Decreased sensitivity to tumour-necrosis factor but normal T-cell development in TNF receptor-2-deficient mice

Erickson, Sharon; Sauvage, Frédéric J. de; Kikly, Kristine; Carver-Moore, Karen; Pitts-Meek, Sharon; Gillett, Nancy A.; Sheehan, Kathleen C. F.; Schreiber, Robert D.; Goeddel, David V.; Moore, Mark

doi:10.1038/372560a0

Cited by 567 publications

(339 citation statements)

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“…Although the proliferative capacity of TNFR2 À/À and WT CD4 + T cells is comparable, a significant difference in the sensitivity to AICD was noticed. Intriguingly, in the initial characterization of the TNFR2 À/À mouse, an increased resistance to TNF-induced T-cell death was in fact reported [38].…”

Section: Discussionmentioning

confidence: 99%

Lack of TNFR2 expression by CD4⁺ T cells exacerbates experimental colitis

et al. 2009

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TNF plays fundamental roles in the induction and perpetuation of inflammation. The effects of TNF are mediated through TNF receptor (TNFR) 1 or 2. As these two receptors mediate different functions, selective targeting of one receptor may represent a more specific treatment for inflammatory disorders than the complete blocking of TNF. TNFR2 expression is up-regulated in inflammatory bowel disease. Hence, we directly assessed the role of TNFR2 signaling in the CD4 + T-cell transfer model of colitis using TNFR2 À/À or WT mice as donors of colitogenic CD4 + CD45RB hi T cells for transfer into syngeneic RAG2 À/À or RAG2 À/À TNFR2 À/À recipient mice. Although the absence of TNFR2 expression by nonlymphoid cells of the recipient mice does not influence the course of colitis, transfer of TNFR2 À/À CD4 + T cells leads to an accelerated onset of disease and to more severe signs of inflammation. The enhanced colitogenic potential of TNFR2 À/À CD4 1 T cells is associated with reduced activation-induced cell death, resulting in an increased accumulation of TNFR2 À/À CD4 1 T cells. Hence, TNFR2 signaling is crucial for the TNF-dependent contraction of the disease-inducing T cells. Therefore, a selective blocking of TNFR2 may lead to exacerbation rather than attenuation of T-cell-mediated inflammatory disorders.Key words: CD4 1 T cells Á Inflammation Á Intestinal immunity Á TNF Introduction TNF plays a fundamental role in immunity and inflammation based on its pleiotropic effects on differentiation, growth and apoptotic cell death of both immune and non-immune cell subsets [1,2]. It is well established that TNF is also critically involved in the pathogenesis of inflammatory and autoimmune diseases such as rheumatoid arthritis, MS and inflammatory bowel diseases (IBD) [3]. Monocytes and macrophages are the main producers of TNF, but T and B lymphocytes and also mast cells can produce significant amounts of TNF. Interestingly, intestinal cell lines are induced to synthesize TNF upon infection with invasive bacterial strains [4]. TNF mediates its functions by binding as a trimer to either TNF receptor (TNFR) 1 or 2. The binding of TNF trimer to the preassembled TNFR complex leads to conformational changes of the receptors facilitating signal transduction through rapid recruitment of downstream signaling molecules. Both receptors have distinct signal transduction pathways and mediate distinct cellular responses [1,[5][6][7][8][9][10]. The 55 kDa receptor, TNFR1 (also known as p55, p60, TNFRSF1a, CD120a) is expressed on most cell types. The intracellular domain of TNFR1 contains a death domain (DD) that leads to apoptosis through caspase activation. TNFR1 signaling can also mediate transcription of anti-apoptotic proteins, inflammatory cytokines and chemokines through activation of NF-kB. The 75 kDa receptor, TNFR2 (also known as p75, p80, TNFRSF1b, CD120b), is Eur. J. Immunol. 2009. 39: 1743-1753 DOI 10.1002 Cellular immune response 1743 expressed predominantly by haematopoietic cells, but expression by other cell types can be i...

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Section: Discussionmentioning

confidence: 99%

Lack of TNFR2 expression by CD4⁺ T cells exacerbates experimental colitis

et al. 2009

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“…Additionally, bone marrow from knockout mice was also used in this study. Knockout mice were on a C57/BL6 background and possessed targeted deletions of either IL-6 (IL-6 −/− ; Kopf et al 1994), TNF receptor 1 (TNFR1 −/− ; Peschon et al 1998), TNF receptor 2 (TNFR2 −/− ; Erickson et al 1994), both TNF receptors 1 and 2 (TNFR1/2 −/− ; Peschon et al 1998), or IL-1 receptor 1 (IL-1R1 −/− ; Glaccum et al 1997). All mice were obtained from Jackson Laboratories (Bar Harbor, ME, USA).…”

Section: Animalsmentioning

confidence: 99%

Lipopolysaccharide-Induced Osteoclastogenesis from Mononuclear Precursors: A Mechanism for Osteolysis in Chronic Otitis

