Your search keyword '"Iwakura Y"' showing total 27 results

1. Induction of inflammatory arthropathy resembling rheumatoid arthritis in mice transgenic for HTLV-1.

Author

Iwakura, Y. and Tosu, M.

Subjects

*ARTHRITIS

Abstract

Explores the pathological role human T cell leukemia virus type-I (HTLV-I) may play in disease. Production of transgenic mice with HTLV-I genome; Development of arthritic condition in mice resembling rheumatoid arthritis; Marked synovial and periarticular inflammation; Possible role of HTLV-I as a etiologic agent of chronic arthritis in humans.

Published

1991

2. Arthritis in mice that are deficient in interleukin-1 receptor antagonist is dependent on genetic background.

Author

Zhou F, He X, Iwakura Y, Horai R, and Stuart JM

Abstract

OBJECTIVE: To determine the effect of deletion of interleukin-1 receptor antagonist (IL-1Ra) protein in an animal model of rheumatoid arthritis. METHODS: BALB/c mice deficient in IL-1Ra (IL-1Ra(-/-)) were bred with collagen-induced arthritis (CIA)-susceptible DBA/1 mice and B10 mice transgenic for HLA-DRB1*0101 (B10.DR1). After generation of IL-1Ra(-/-) mice on the DBA/1 and B10.DR1 backgrounds, the mice were observed for the development of spontaneous arthritis and immunized for induction of CIA. RESULTS: We found that although BALB/c mice deficient in IL-1Ra (BALB/c(-/-)) spontaneously developed chronic inflammatory arthritis, DBA/1 IL-1Ra-deficient (DBA/1(-/-)) and B10.DR1 IL-1Ra-deficient (B10.DR1(-/-)) mice did not. Splenocytes from BALB/c(-/-) mice produced elevated levels of IL-2, IL-4, IL-6, IL-10, IL-17, and granulocyte-macrophage colony-stimulating factor in response to anti-CD3 stimulation. After immunization with type II collagen (CII), DBA/1(-/-) and B10.DR1(-/-) mice had a significantly earlier onset of CIA, and with increased severity compared with IL-1Ra(+/+) mice. Immunization of BALB/c(-/-) mice with CII did not aggravate spontaneous arthritis. All of the immunized mice developed antibodies to CII that correlated with arthritis severity. Levels of antibody to CII in the BALB/c(-/-) strain were relatively low. CONCLUSION: These data indicate that the spontaneous arthritis of IL-1Ra deficiency is highly dependent on non-major histocompatibility complex genes and that autoimmunity to CII is not the major disease-inducing event. Class II immune response genes are more important for the regulation of CIA, and although these 2 models of arthritis share many pathogenic mechanisms, they also have significant differences. [ABSTRACT FROM AUTHOR]

Published

2005

3. Chemokine synthesis and cellular inflammatory changes in lungs of mice bearing p40tax of human T-lymphotropic virus type 1.

Author

Miyazato, A., Kawakami, K., Iwakura, Y., and Saito, A.

Subjects

*HTLV-I, *LUNGS, *CYTOKINES, *CHEMOKINES, *HISTOPATHOLOGY

Abstract

To elucidate the pathogenic mechanisms of human T-lymphotropic virus type 1 (HTLV-1)-associated lung inflammation, we conducted a histopathological and molecular analysis study using transgenic mice bearing pX region of this virus. In these mice, accumulations of inflammatory cells consisting mainly of lymphocytes were present in peribronchiolar and perivascular areas and alveolar septa, while control littermate mice did not show such changes. In situ hybridization showed that the anatomic distribution of p40tax mRNA was similar to that of inflammatory cells, typically in peribronchiolar areas and to a lesser extent in perivascular and alveolar septa. Inflammatory cytokines, including IL-1β, tumour necrosis factor-alpha and interferon-gamma, and several chemokines, such as monocyte chemotactic protein-1 (MCP-1), RANTES, macrophage inflammatory protein-1α (MIP-1α) and IP-10, were detected in lungs of transgenic mice but not control mice. Semiquantitative analysis using reverse transcription-polymerase chain reaction showed a significant correlation between MCP-1 mRNA expression and p40tax mRNA, but not with other chemokines. The gene expression of the above chemokines, with the exception of MIP-1α, correlated with the severity of histopathological changes in the lung. Considered together, our results suggested that p40tax synthesis may be involved in the development of lung lesions caused by HTLV-1 through the induction of local production of chemokines. [ABSTRACT FROM AUTHOR]

