Licensed human natural killer cells aid dendritic cell maturation via TNFSF14/LIGHT

Holmes, Tim D.; Wilson, Erica; Black, Emma; Benest, Andrew V.; Vaz, Candida; Tan, Betty; Tanavde, Vivek; Cook, Graham P.

doi:10.1073/pnas.1411072112

Cited by 63 publications

(50 citation statements)

References 68 publications

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“…45)), neutrophils (for example, TNF-α46), ILC2 cells (for example, leukotrienes47) and lung structural cells (for example, histamine, leukotrienes and TNF-α4849). Indeed, by being one of the first cells to respond to Ag challenge (via IgE bound to their FcɛRI) and by also being responsive to TNFSF14, which might be produced at sites of developing inflammation by many cells, including various myeloid or lymphoid cells205051 that can be recruited in part in response to MC-derived mediators, MCs might function as powerful local amplifiers of airway responses to Ag.…”

Section: Discussionmentioning

confidence: 99%

A TNFRSF14-FcɛRI-mast cell pathway contributes to development of multiple features of asthma pathology in mice

et al. 2016

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Asthma has multiple features, including airway hyperreactivity, inflammation and remodelling. The TNF superfamily member TNFSF14 (LIGHT), via interactions with the receptor TNFRSF14 (HVEM), can support TH2 cell generation and longevity and promote airway remodelling in mouse models of asthma, but the mechanisms by which TNFSF14 functions in this setting are incompletely understood. Here we find that mouse and human mast cells (MCs) express TNFRSF14 and that TNFSF14:TNFRSF14 interactions can enhance IgE-mediated MC signalling and mediator production. In mouse models of asthma, TNFRSF14 blockade with a neutralizing antibody administered after antigen sensitization, or genetic deletion of Tnfrsf14, diminishes plasma levels of antigen-specific IgG1 and IgE antibodies, airway hyperreactivity, airway inflammation and airway remodelling. Finally, by analysing two types of genetically MC-deficient mice after engrafting MCs that either do or do not express TNFRSF14, we show that TNFRSF14 expression on MCs significantly contributes to the development of multiple features of asthma pathology.

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Section: Discussionmentioning

confidence: 99%

A TNFRSF14-FcɛRI-mast cell pathway contributes to development of multiple features of asthma pathology in mice

et al. 2016

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“…Upon recognition of target cells, NK cells upregulate their cell surface expression of LIGHT. LIGHT-expressing NK cells were able to induce upregulation of CD86 on the surface of autologous DC in a cytokine-independent manner (Holmes et al, 2014). Thus in addition to playing a role in the recruitment of lymphocytes to the TME, LIGHT appears to also have a direct role in priming anti-tumor immune responses, pointing to LIGHT as a potential therapeutic agent to be explored in the clinic.…”

Section: Cues For Tls Developmentmentioning

confidence: 99%

Therapeutic Lymphoid Organogenesis in the Tumor Microenvironment

Weinstein

Storkus

2015

Advances in Cancer Research

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The inflammatory status of the tumor microenvironment (TME) has been heavily investigated in recent years. Chemokine and cytokine signaling pathways such as CCR7, CXCR5, lymphotoxin, and IL-36, which are involved in the generation of secondary lymphoid organs and effector immune responses, are now recognized as having value both as prognostic factors and as immunomodulatory therapeutics in the context of cancer. Furthermore, when produced in the TME, these mediators have been shown to promote the recruitment of immune cells, including T cells, B cells, dendritic cells (DC), and other specialized immune cell subsets such as follicular dendritic cells (FDC) and T follicular helper (Tfh) cells, in association with the formation of “tertiary” lymphoid structures (TLS) within or adjacent to sites of disease. Although TLS are composed of a heterogeneous collection of immune cell types, whose composition differs based on cancer subtype, the qualitative presence of TLS has been shown to represent a biomarker of good prognosis for cancer patients. A comprehensive understanding of the role each of these pathways plays within the TME may support the rational design of future immunotherapies to selectively promote/bolster TLS formation and function, leading to improved clinical outcomes across the vast range of solid cancer types.