Nason

Jung

Chole

2009

JARO

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Osteoclasts are the only cells capable of carrying out bone resorption and therefore are responsible for the osteolysis seen in infectious diseases such as chronic otitis media and infected cholesteatoma. Pseudomonas aeruginosa is the most common organism isolated from these infectious middle ear diseases. In this study, we examined the mechanisms by which P. aeruginosa lipopolysaccharide (LPS) stimulates osteoclastogenesis directly from mononuclear osteoclast precursor cells. Osteoclast precursors demonstrated robust, bone-resorbing osteoclast formation when stimulated by P. aeruginosa LPS only if previously primed with permissive, sub-osteoclastogenic doses of receptor activator of NF-κB ligand (RANKL), suggesting that LPS is osteoclastogenic only during a specific developmental window. Numerous LPS-elicited cytokines were found to be released by osteoclast precursors undergoing P. aeruginosa LPS-mediated osteoclast formation. Two lines of evidence suggest that several cytokines promote Oc formation in an autocrine/paracrine manner. First, inhibition of several cytokine pathways including TNF-α, IL-1, and IL-6 block the osteoclastogenesis induced by LPS. Secondly, increased expression of the receptors for TNF-α and IL-1 was demonstrated by real-time quantitative polymerase chain reaction. Such a mechanism has not previously been established and demonstrates the ability of osteoclast precursors to autonomously facilitate bone destruction.

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“…The TNF-␣, lymphotoxin ␣ (LT␣), and LT␤ genes and their receptors have been disrupted. [23][24][25][26][27][28][29][30][31][32][33][34][35][36][37][38] The results obtained demonstrate a previously unrealized role for these cytokines in peripheral lymphoid organ development. TNF-␣ Ϫ/Ϫ mice have expanded marginal zones in the spleen but are deficient in follicles and follicular dendritic cells, whereas LT␣ Ϫ/Ϫ mice show a more severe developmental defect, as they are missing peripheral lymph nodes and Peyer's patches (PP).…”

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confidence: 95%

“…LT␤ Ϫ/Ϫ mice have a somewhat intermediate phenotype, as they lack peripheral lymph nodes, PP, primary and secondary follicles, and follicular dendritic cells, but have mesenteric and cervical lymph nodes. Mice lacking the p75 TNF receptor (TNFR) develop lymph nodes and PP, 25 whereas mice with interrupted p55 TNFR have been reported to have normal or absent PP. 32,38 Defective GC formation is also seen in mice after inactivation of nuclear factor-B2 and bcl-3 genes, which are also involved in TNFR signaling pathways.…”

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confidence: 99%

Lymphoid abnormalities in CD40 ligand transgenic mice suggest the need for tight regulation in gene therapy approaches to hyper immunoglobulin M (IgM) syndrome

et al. 2000

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Mutations in the CD40 ligand (CD40L) are responsible for human hyper immunoglobulin M (IgM) syndrome. The absence of the interaction between CD40L, expressed by T lymphocytes, and the CD40 receptor present on the surface of B cells is responsible for the inability of B cells to carry out the isotype switch from IgM to the other Ig classes. This leads to a fatal immunodeficiency for which no cure exists. For these reasons, the CD40L gene is a good candidate for gene therapy studies. To investigate the possible effects of the expression of this tightly regulated gene in vivo, we produced transgenic mice in which CD40L expression was deregulated. Widespread ectopic expression appears to be lethal. Overexpression in mature T cells is compatible with life, but in one-third of the cases, mice developed atypical lymphoid proliferations which, occasionally, progressed into frank lymphomas. Even though gene therapy is one of the most promising approaches to cure human hyper IgM syndrome, these results suggest that when we modify very tightly regulated genes such as cytokines or other growth factors, particular care has to be taken to avoid excessive stimulation of the target cells.

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Decreased sensitivity to tumour-necrosis factor but normal T-cell development in TNF receptor-2-deficient mice

Cited by 567 publications

References 21 publications

Lack of TNFR2 expression by CD4⁺ T cells exacerbates experimental colitis

Lack of TNFR2 expression by CD4⁺ T cells exacerbates experimental colitis

Lipopolysaccharide-Induced Osteoclastogenesis from Mononuclear Precursors: A Mechanism for Osteolysis in Chronic Otitis

Lymphoid abnormalities in CD40 ligand transgenic mice suggest the need for tight regulation in gene therapy approaches to hyper immunoglobulin M (IgM) syndrome

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Decreased sensitivity to tumour-necrosis factor but normal T-cell development in TNF receptor-2-deficient mice

Cited by 567 publications

References 21 publications

Lack of TNFR2 expression by CD4+ T cells exacerbates experimental colitis

Lack of TNFR2 expression by CD4+ T cells exacerbates experimental colitis

Lipopolysaccharide-Induced Osteoclastogenesis from Mononuclear Precursors: A Mechanism for Osteolysis in Chronic Otitis

Lymphoid abnormalities in CD40 ligand transgenic mice suggest the need for tight regulation in gene therapy approaches to hyper immunoglobulin M (IgM) syndrome

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Lack of TNFR2 expression by CD4⁺ T cells exacerbates experimental colitis

Lack of TNFR2 expression by CD4⁺ T cells exacerbates experimental colitis