IFN-γ–Producing and IL-17–Producing γδ T Cells Differentiate at Distinct Developmental Stages in Murine Fetal Thymus

Shibata, Kensuke; Yamada, Hisakata; Nakamura, Masataka; Hatano, Shoji; Katsuragi, Yoshihisa; Kominami, Ryo; Yoshikai, Yasunobu

doi:10.4049/jimmunol.1302145

Cited by 67 publications

(75 citation statements)

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“…Lck-GFP mice showed that the Lck protein was expressed in late DN2 (also known as DN2b) cells but not early DN2 (also known as DN2a) cells (41,42). We recently found that gd T cells were generated directly from both DN2a and DN2b stages (14). These results suggested that Cre recombinase driven by proximal Lck promoter might not delete RBP-Jk in DN2a-derived gd T cells, whereas Cre recombinase driven by the Rag-1 promoter almost completely inactivated RBP-Jk in gd expression on gdTCR + thymocytes was analyzed.…”

Section: Discussionmentioning

confidence: 99%

“…They are disproportionately distributed and persist in mucosal epithelia, such as skin, intestine, uterus, and lung, as tissue-associated, long-lived self-renewing cells that are important players in mucosal immunity in infections, wound healing, autoimmune disorders, and tumors (7)(8)(9)(10)(11). Interaction between Notch1 and Dll4 is essential for gd T cell development from T cell precursors, and Notch1 expression is maintained on gd T cells (12)(13)(14). We reported previously that the Notch1-Hes1 pathway is involved in the development of IL-17 + gd T cells in the fetal thymus (15).…”

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confidence: 99%

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A Genome-Wide Analysis Identifies a Notch–RBP-Jκ–IL-7Rα Axis That Controls IL-17–Producing γδ T Cell Homeostasis in Mice

Nakamura

Shibata

Hatano

et al. 2015

The Journal of Immunology

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Notch signaling is an important regulator for the development and function of both αβ and γδ T cells, whereas roles of Notch signaling in T cell maintenance remain unclear. We reported previously that the Notch–Hes1 pathway was involved in the intrathymic development of naturally occurring IL-17–producing (IL-17+) γδ T cells. To gain insight into additional roles for the Notch axis in the homeostasis of γδ T cells, we performed a genome-wide analysis of Notch target genes and identified the novel promoter site of IL-7Rα driven by the Notch–RBP-Jκ pathway. Constitutive Notch signaling had the potential to induce IL-7Rα expression on γδ T cells in vivo, as well as in vitro, whereas conditional deletion of RBP-Jκ abrogated IL-7Rα expression, but not Hes1 expression, by γδ T cells and selectively reduced the pool size of IL-7Rαhigh IL-17+ γδ T cells in the periphery. In the absence of IL-7Rα–mediated signaling, IL-17+ γδ T cells were barely maintained in adult mice. Addition of exogenous IL-7 in vitro selectively expanded IL-17+ γδ T cells. Thus, our results revealed a novel role for the Notch–RBP-Jκ–IL-7Rα axis that is independent of Hes1 for homeostasis of IL-17+ γδ T cells.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

A Genome-Wide Analysis Identifies a Notch–RBP-Jκ–IL-7Rα Axis That Controls IL-17–Producing γδ T Cell Homeostasis in Mice

Nakamura

Shibata

Hatano

et al. 2015

The Journal of Immunology

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“…It remains to be established whether NK receptors as well as other innate receptors are expressed on in vivo on Bcl11b −/− DN3 thymocytes, similar to what was observed on ex vivo generated Bcl11b −/− DN3 thymocytes(16), which may interfere with appropriate signaling required for selection. Though γδT cells were reported to develop in normal numbers in the absence of Bcl11b(26, 27), more recent studies demonstrated that IL-17-producing γδT cells were absent in these mice(29). …”

Section: Bcl11b Is Essential For Multiple Checkpoints During T Celmentioning

confidence: 99%

“…Bcl11b was also identified as a radiation-induced tumor suppressor gene 1 (Rit1) in p53 + thymic lymphomas(24). Years of in depth study revealed that Bcl11b is necessary for several developmental checkpoints, including T cell commitment at DN2 stage(16, 25, 26), survival of DN3 and DP thymocytes(18, 27), β selection at DN3 stage, positive selection of CD4 and CD8 single positive (SP) thymocytes(18, 27, 28), development of Treg(22) and iNKT(23) cells, and most recently development of a subpopulation of γδ T cells(29). In mature T cells Bcl11b was demonstrated to control expansion and effector function of cytotoxic T cells (CTLs)(19), to restrict plasticity of Th17 cells by blocking expression of the Th2 program(21), as well as to control generation of iTreg cells from conventional CD4 + T cells, and overall to control the suppression function of Treg cells(22).…”