Published

2000

4. β-Glucans in food modify colonic microflora by inducing antimicrobial protein, calprotectin, in a Dectin-1-induced-IL-17F-dependent manner.

Author

Kamiya, T, Tang, C, Kadoki, M, Oshima, K, Hattori, M, Saijo, S, Adachi, Y, Ohno, N, and Iwakura, Y

Published

2018

5. Fungal-derived cues promote ocular autoimmunity through a Dectin-2/Card9-mediated mechanism.

Author

Brown, B. R., Lee, E. J., Snow, P. E., Vance, E. E., Iwakura, Y., Ohno, N., Miura, N., Lin, X., Brown, G. D., Wells, C. A., Smith, J. R., Caspi, R. R., and Rosenzweig, H. L.

Subjects

*UVEITIS, *EYE diseases, *T cells, *RETINOIDS, *ANTIGENS

Abstract

Uveitis (intraocular inflammation) is a leading cause of loss of vision. Although its aetiology is largely speculative, it is thought to arise from complex genetic-environmental interactions that break immune tolerance to generate eye-specific autoreactive T cells. Experimental autoimmune uveitis (EAU), induced by immunization with the ocular antigen, interphotoreceptor retinoid binding protein (IRBP), in combination with mycobacteria-containing complete Freund's adjuvant (CFA), has many clinical and histopathological features of human posterior uveitis. Studies in EAU have focused on defining pathogenic CD4+ T cell effector responses, such as those of T helper type 17 (Th17) cells, but the innate receptor pathways precipitating development of autoreactive, eye-specific T cells remain poorly defined. In this study, we found that fungal-derived antigens possess autoimmune uveitis-promoting function akin to CFA in conventional EAU. The capacity of commensal fungi such as Candida albicans or Saccharomyces cerevisae to promote IRBP-triggered EAU was mediated by Card9. Because Card9 is an essential signalling molecule of a subgroup of C-type lectin receptors (CLRs) important in host defence, we evaluated further the proximal Card9-activating CLRs. Using single receptor-deficient mice we identified Dectin-2, but not Mincle or Dectin-1, as a predominant mediator of fungal-promoted uveitis. Conversely, Dectin-2 activation by α-mannan reproduced the uveitic phenotype of EAU sufficiently, in a process mediated by the Card9-coupled signalling axis and interleukin (IL)-17 production. Taken together, this report relates the potential of the Dectin-2/Card9-coupled pathway in ocular autoimmunity. Not only does it contribute to understanding of how innate immune receptors orchestrate T cell-mediated autoimmunity, it also reveals a previously unappreciated ability of fungal-derived signals to promote autoimmunity. [ABSTRACT FROM AUTHOR]

Published

2017

6. Bone marrow transplantation alters lung antigen-presenting cells to promote TH17 response and the development of pneumonitis and fibrosis following gammaherpesvirus infection.

Author

Zhou, X, Loomis-King, H, Gurczynski, S J, Wilke, C A, Konopka, K E, Ptaschinski, C, Coomes, S M, Iwakura, Y, van Dyk, L F, Lukacs, N W, and Moore, B B

Published

2016

7. IFN-γ induction by neutrophil-derived IL-17A homodimer augments pulmonary antibacterial defense.

Author

Cai, S, Batra, S, Langohr, I, Iwakura, Y, and Jeyaseelan, S

Published

2016

8. Cost-Effectiveness Analysis of the Diagnosis and Treatment of Primary Aldosteronism in Japan.

Author

Sato, M., Morimoto, R., Seiji, K., Iwakura, Y., Ono, Y., Kudo, M., Satoh, F., Ito, S., Ishibashi, T., and Takase, K.

