Stimulation of the Intracellular Bacterial Sensor NOD2 Programs Dendritic Cells to Promote Interleukin-17 Production in Human Memory T Cells

Beelen, Astrid J. van; Zelinková, Zuzana; Taanman-Kueter, Esther W. M.; Muller, Femke J. M.; Hommes, Daniël W.; Zaat, Sebastian A. J.; Kapsenberg, Martien L.; Jong, Esther C. de

doi:10.1016/j.immuni.2007.08.013

Cited by 462 publications

(456 citation statements)

References 45 publications

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“…In DC of Crohn's disease patients that are deficient for detection of intracellular PGN derivate and with a lack of sensing MDP, diminished IL-17 was detected [43]. In line with these results it was previously observed that Th17 phenotype could be induced by human monocytes stimulated by hyphae of C. albicans [25], compounds of which are discussed as TLR2 ligands.…”

Section: Discussionsupporting

confidence: 77%

TLR2‐activated human langerhans cells promote Th17 polarization via IL‐1β, TGF‐β and IL‐23

et al. 2009

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Section: Discussionsupporting

confidence: 77%

TLR2‐activated human langerhans cells promote Th17 polarization via IL‐1β, TGF‐β and IL‐23

et al. 2009

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“…Experimental autoimmune disease in many animal models such as EAE, EAU and CIA is induced by immunization with autoantigen in the presence of CFA; this is likely to involve the activation of innate inflammatory cytokines that drive Th1 and Th17 cells. Indeed there is already evidence that pathogens or PAMPs can promote the production of inflammatory cytokines from monocytes and DC, which activate IL-17 production by T cells [14,38,64]. Stimulation of DC with TLR3, TLR4 and TLR9 ligands was found to induce MyD88-dependent production of cytokines that promoted differentiation of IL-17 producing CD4 1 T cells [41].…”

Section: Differentiation and Expansion Of Il-17-secreting Cd4 1 T Cellsmentioning

confidence: 99%

“…38: 2636Immunol. -2649 Th17 cells in response to IL-23 stimulation in vitro [22,38]. Conversely, it was demonstrated that IL-23 could expand a population of IL-17-producing T cells from memory CD4 1 T cells in vitro [37] and IL-23-driven IL-17 secreting cells were pathogenic in EAE [22].…”

Section: Differentiation and Expansion Of Il-17-secreting Cd4 1 T Cellsmentioning

confidence: 99%

“…An independent study reported that IL-1b and IL-6 induced differentiation of naïve human T cells into Th17 cells following co-stimulation with anti-CD3 and anti-CD28 in vitro [51]. These studies found that, unlike murine T cells, human naïve T cells did not differentiate into IL-17-secreting T cells in response to TGF-b and IL-6 in vitro [38,50,52,53]. Furthermore, in a study of patients with genetic traits affecting TGF-b, IL-1, IL-6 and IL-23 production, enhanced TGF-b responses, due to mutations in TGFB1 and TGFBR2, did not alter expression of Th17 cells, whereas mutations in STAT3 and IL-12RB1 impaired dedifferentiation or expansion of Th17 cells in vivo [54].…”

Section: Differentiation and Expansion Of Il-17-secreting Cd4 1 T Cellsmentioning

confidence: 99%

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Induction, function and regulation of IL‐17‐producing T cells