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“…LTab/LTbR and CD40/CD40L interactions appear to be the most relevant, while LIGHT provides a second layer of regulation. 20,21,22,66,67,68 Between LIGHT/LTbR and LIGHT/HVEM, the predominant interaction is the former, because LTbR outcompetes HVEM due its higher affinity for LIGHT. 12 Indirectly, LTbR signaling in stromal cells is also important for maintaining the integrity of lymphoid tissue, which is indispensable for the development of the immune response.…”

Section: Discussionmentioning

confidence: 99%

“…16,17,18 and from the phenotype of LIGHT-deficient mice, 19,12,17 we postulated that a complete blockade of LIGHT interaction with its receptors would contribute to achieve a more suitable pharmacological control of the allogeneic immune response. LIGHT blockade on T cells would impede its interaction with LTbR or HVEM on dendritic cells, and therefore hinder their maturation, 19,20,21,22 as well as prevent T/T cell collaboration through LIGHT/HVEM interactions that would contribute to maintenance of T cell survival during T cell expansion and differentiation. 23,24,25,26 To confirm this hypothesis, we characterized a set of anti-LIGHT antibodies raised in LIGHT-deficient mice and chose one that fully blocked the binding of soluble LTbR or HVEM to membrane LIGHT.…”

Section: Introductionmentioning

confidence: 99%

Immunotherapeutic targeting of LIGHT/LTβR/HVEM pathway fully recapitulates the reduced cytotoxic phenotype of LIGHT-deficient T cells

Rio

Fernández-Renedo

Chaloin

et al. 2016

mAbs

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(2016) Immunotherapeutic targeting of LIGHT/LTβR/HVEM pathway fully recapitulates the reduced cytotoxic phenotype of LIGHT-deficient T cells, mAbs, 8:3, 478-490, DOI: 10.1080/19420862.2015 To link to this article: https://doi.org/10. 1080/19420862.2015 ABSTRACTTumor necrosis factor (TNF)/TNF receptor (TNFR) superfamily members play essential roles in the development of the different phases of the immune response. Mouse LIGHT (TNFSF14) is a type II transmembrane protein with a C-terminus extracellular TNF homology domain (THD) that assembles in homotrimers and regulates the course of the immune responses by signaling through 2 receptors, the herpes virus entry mediator (HVEM, TNFSFR14) and the lymphotoxin b receptor (LTbR, TNFSFR3). LIGHT is a membrane-bound protein transiently expressed on activated T cells, natural killer (NK) cells and immature dendritic cells that can be proteolytically cleaved by a metalloprotease and released to the extracellular milieu. The immunotherapeutic potential of LIGHT blockade was evaluated in vivo. Administration of an antagonist of LIGHT interaction with its receptors attenuated the course of graftversus-host reaction and recapitulated the reduced cytotoxic activity of LIGHT-deficient T cells adoptively transferred into non-irradiated semiallogeneic recipients. The lack of LIGHT expression on donor T cells or blockade of LIGHT interaction with its receptors slowed down the rate of T cell proliferation and decreased the frequency of precursor alloreactive T cells, retarding T cell differentiation toward effector T cells. The blockade of LIGHT/LTbR/HVEM pathway was associated with delayed downregulation of interleukin-7Ra and delayed upregulation of inducible costimulatory molecule expression on donor alloreactive CD8 T cells that are typical features of impaired T cell differentiation. These results expose the relevance of LIGHT/LTbR/HVEM interaction for the potential therapeutic control of the allogeneic immune responses mediated by alloreactive CD8 T cells that can contribute to prolong allograft survival.Abbreviations: LIGHT, homologous to lymphotoxin, exhibits inducible expression and competes with HSV glycoprotein D for binding to herpesvirus entry mediator, a receptor expressed on T

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Licensed human natural killer cells aid dendritic cell maturation via TNFSF14/LIGHT

Cited by 63 publications

References 68 publications

A TNFRSF14-FcɛRI-mast cell pathway contributes to development of multiple features of asthma pathology in mice

A TNFRSF14-FcɛRI-mast cell pathway contributes to development of multiple features of asthma pathology in mice

Therapeutic Lymphoid Organogenesis in the Tumor Microenvironment

Immunotherapeutic targeting of LIGHT/LTβR/HVEM pathway fully recapitulates the reduced cytotoxic phenotype of LIGHT-deficient T cells

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