Subjects

*HYPERALDOSTERONISM, *MEDICAL technology, *HEALTH outcome assessment, *ADRENALECTOMY, *COST effectiveness, *THERAPEUTICS

Abstract

Approximately 10 % of cases of hypertension in Japan are caused by primary aldosteronism (PA), amounting to about 4 million patients in total. Primary aldosteronism due to unilateral aldosterone hypersecretion is potentially curable by adrenalectomy. The clinical benefits of identifying and treating PA have been reported internationally, but its cost-effectiveness is unclear. We examined whether diagnosing and treating hidden PA in hypertensive population was costeffective compared with suboptimal treatment. Our hypothetical patient was a 50-year-old man diagnosed with stage I--III hypertension. We established a Markov decision model based on plausible clinical pathways and prognoses of PA. We applied cost-effectiveness analysis comparing a comprehensive diagnostic strategy for PA (measurement of plasma aldosterone/renin ratio, 2 loading tests, imaging, and selective adrenal venous sampling) with a suboptimal strategy to manage hypertension by medication unless the typical signs of PA or other complication were manifest. Outcome measures were expected costs, expected effectiveness, and incremental cost-effectiveness ratio. The robustness of the findings was established by one-way and scenario sensitivity analyses. The comprehensive PA diagnostic strategy increased the expected costs by 64 004 JPY and expected life-years by 0.013 compared with standard treatment. The incremental cost-effectiveness ratio for the diagnosis of PA was 4 923 385 JPY per year. Our findings were sensitive to the outcomes of screening and treatment, and the costs of continuous or periodic medication for hypertension and the treatment of stroke and its complications. [ABSTRACT FROM AUTHOR]

Published

2015

9. Neutrophils negatively regulate induction of mucosal IgA responses after sublingual immunization.

Author

Jee, J, Bonnegarde-Bernard, A, Duverger, A, Iwakura, Y, Cormet-Boyaka, E, Martin, T L, Steiner, H E, Bachman, R C, and Boyaka, P N

Subjects

*NEUTROPHILS, *IMMUNIZATION, *PREVENTIVE medicine, *IMMUNOGLOBULIN A, *MYELOID leukemia

Abstract

Induction of mucosal immunoglobulin-A (IgA) capable of providing a first line of defense against bacterial and viral pathogens remains a major goal of needle-free vaccines given via mucosal routes. Innate immune cells are known to play a central role in induction of IgA responses by mucosal vaccines, but the relative contribution of myeloid cell subsets to these responses has not firmly been established. Using an in vivo model of sublingual vaccination with Bacillus anthracis edema toxin (EdTx) as adjuvant, we examined the role of myeloid cell subsets for mucosal secretory IgA responses. Sublingual immunization of wild-type mice resulted in a transient increase of neutrophils in sublingual tissues and cervical lymph nodes. These mice later developed Ag-specific serum IgG responses, but not serum or mucosal IgA. Interestingly, EdTx failed to increase neutrophils in sublingual tissues and cervical lymph nodes of IKKβΔMye mice, and these mice developed IgA responses. Partial depletion of neutrophils before immunization of wild-type mice allowed the development of both mucosal and serum IgA responses. Finally, co-culture of B cells with neutrophils from either wild-type or IKKβΔMye mice suppressed secretion of IgA, but not IgM or IgG. These results identify a new role for neutrophils as negative regulators of IgA responses. [ABSTRACT FROM AUTHOR]

Published

2015

10. Vaspin is an adipokine ameliorating ER stress in obesity as a ligand for cell-surface GRP78/MTJ-1 complex.

Author

Nakatsuka A, Wada J, Iseda I, Teshigawara S, Higashio K, Murakami K, Kanzaki M, Inoue K, Terami T, Katayama A, Hida K, Eguchi J, Horiguchi CS, Ogawa D, Matsuki Y, Hiramatsu R, Yagita H, Kakuta S, Iwakura Y, and Makino H

