, Beatrice; Putintseva, Ekaterina V.; Chaudhry, Ashutosh; Dikiy, Stanislav; Fujisawa, Sho; Chudakov, Dmitriy M.; Treuting, Piper M.; Rudensky, Alexander Y.

doi:10.1038/nature22360

Cited by 296 publications

(295 citation statements)

References 31 publications

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“…According to a recent study, it is possible that depletion of RORγt + Treg cells is needed to examine their function rather than deletion of RORγt expression in Treg cells (Levine et al, 2017). However, availability of an experimental system for selective depletion of RORγt + Treg cells in vivo is limited at the moment.…”

Section: Resultsmentioning

confidence: 99%

“…Considering that total ICOS hi Treg cell frequency were not changed after immunization even in the absence of RORγt (Figure 4A), ICOS hi CCR6 − Treg cells might have compensated for the absence of ICOS hi RORγt + CCR6 + Treg cells in RORγ f/f Foxp3 Cre mice. A recent study demonstrated that depletion of T-bet + Treg cells rather than deletion of Tbx21 gene in Treg cells resulted in Th1-dependent immunopathology (Levine et al, 2017). In this regard, selective depletion of RORγt + CCR6 + Treg cells after their development is required to address the functional relevance of the population in EAE as previously suggested (Kim et al, 2007).…”

Section: Discussionmentioning

confidence: 99%

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Generation of RORγt+ Antigen-Specific T Regulatory 17 Cells from Foxp3+ Precursors in Autoimmunity

et al. 2017

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SUMMARY Th17 cells are potent mediators in autoimmune diseases and RORγt is required for their development. Recent studies have shown that RORγt+ Treg cells in the gut regulate intestinal inflammation by inhibiting effector T cell function. In the current study, we report that RORγt+ Treg cells were also found in lymph nodes following immunization. Not only distinct from intestinal RORγt+ Treg in their transcriptomes, peripheral RORγt+ Treg cells were derived from Foxp3+ thymic Treg cells, in an antigen-specific manner. Development of these RORγt+ Treg cells, coined as T regulatory 17 (Tr17) cells, depended on IL-6/Stat3 signaling. Tr17 cells showed suppressive activity against antigen-specific effector T cells in vitro. In addition, Tr17 cells efficiently inhibited myelin-specific Th17 cell-mediated CNS auto-inflammation in a passive EAE model. Collectively, our study demonstrates Tr17 cells as effector Treg cells that potentially restrict autoimmunity.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Generation of RORγt+ Antigen-Specific T Regulatory 17 Cells from Foxp3+ Precursors in Autoimmunity

et al. 2017

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“…This is supported by the detection of lineage‐specific transcription factors (e.g. Tbet,20 IRF421) being co‐expressed with FOXP3 in Treg subsets, using various mouse models, but this has yet to be confirmed in humans. It is possible that the balance of Treg to effector lineages may be altered under specific circumstances or that the Treg themselves may switch fates.…”

Section: Introduction: the Treg Phenotypementioning

confidence: 99%

Unravelling the molecular basis for regulatory T‐cell plasticity and loss of function in disease

et al. 2018

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Regulatory T cells (Treg) are critical for preventing autoimmunity and curtailing responses of conventional effector T cells (Tconv). The reprogramming of T‐cell fate and function to generate Treg requires switching on and off of key gene regulatory networks, which may be initiated by a subtle shift in expression levels of specific genes. This can be achieved by intermediary regulatory processes that include microRNA and long noncoding RNA‐based regulation of gene expression. There are well‐documented microRNA profiles in Treg and Tconv, and these can operate to either reinforce or reduce expression of a specific set of target genes, including FOXP3 itself. This type of feedforward/feedback regulatory loop is normally stable in the steady state, but can alter in response to local cues or genetic risk. This may go some way to explaining T‐cell plasticity. In addition, in chronic inflammation or autoimmunity, altered Treg/Tconv function may be influenced by changes in enhancer–promoter interactions, which are highly cell type‐specific. These interactions are impacted by genetic risk based on genome‐wide association studies and may cause subtle alterations to the gene regulatory networks controlled by or controlling FOXP3 and its target genes. Recent insights into the 3D organisation of chromatin and the mapping of noncoding regulatory regions to the genes they control are shedding new light on the direct impact of genetic risk on T‐cell function and susceptibility to inflammatory and autoimmune conditions.

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“…In line with the idea that TCR signaling strength is driving the transcriptional difference between CD5 hi and CD5 lo islet Tregs, CD5 hi Tregs from the islets showed a significant increase in expression of genes associated with TCR signaling (Zap70), as well as genes regulated by Nur77 directly downstream of TCR activation (Helios, Tnfrsf9, Itgae, Cst7) (30) ( Figure 3D). Moreover, many of the genes associated with Treg-suppressive function that were upregulated in CD5 hi islet Tregs were previously shown to be under the control of TCR (Ctla4, Icos, Lag3, Il10, Tigit) ( Figure 3E) (17,31). Interestingly, CD5…”

Section: Among the 1328 Genetic Transcripts Increased In Cd5mentioning

confidence: 99%

“…Overall, this suggests that high TCR self-reactivity drives Treg functional potential in the islets. Recent studies have shown that Tregs expressing T-bet and CXCR3 are indispensable for the control of Th1 immune responses, including autoimmune diabetes (31,32). Interestingly, CD5…”

Section: Among the 1328 Genetic Transcripts Increased In Cd5mentioning

confidence: 99%

High self-reactivity drives T-bet and potentiates Treg function in tissue-specific autoimmunity

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et al. 2018

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Stability and function of regulatory T cells expressing the transcription factor T-bet

Cited by 296 publications

References 31 publications

Generation of RORγt+ Antigen-Specific T Regulatory 17 Cells from Foxp3+ Precursors in Autoimmunity

Generation of RORγt+ Antigen-Specific T Regulatory 17 Cells from Foxp3+ Precursors in Autoimmunity

Unravelling the molecular basis for regulatory T‐cell plasticity and loss of function in disease

High self-reactivity drives T-bet and potentiates Treg function in tissue-specific autoimmunity

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