Transcription factors T-bet and Runx3 cooperate to activate Ifng and silence Il4 in T helper type 1 cells

Djuretic, Ivana; Levanon, Ditsa; Negreanu, Varda; Groner, Yoram; Rao, Anjana; Ansel, K. Mark

doi:10.1038/ni1424

Cited by 456 publications

(500 citation statements)

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“…Results assessing in vitro IL-4 secretion were similar to results of the in vivo assays, namely, markedly reduced IL-4 levels were observed in iNKT cells from ThPok-deficient mice both at 2 and 24 h. However, it was noteworthy that iNKT cells from DKO mice produced more IL-4 than iNKT cells from ThPok-deficient mice, although the levels were lower than those produced by iNKT cells from Runx3-deficient and WT mice. The recovered IL-4 production in DKO mice was expected because several studies have reported an inhibitory effect of Runx3 on IL-4 expression in T cells, 33,49 suggesting a similar mechanism of action of Runx3 in iNKT cells. In accord with the findings of IL-17A secretion in response to aGalCer in vivo, the in vitro experiments indicated that ThPok disruption led to significantly higher expression of IL-17A by thymus-derived iNKT cells upon stimulation compared with iNKT cells from Runx3-deficient and WT control mice, whereas the sorted iNKT cells from DKO mice secreted less IL-17A than the iNKT cells from ThPok-deficient mice (Figure 4c).…”

Section: Resultsmentioning

confidence: 93%

“…31,32 Furthermore, Runx3 functions to skew naive CD4 1 T cells toward the Th1 lineage, and Runx3 and T-bet interact to enhance the expression of IFN-c and silence IL-4 in Th1-type cells. 33 Moreover, Runx1 and Runx3 are both involved in IL-17 production by T regulatory cells. 34 Studies in mice have confirmed that in the absence of ThPok, CD4 1 NKT cells completely disappear and a new population of CD8 1 NKT cells emerges; thus, we sought to determine whether Runx1 and Runx3 are involved in the development of CD8 1 iNKT cells in ThPok-deficient mice and whether they play a part in the response of iNKT cells to antigen stimulation.…”

Section: Introductionmentioning

confidence: 99%

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Runt-related transcription factor 3 is involved in the altered phenotype and function in ThPok-deficient invariant natural killer T cells

et al. 2014

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The interplay between the CD4-lineage transcription factor ThPok and the CD8-lineage transcription factor, runt-related transcription factor 3 (Runx3), in T-cell development has been extensively documented. However, little is known about the roles of these transcription factors in invariant natural killer T (iNKT) cell development. CD1d-restricted iNKT cells are committed to the CD4 1 CD8 2 and CD4 2 CD8 2 sublineages, which respond to antigen stimulation with rapid and potent release of T helper (Th) 1 and Th2 cytokines. However, previous reports have demonstrated a new population of CD8 1 NKT cells in ThPok-deficient mice. In the current study, we sought to determine whether Runx3 was involved in the re-expression of CD8 and function of iNKT cells in the absence of ThPok. We used mice lacking Runx3, ThPok or both and verified that Runx3 was partially responsible for the appearance of CD8 1 iNKT cells in ThPok knockout mice. Additionally, Runx3 participated in the immune response mediated by iNKT cells in a model of a-galactosylceramide-induced acute hepatitis. These results indicate that Runx3 is crucial for the phenotypic and functional changes observed in ThPok-deficient iNKT cells. and the canonical T-cell receptor a (TCRa) chain (Va14-Ja18 in mice and V24-J18 in humans) coupled to specific Vb chains (Vb8, Vb7 and Vb2 in mice and Vb11 in humans). These receptors are responsible for the interaction of NKT cells with CD1d molecules expressed on CD4 1 CD8 1 double-positive (DP) thymocytes. 1 NKT cells are classified into type I (defined as invariant (iNKT) or classical NKT cells) and type II based on the antigens recognized by each and their TCR repertoires. 2 Our study focused on type I NKT cells (hereafter referred to as iNKT cells). iNKT cells recognize the glycosphingolipid antigen a-galactosylceramide (a-GalCer) and a-GalCer loading with the tetrameric form of CD1d is often used to define the iNKT cell subset because of the high affinity of CD1d for the iNKT cell TCR. 3 Although iNKT cells originate from CD4 1 CD8 1 (DP) thymocytes 4 and are selected by MHC class