Abstract

It is unknown whether adipokines derived from adipose tissues modulate endoplasmic reticulum (ER) stress induced in obesity. Here, we show that visceral adipose tissue-derived serine protease inhibitor (vaspin) binds to cell-surface 78-kDa glucose-regulated protein (GRP78), which is recruited from ER to plasma membrane under ER stress. Vaspin transgenic mice were protected from diet-induced obesity, glucose intolerance, and hepatic steatosis, while vaspin-deficient mice developed glucose intolerance associated with upregulation of ER stress markers. With tandem affinity tag purification using HepG2 cells, we identified GRP78 as an interacting molecule. The complex formation of vaspin, GRP78, and murine tumor cell DnaJ-like protein 1 (MTJ-1) (DnaJ homolog, subfamily C, member 1) on plasma membrane was confirmed by cell-surface labeling with biotin and immunoprecipitation in liver tissues and H-4-II-E-C3 cells. The addition of recombinant human vaspin in the cultured H-4-II-E-C3 cells also increased the phosphorylation of Akt and AMP-activated protein kinase (AMPK) in a dose-dependent manner, and anti-GRP78 antibodies completely abrogated the vaspin-induced upregulation of pAkt and pAMPK. Vaspin is a novel ligand for cell-surface GRP78/MTJ-1 complex, and its subsequent signals exert beneficial effects on ER stress-induced metabolic dysfunctions. [ABSTRACT FROM AUTHOR]

Published

2012

11. Upregulation of Polymeric Immunoglobulin Receptor Expression by the Heat-Inactivated Potential Probiotic Bifidobacterium bifidum OLB6378 in a Mouse Intestinal Explant Model.

Author

Nakamura, Y., Terahara, M., Iwamoto, T., Yamada, K., Asano, M., Kakuta, S., Iwakura, Y., and Totsuka, M.

Subjects

*IMMUNOGLOBULIN receptors, *PROBIOTICS, *BIFIDOBACTERIUM bifidum, *GENE expression, *IMMUNE system, *DNA microarrays, *INTERLEUKINS, *LABORATORY mice

Abstract

We determined whether a potential probiotic bacterium, Bifidobacterium bifidum OLB6378 (BB6378), exerts beneficial effects on the mucosal immune system in a mouse intestinal explant model. The addition of heat-inactivated BB6378 to intestinal explants prepared from embryonic day 18 BALB/c mice increased the expression of polymeric immunoglobulin receptor (pIgR) mRNA by two- to fivefold. These effects were observed on ileal and colonic explants but not on jejunal explants, suggesting that the BB6378-induced pIgR upregulation is site-specific within the mouse intestine. The upregulation of pIgR protein expression in colonic explants was also detected after 24 h of culture. The results of DNA microarray analysis of ileal and colonic samples indicated that BB6378 increased the gene expression of interleukin (IL)-1α and IL-1β, and IL-1α content in colonic explants was significantly increased after 20 h of culture with BB6378. We then examined the involvement of endogenously induced IL-1α in pIgR mRNA upregulation by using IL-1α knockout (KO) mice. Contrary to our expectations, pIgR mRNA expression was equally upregulated by BB6378 in colonic explants from BALB/c and IL-1α KO mice. Conversely, we examined the involvement of Toll-like receptors in pIgR mRNA upregulation by using MyD88 KO mice. The upregulation of pIgR was completely suppressed in the explants derived from MyD88 KO mice. Taken together, we conclude that in a mouse intestinal explant model, the heat-inactivated potential probiotic BB6378 increases intestinal pIgR expression in a site-specific manner and that the upregulation of pIgR could be explained by a direct microbial effect on the epithelium via Toll-like receptors. [ABSTRACT FROM AUTHOR]

Published

2012

12. Age-dependent regulation of depression-like behaviors through modulation of adrenergic receptor α1A subtype expression revealed by the analysis of interleukin-1 receptor antagonist knockout mice

Author

Wakabayashi, C., Kiyama, Y., Kunugi, H., Manabe, T., and Iwakura, Y.