2008

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Recent reports have provided convincing evidence that IL-17-producing T cells play a key role in the pathogenesis of organ-specific autoimmune diseases, a function previously attributed exclusively to IFN-c-secreting Th1 cells. Furthermore, it appears that IL-17-producing T cells can also function with Th1 cells to mediate protective immunity to pathogens. Although much of the focus has been on IL-17-secreting CD4 1 T cells, termed The main function of IL-17-secreting T cells is to mediate inflammation, by stimulating production of inflammatory cytokines, such as TNF-a, IL-1b and IL-6, and inflammatory chemokines that promote the recruitment of neutrophils and macrophages.Key words: Autoimmunity . IL-17 . Infection . Inflammation IntroductionMore than 20 years ago Mosmann and Coffman reported that distinct CD4 1 T-cell subtypes, termed Th1 and Th2 cells, could be distinguished on the basis of cytokine secretion and function [1]. The Th1-Th2 model provided a useful but simplistic basis for our understanding of the mechanisms of immunity to infection and also attempted to explain the role of T cells in the pathogenesis of autoimmunity and allergy/asthma. The original hypothesis was that IFN-g-secreting CD4 1 cells mediated protective immunity to intracellular pathogens by promoting macrophage activation and stimulating production of complement fixing and virus neutralizing antibodies, but also promoted inflammatory responses and mediated the pathology in certain autoimmune diseases. In contrast, CD4 1 T cells that secreted IL-4, IL-5, IL-10 and IL-13 were considered to be the main helper T cells providing help for B-cell production of antibody, especially IgG1 in mice, and mediated protective immunity to extracellular pathogens. These Th2 cells were also anti-inflammatory, controlling Th1 responses, but at the same time mediated allergic reactions and had an inflammatory and pathological role in asthma.The identification of additional T-cell subtypes has led to a shift in the Th1-Th2 paradigm and has helped to explain some anomalies in the original model. In the mid 1990s suppressor T cells were re-discovered as Treg cells and were shown to have a major role in controlling immune responses to self-antigens, thereby preventing autoimmunity. Furthermore, these cells rather than the reciprocal Th1 or Th2 populations were shown to be the major regulator of effector T cells, functioning to maintain self-tolerance, prevent autoimmunity and limit collateral damage during immune responses to pathogens [2,3].There were a number of other observations which could not be explained on the basis of the two Th1 and Th2 subtypes. Mini-ReviewDespite the assumption that Th1 cells mediated autoimmunity, mice deficient in IFN-g or IFN-g receptors were found to have increased susceptibility to EAE and collagen-induced arthritis (CIA) [4,5]. Furthermore, EAE was exacerbated in mice deficient in the Th1 polarizing cytokine, 7]. It was then discovered that mice deficient in the novel IL-12 family member, IL-23 were resistant to EAE [6]....

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“…79 IL-1b plays an important role in activating and sustaining the Th17-mediated response, especially in humans. [107][108][109][110] Considering the central role of Th17 cells in autoimmune diseases including rheumatoid arthritis (RA) and psoriasis, mutations in inflammasome-encoding genes may result in a broad spectrum of Th17 cell-mediated autoimmune disorders, through deregulation of IL-1b secretion. 107,[111][112][113][114][115][116] Genetic variants in several inflammatory genes, including NLRP3, are associated with two forms of autoimmune arthritis: juvenile idiopathic arthritis and RA, characterized by Th17 cells.…”

Section: Adaptive Immunity-mediated Diseasesmentioning

confidence: 99%

The inflammasomes in health and disease: from genetics to molecular mechanisms of autoinflammation and beyond

2011

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Nucleotide-binding oligomerization domain (NOD)-containing protein-like receptors (NLRs) are a recently discovered class of innate immune receptors that play a crucial role in initiating the inflammatory response following pathogen recognition. Some NLRs form the framework for cytosolic platforms called inflammasomes, which orchestrate the early inflammatory process via IL-1b activation. Mutations and polymorphisms in NLR-coding genes or in genetic loci encoding inflammasome-related proteins correlate with a variety of autoinflammatory diseases. Moreover, the activity of certain inflammasomes is associated with susceptibility to infections as well as autoimmunity and tumorigenesis. In this review, we will discuss how identifying the genetic characteristics of inflammasomes is assisting our understanding of both autoinflammatory diseases as well as other immune system-driven disorders.

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Stimulation of the Intracellular Bacterial Sensor NOD2 Programs Dendritic Cells to Promote Interleukin-17 Production in Human Memory T Cells

Cited by 462 publications

References 45 publications

TLR2‐activated human langerhans cells promote Th17 polarization via IL‐1β, TGF‐β and IL‐23

TLR2‐activated human langerhans cells promote Th17 polarization via IL‐1β, TGF‐β and IL‐23

Induction, function and regulation of IL‐17‐producing T cells

The inflammasomes in health and disease: from genetics to molecular mechanisms of autoinflammation and beyond

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