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Section: Resultsmentioning

confidence: 93%

Section: Introductionmentioning

confidence: 99%

Runt-related transcription factor 3 is involved in the altered phenotype and function in ThPok-deficient invariant natural killer T cells

et al. 2014

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“…[22][23][24] Moreover, IL-12 polarizes T cells into a type 1 helper T (Th1) effector cell phenotype. [25][26][27] Th1 polarization is further pronounced by IL-12 inhibiting the developmental program of type 2 helper T cells 28 and interference with the differentiation of regulatory T cells (Tregs) and Th17 cells induced by TGF-b. 29 Additionally, IL-12 programs effector T cells for optimal generation of effector memory T cells and T follicular helper cells.…”

Section: Il-12 Sensing By Innate and Adaptive Lymphocytesmentioning

confidence: 99%

New insights into IL-12-mediated tumor suppression

et al. 2014

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During the past two decades, interleukin-12 (IL-12) has emerged as one of the most potent cytokines in mediating antitumor activity in a variety of preclinical models. Through pleiotropic effects on different immune cells that form the tumor microenvironment, IL-12 establishes a link between innate and adaptive immunity that involves different immune effector cells and cytokines depending on the type of tumor or the affected tissue. The robust antitumor response exerted by IL-12, however, has not yet been successfully translated into the clinics. The majority of clinical trials involving treatment with IL-12 failed to show sustained antitumor responses and were associated to toxic side effects. Here we discuss the therapeutic effects of IL-12 from preclinical to clinical studies, and will highlight promising strategies to take advantage of the antitumor activity of IL-12 while limiting adverse effects.

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“…36,37 Additionally, experiments have shown that master transcription factors form homodimers facilitating cooperative binding to DNA. 38,39 The formation of heterodimeric complexes leads to crossinhibition between master transcription factors. [40][41][42] When these biochemical properties are modelled mathematically, the resulting model includes high and low stable expression states 9,10 (see Box 1).…”

Section: Box 1 Positive Feedback Creates Attractorsmentioning

confidence: 99%

Cell division curtails helper phenotype plasticity and expedites helper T‐cell differentiation

Ham

Boer

2012

Immunol Cell Biol

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Following activation by antigen, helper T cells differentiate into one of many effector phenotypes. Formulating mechanistic mathematical models combining regulatory networks at the transcriptional, translational and epigenetic level, we study how individual helper T cells may adopt their different phenotypes. For each cytokine phenotype, for example, T helper type 1 (Th1) and type 2 (Th2) cells, we find that the intracellular molecular network allows a cell to adopt one of the three states, which we interpret as naive, active and memory states. Cell division markedly speeds up the differentiation into a particular memory state because of DNA demythelation. In a memory state, cells readily resume production of the same cytokine they produced before. Using stochastic models we show that helper T-cell plasticity (that is, the ability to switch phenotype) is low during clonal expansion. Although most memory cells rapidly secrete the original cytokine upon restimulation, some adopt another phenotype and produce different cytokines, allowing for considerable diversity in the phenotypes that are adopted during a memory response. In summary, we show that helper T-cell division expedites cell differentiation by increasing DNA demethylation. We also show that plasticity is low during the clonal expansion phase, but that helper T cells may adopt alternative phenotypes during a memory response. Keywords: epigenetic regulation; helper T-cell phenotypes; mathematical modelling; transcriptional regulation For more than a century, biologists have studied the mechanisms that enable cells to encode genetic information, and how this information is passed on to the cell's progeny. 1 Besides the genetic DNA code of a cell that is replicated faithfully upon every cell division and therefore virtually identical in every cell within an individual, 2 additional 'epigenetic' information fixes differential cell development by prompting daughter cells to express a similar set of genes as their mother cell. 3 This facilitates and thus preserves the differentiation process that the mother cell and its ancestors have undergone as part of cellular diversification within an organism.A variety of biological systems have now been studied using highthroughput technologies, which provide data that allow a better understanding of information processing within a cell. [4][5][6][7] The availability of quantitative data and the apparent complexity of cellular regulatory networks have led to a data-driven mathematical modelling approach that is usually referred to as computational or systems biology. Mathematical models have revealed nonlinearity in genetic networks that allow cells to switch between states. Examples are the Lac operon 8 and cells of the haematopoietic lineage. [9][10][11][12] Recently, epigenetic regulation mediated by histone modification has been studied using similar mathematical models. [13][14][15] At the molecular level these mathematical models describe quite different genetic and epigenetic systems. Mathematically they share im...

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Transcription factors T-bet and Runx3 cooperate to activate Ifng and silence Il4 in T helper type 1 cells

Cited by 456 publications

References 56 publications

Runt-related transcription factor 3 is involved in the altered phenotype and function in ThPok-deficient invariant natural killer T cells

Runt-related transcription factor 3 is involved in the altered phenotype and function in ThPok-deficient invariant natural killer T cells

New insights into IL-12-mediated tumor suppression

Cell division curtails helper phenotype plasticity and expedites helper T‐cell differentiation

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