Subjects

*MENTAL depression, *ADRENERGIC receptors, *GENE expression, *INTERLEUKIN-1, *LABORATORY mice, *MESSENGER RNA, *CEREBRAL cortex, *ETHYLENEDIAMINETETRAACETIC acid

Abstract

Abstract: Interleukin-1 (IL-1) plays a crucial role in stress responses and its mRNA is induced in the brain by stress load; however, the precise role of IL-1 in higher brain functions and their abnormalities is largely unknown. Here, we report that IL-1 receptor antagonist (IL-1Ra) knockout (KO) mice, which lack IL-1Ra molecules that antagonize the IL-1 receptor, displayed anti-depression-like phenotypes in the tail suspension test (TST) and forced-swim test (FST) only at a young stage (8 weeks), whereas the phenotypes disappeared at later stages (20 and 32 weeks). These anti-depression-like phenotypes were reversed by administration of adrenergic receptor (AR) antagonists against the ARα1, ARα2, and ARβ subtypes. Although the contents of 5-HT, norepinephrine (NE), and dopamine (DA), which are known to be associated with major symptoms of psychiatric disorders, were not significantly different in the hippocampus or cerebral cortex between IL-1Ra KO and their wild-type (WT) littermate mice, the mRNA expression level of the ARα1A subtype was significantly changed in the cerebral cortex. Interestingly, the change in expression of the ARα1A subtype was correlated with an age-dependent alteration in the TST and FST in IL-1Ra KO mice. Furthermore, mild immobilization stress loaded on C57BL/6J male mice caused similar anti-depression-like phenotypes in the TST and FST to those observed in mutant mice. These results suggest that sustained activation of IL-1 signaling induced by gene manipulation in mutant mice affects the expression of the ARα1A subtype and that modification of adrenergic signaling by the IL-1 system may ultimately cause significant psychiatric abnormalities such as depression, and this mutant mouse could be regarded as a model animal of depression that specifically appears in children and adolescents. [Copyright &y& Elsevier]

Published

2011

13. NLRP3 inflammasome is required in murine asthma in the absence of aluminum adjuvant.

Author

Besnard, A.-G., Guillou, N., Tschopp, J., Erard, F., Couillin, I., Iwakura, Y., Quesniaux, V., Ryffel, B., and Togbe, D.

Subjects

*PNEUMONIA, *RESPIRATORY allergy, *IMMUNOLOGICAL adjuvants, *IMMUNOREGULATION, *CHEMOKINES

Abstract

Background: Inflammasome activation with the production of IL-1β received substantial attention recently in inflammatory diseases. However, the role of inflammasome in the pathogenesis of asthma is not clear. Using an adjuvant-free model of allergic lung inflammation induced by ovalbumin (OVA), we investigated the role of NLRP3 inflammasome and related it to IL-1R1 signaling pathway. Methods: Allergic lung inflammation induced by OVA was evaluated in vivo in mice deficient in NLRP3 inflammasome, IL-1R1, IL-1β or IL-1α. Eosinophil recruitment, Th2 cytokine, and chemokine levels were determined in bronchoalveolar lavage fluid, lung homogenates, and mediastinal lymph node cells ex vivo. Results: Allergic airway inflammation depends on NLRP3 inflammasome activation. Dendritic cell recruitment into lymph nodes, Th2 lymphocyte activation in the lung and secretion of Th2 cytokines and chemokines are reduced in the absence of NLRP3. Absence of NLRP3 and IL-1β is associated with reduced expression of other proinflammatory cytokines such as IL-5, IL-13, IL-33, and thymic stromal lymphopoietin. Furthermore, the critical role of IL-1R1 signaling in allergic inflammation is confirmed in IL-1R1-, IL-1β-, and IL-1α-deficient mice. Conclusion: NLRP3 inflammasome activation leading to IL-1 production is critical for the induction of a Th2 inflammatory allergic response. [ABSTRACT FROM AUTHOR]

Published

2011

14. Biotin status affects nickel allergy via regulation of interleukin-1beta production in mice.

Author

Kuroishi T, Kinbara M, Sato N, Tanaka Y, Nagai Y, Iwakura Y, Endo Y, and Sugawara S

Published

2009

15. Lipopolysaccharide promotes and augments metal allergies in mice, dependent on innate immunity and histidine decarboxylase.