Section: Introductionmentioning

confidence: 99%

The Multifaceted Roles of Bcl11b in Thymic and Peripheral T Cells: Impact on Immune Diseases

Avram

Califano

2014

The Journal of Immunology

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The transcription factor Bcl11b is expressed in all T cell subsets and progenitors starting from DN2 stage of T cell development, and regulates critical processes implicated in development, function and survival of many of these cells. Among common roles of Bcl11b in T cell progenitors and mature T cell subsets are the repression of the innate genetic program and to some extent expression maintenance of TCR signaling components. However, Bcl11b also has unique roles in specific T cell populations, suggesting that its functions depend on cell type and activation state of the cell. Here we provide a comprehensive review of the roles of Bcl11b in progenitors, effector T cells, as well as in Tregulatory and iNKT cells, and the impact on immune diseases. While emphasizing common themes, including some that might be extended to skin and neurons, we also describe the control of specific functions in different T cell subsets.

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“…If γδ vs. αβ lineage choice were only determined stochastically, by the luck of rearrangement, then lineage fate should only be settled at the DN3a stage. However, both genetic and single-cell tests of differentiation in vitro show that by the time cells reach the DN3a stage, ready to carry out the definitive V-DJ rearrangements of their TCRβ genes, their ability to give rise to γδ cells has contracted to a small fraction of what it was earlier (Ciofani et al , 2006; Feng et al , 2011; Shibata et al , 2014). This implies that many cells with γδ potential leave the mainstream after the early DN2 stages, even before the peak of TCR gene rearrangement activity.…”

Section: Introduction: T-cell Identity and Processing Of T-cell Prmentioning

confidence: 99%

Forging T-Lymphocyte Identity

Rothenberg

Ungerbäck

Champhekar

2016

Advances in Immunology

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T lymphocyte development branches off from other lymphoid developmental programs through its requirement for sustained environmental signals through the Notch pathway. In the thymus, Notch signaling induces a succession of T-lineage regulatory factors that collectively create the T-cell identity through distinct steps. This process involves both the staged activation of T-cell identity genes and the staged repression of progenitor-cell-inherited regulatory genes once their roles in self-renewal and population expansion are no longer needed. With the recent characterization of Innate Lymphoid Cells (ILCs) that share transcriptional regulation programs extensively with T cell subsets, T-cell identity can increasingly be seen as defined in modular terms, as the processes selecting and actuating effector function are potentially detachable from the processes generating and selecting clonally unique T-cell receptor structures. The developmental pathways of different classes of T cells and ILCs are distinguished by the numbers of prerequisites of gene rearrangement, selection, and antigen contact before the cells gain access to nearly-common regulatory mechanisms for choosing effector function. Here, the major classes of transcription factors that interact with Notch signals during T-lineage specification are discussed in terms of their roles in these programs, the evidence for their spectra of target genes at different stages, and their cross-regulatory and cooperative actions with each other. Specific topics include Notch modulation of PU.1 and GATA-3, PU.1-Notch competition, the relationship between PU.1 and GATA-3, and the roles of E proteins, Bcl11b, and GATA-3 in guiding acquisition of T-cell identity while avoiding redirection to an ILC fate.

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IFN-γ–Producing and IL-17–Producing γδ T Cells Differentiate at Distinct Developmental Stages in Murine Fetal Thymus

Cited by 67 publications

References 50 publications

A Genome-Wide Analysis Identifies a Notch–RBP-Jκ–IL-7Rα Axis That Controls IL-17–Producing γδ T Cell Homeostasis in Mice

A Genome-Wide Analysis Identifies a Notch–RBP-Jκ–IL-7Rα Axis That Controls IL-17–Producing γδ T Cell Homeostasis in Mice

The Multifaceted Roles of Bcl11b in Thymic and Peripheral T Cells: Impact on Immune Diseases

Forging T-Lymphocyte Identity

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