Nuclear receptor Nr4a1 modulates both regulatory T-cell (Treg) differentiation and clonal deletion

Fassett, Marlys S.; Jiang, Wanlin; D’Alise, Anna Morena; Mathis, Diane; Benoist, Christophe

doi:10.1073/pnas.1200090109

Cited by 109 publications

(131 citation statements)

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“…Previous studies have concluded that deficiency in Nur77 alone does not impair UbA-mediated clonal deletion, perhaps due to redundant functions of its family member Nor-1 (also known as Nr4a3) (23,28,29). However, recent data suggest that Nur77 deficiency is sufficient to impair TRA-mediated clonal deletion (27), arguing against complete redundancy by Nor-1 in some contexts.…”

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confidence: 99%

“…Furthermore, overexpression of Nur77 results in dramatic decreases in thymocyte numbers and an increased frequency of thymocytes with DNA fragmentation (23). Two mechanisms of Nur77-mediated death have suggested: induction of proapoptotic genes through its role as a transcription factor in the nucleus and conversion of Bcl-2 to a proapoptotic form via exposure of its Bcl-2 homology domain 3 (BH3) at mitochondria (24)(25)(26)(27). Previous studies have concluded that deficiency in Nur77 alone does not impair UbA-mediated clonal deletion, perhaps due to redundant functions of its family member Nor-1 (also known as Nr4a3) (23,28,29).…”

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Differential Roles for Bim and Nur77 in Thymocyte Clonal Deletion Induced by Ubiquitous Self-Antigen

Baldwin

2015

The Journal of Immunology

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Negative selection, primarily mediated through clonal deletion of self-reactive thymocytes, is critical for establishing self-tolerance and preventing autoimmunity. Recent studies suggest that the molecular mechanisms of negative selection differ depending on the thymic compartment and developmental stage at which thymocytes are deleted. Using the physiological HYcd4 TCR transgenic model of negative selection against ubiquitous self-antigen, we previously found that one of the principal mediators implicated in clonal deletion, Bim, is required for caspase-3 activation but is ultimately dispensable for negative selection. On the basis of these data, we hypothesized that Nur77, another molecule thought to be a key mediator of clonal deletion, could be responsible for Bim-independent deletion. Despite comparable Nur77 induction in thymocytes during negative selection, Bim deficiency resulted in an accumulation of high-affinity–signaled thymocytes as well as impairment in caspase-mediated and caspase-independent cell death. Although these data suggested that Bim may be required for Nur77-mediated cell death, we found that transgenic Nur77 expression was sufficient to induce apoptosis independently of Bim. However, transgenic Nur77-induced apoptosis was significantly inhibited in the context of TCR signaling, suggesting that endogenous Nur77 could be similarly regulated during negative selection. Although Nur77 deficiency alone did not alter positive or negative selection, combined deficiency in Bim and Nur77 impaired clonal deletion efficiency and significantly increased positive selection efficiency. Collectively, these data shed light on the different roles for Bim and Nur77 during ubiquitous Ag-mediated clonal deletion and highlight potential differences from their reported roles in tissue-restricted Ag-mediated clonal deletion.

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confidence: 99%

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Differential Roles for Bim and Nur77 in Thymocyte Clonal Deletion Induced by Ubiquitous Self-Antigen

Baldwin

2015

The Journal of Immunology

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“…33 Unlike the dramatic reduction of both total thymic cellularity and the percentage of the CD24 lo Vα2 hi population in non-transgenic littermate control (NLC) mice, negative selection was impaired in Twist2-Tg mice (Figures 5b-d).…”

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confidence: 97%

“…Nur77 is required for the negative selection in OT2-TCR × mOVA-Tg mice system. 33,34 To determine whether Twist2 regulates Nur77 induction in this system, we measured Nur77 levels in the CD24 lo Vα2 hi CD4 + population (Figure 6a). In OT2-TCR × mOVA-Tg mice, both the percentage of Nur77 hi cells and the expression of Nur77 were significantly increased compared with OT2-TCR-Tg mice (Figures 6a-c).…”

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confidence: 99%

Expression of Twist2 is controlled by T-cell receptor signaling and determines the survival and death of thymocytes

Lee

et al. 2016

Cell Death Differ

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Self-reactive thymocytes are eliminated by negative selection, whereas competent thymocytes survive by positive selection. The strength of the T-cell receptor (TCR) signal determines the fate of thymocytes undergoing either positive or negative selection. The TCR signal strength is relatively higher in negative selection than in positive selection and induces pro-apoptotic molecules such as Nur77 and Nor-1, which are members of the orphan nuclear receptor family, that then cause TCR-mediated apoptosis. However, at the molecular level, it remains unclear how positive or negative selection is distinguished based on the TCR signal. We found that the expression of Twist2 is differentially regulated in positively and negatively selected thymocytes. In particular, TCR signal strength that elicits positive selection induces Twist2 expression via the Ca 2+ -Cacineurin-NFATc3 pathway, whereas strength of the TCR signal that results in negative selection abolishes NFATc3-dependent Twist2 induction via specific activation of the JNK pathway. Using Twist2-deficient and Twist2 transgenic mice, we also found that Twist2 determines thymocyte sensitivity to TCR-mediated apoptosis by regulating the expression of Nur77 and Nor-1. Twist2 partially retains histone deacetylase 7 (HDAC7) in the nucleus and recruits it to the Nur77 promoter region to repress Nur77 in positively selected thymocytes. Thus our results suggest a molecular mechanism of how thymocytes interpret the strength of the TCR signal and how TCR sensitivity is controlled during thymic selection.

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“…Nevertheless, little is known about Nor-1 compared to Nur77. Recently, Nur77 deficiency alone has also been shown to impair negative selection (Fassett et al 2012). The MEK5-ERK5 pathway has been reported to induce Nur77 expression in thymocytes and DO11.10 cells (Kasler et al 2000;Sohn et al 2008).…”

Section: Programmed Cell Death In T Cell Development 139mentioning

confidence: 99%

Programmed Cell Death in T Cell Development

Hu¹,

Baldwin²

2013

Apoptosis

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Nuclear receptor Nr4a1 modulates both regulatory T-cell (Treg) differentiation and clonal deletion

Cited by 109 publications

References 50 publications

Differential Roles for Bim and Nur77 in Thymocyte Clonal Deletion Induced by Ubiquitous Self-Antigen

Differential Roles for Bim and Nur77 in Thymocyte Clonal Deletion Induced by Ubiquitous Self-Antigen

Expression of Twist2 is controlled by T-cell receptor signaling and determines the survival and death of thymocytes

Programmed Cell Death in T Cell Development

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