NIK-dependent RelB Activation Defines a Unique Signaling Pathway for the Development of Vα14<i>i</i> NKT Cells

Elewaut, Dirk; Shaikh, Raziya B.; Hammond, Kirsten J. L.; Winter, Hilde De; Leishman, Andrew J.; Sidobre, Stéphane; Turovskaya, Olga; Prigozy, Theodore I.; Ma, Lisa; Banks, Theresa A.; Lo, David; Ware, Carl F.; Cheroutre, Hilde; Kronenberg, Mitchell

doi:10.1084/jem.20030141

Cited by 112 publications

(103 citation statements)

References 60 publications

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“…Based on the findings that production of p52 is impaired in NIK aly/aly thymic stroma (Fig. 1C) and that NIK has been demonstrated necessary for the production of NK T cells through the action of RelB (43,44), we further speculate that the NIK-related signaling pathway(s) activate the NF-B complex in thymic stroma mainly consisting of p52/RelB heterodimers to generate the thymic microenvironment that is necessary for the establishment of self-tolerance. The molecular link between the NF-B activation pathway and the regulatory mechanisms of the thymic microenvironment as well as of autoimmunity requires further study.…”

Section: Discussionmentioning

confidence: 62%

NF-κB-Inducing Kinase Establishes Self-Tolerance in a Thymic Stroma-Dependent Manner

Kajiura¹,

Sun²,

Nomura

et al. 2004

The Journal of Immunology

197

225

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Physical contact between thymocytes and the thymic stroma is essential for T cell maturation and shapes the T cell repertoire in the periphery. Stromal elements that control these processes still remain elusive. We used a mouse strain with mutant NF-κB-inducing kinase (NIK) to examine the mechanisms underlying the breakdown of self-tolerance. This NIK-mutant strain manifests autoimmunity and disorganized thymic structure with abnormal expression of Rel proteins in the stroma. Production of immunoregulatory T cells that control autoreactive T cells was impaired in NIK-mutant mice. The autoimmune disease seen in NIK-mutant mice was reproduced in athymic nude mice by grafting embryonic thymus from NIK-mutant mice, and this was rescued by supply of exogenous immunoregulatory T cells. Impaired production of immunoregulatory T cells by thymic stroma without normal NIK was associated with altered expression of peripheral tissue-restricted Ags, suggesting an essential role of NIK in the thymic microenvironment in the establishment of central tolerance.

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Section: Discussionmentioning

confidence: 62%

NF-κB-Inducing Kinase Establishes Self-Tolerance in a Thymic Stroma-Dependent Manner

Kajiura¹,

Sun²,

Nomura

et al. 2004

The Journal of Immunology

197

225

View full text Add to dashboard Cite

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“…In the thymus, the generation of early NK1.1 À natural killer T cell (NKT) precursors is dependent on RelB expression in radiation-resistant thymic stromal cells (Elewaut et al, 2003;Sivakumar et al, 2003), whereas T-cell-intrinsic expression of RelB is necessary for the proliferation and survival of single positive thymocytes during the final stages of development (Guerin et al, 2002). In mature CD4 þ T cells, RelB is required for normal Th1 function and IFNg production, with impaired Th1 differentiation of relb À/À T cells linked to a decrease in Stat4 expression (Corn et al, 2005).…”

Section: Relbmentioning

confidence: 99%

Unravelling the complexities of the NF-κB signalling pathway using mouse knockout and transgenic models

et al. 2006

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The nuclear factor-jB (NF-jB) signalling pathway serves a crucial role in regulating the transcriptional responses of physiological processes that include cell division, cell survival, differentiation, immunity and inflammation. Here we outline studies using mouse models in which the core components of the NF-jB pathway, namely the IjB kinase subunits (IKKa, IKKb and NEMO), the IjB proteins (IjBa, IjBb, IjBe and Bcl-3) and the five NF-jB transcription factors (NF-jB1, NF-jB2, c-Rel, RelA and RelB), have been genetically manipulated using transgenic and knockout technology.

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“…The convergence of signaling factors influencing Aire expression and NKT development is perhaps best illustrated in mice lacking NF-kB family members such as RelB or NIK [2]. These mice have significantly reduced levels of Aire [20] and NKT cells [21,22], but relatively normal conventional T-cell numbers. A similar correlation between Aire expression and NKT cell numbers was reported in lymphotoxin-deficient mice [23,24], although the link between the expression of lymphotoxin and Aire-dependent genes has been disputed in more recent studies [25][26][27].…”

Section: Introductionmentioning

confidence: 99%

NKT cell development in the absence of the autoimmune regulator gene (Aire)

et al. 2008

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Autoimmune regulator gene (Aire)-deficient mice develop an array of autoimmune lesions that reflect failures of immune tolerance. Negative selection is clearly compromised in these mice, but there is evidence to suggest that other mechanisms of tolerance might also be affected, including a possible impairment of regulatory T cell (Treg) development. Studies to date have failed to demonstrate any significant impact on the development or function of the FOXP3 1 Treg compartment, but NKT cells represent a distinct regulatory cell lineage that also develop in the thymus and which are known to influence selftolerance. Aire-related defects coincide with NKT cell deficiencies in a number of animal models, but the direct consequence of Aire-deficiency on NKT cell development has not been established. In this study, we demonstrate that the frequency, distribution and cytokine production of NKT cells and their subsets is principally normal in Aire-deficient mice. We conclude that Aire has little or no effect on regulatory T cell development in general and NKT cells in particular.

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NIK-dependent RelB Activation Defines a Unique Signaling Pathway for the Development of Vα14i NKT Cells

Cited by 112 publications

References 60 publications

NF-κB-Inducing Kinase Establishes Self-Tolerance in a Thymic Stroma-Dependent Manner

NF-κB-Inducing Kinase Establishes Self-Tolerance in a Thymic Stroma-Dependent Manner

Unravelling the complexities of the NF-κB signalling pathway using mouse knockout and transgenic models

NKT cell development in the absence of the autoimmune regulator gene (Aire)

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