Author

Sato, N., Kinbara, M., Kuroishi, T., Kimura, K., Iwakura, Y., Ohtsu, H., Sugawara, S., and Endo, Y.

Subjects

*ALLERGIES, *HISTAMINE, *IMMUNOLOGIC diseases, *INFLAMMATORY mediators, *RODENTS, *CELLS

Abstract

Background Few adequate murine models exist for metal allergies, it being especially difficult to induce Ni allergy in mice. Objective We examined the effect of lipopolysaccharide (LPS) on allergies to Ni and other metals in mice. Methods Ten days after sensitization with a metal salt and LPS, the ears were challenged with the same metal salt. Results LPS+NiCl2 (1 mm) was effective at sensitizing mice to Ni, LPS being effective at very low concentrations whether injected intradermally or intraperitoneally. The ear-swelling response to Ni was more severe and more rapid in C57BL/6 mice than in BALB/c mice. In mast-cell-deficient mice, TNF-α-deficient mice, and interestingly even in nude (T cell deficient) mice, NiCl2+LPS induced a Ni allergy similar in degree to that in the respective control mice, but it induced Ni allergy only weakly in TLR4-mutant mice, macrophage-depleted mice, and IL-1-deficient mice. The activity of the histamine-forming enzyme histidine decarboxylase (HDC) in the ears increased in parallel with ear swelling, and HDC-deficient mice were resistant to ear swelling. Challenge with NiCl2+LPS augmented ear swelling (vs. NiCl2 alone). LPS induced effective sensitization to other metals (Cr, Co, Pd, or Ag). Conclusions These results indicate that in mice, LPS is a very important inducer of metal allergies, and potently promotes them (dependent on both innate immunity and HDC induction in cells other than mast cells). We discussed the idea that the bacterial environment is important for the establishment of metal allergies and for their provocation, and that the current thinking (including the contribution of T cells) should be reappraised in future studies. [ABSTRACT FROM AUTHOR]

Published

2007

16. Interferon-gamma is causatively involved in experimental inflammatory bowel disease in mice.

Author

Ito, R., Shin-Ya, M., Kishida, T., Urano, A., Takada, R., Sakagami, J., Imanishi, J., Kita, M., Ueda, Y., Iwakura, Y., Kataoka, K., Okanoue, T., and Mazda, O.

Subjects

*CYTOKINES, *INFLAMMATORY bowel diseases, *INTERFERONS, *DEXTRAN, *CHEMOKINES, *BODY weight, *MORTALITY, *THERAPEUTICS

Abstract

Cytokines may be crucially involved in the pathogenesis of inflammatory bowel diseases (IBD), but it remains controversial whether interferon (IFN)-γ, a typical proinflammatory cytokine, is an essential mediator to cause the disorders. In the present study, IFN-γ–/– and wild-type (WT) C57BL/6 mice were fed 2·5% dextran sodium sulphate (DSS) in drinking water for 7 days, in order to investigate DSS-induced intestinal inflammation. The DSS-treated WT mice exhibited a robust production of IFN-γ in the gut, a remarkable loss of body weight, as well as high rate of mortality (60%). In striking contrast, IFN-γ deficient mice did not develop DSS-induced colitis, as indicated by the maintenance of body weight and survival rate of 100%. Severe intestinal inflammation was demonstrated exclusively in WT animals in terms of the shortening of the bowel as well as the elevation of the disease activity index, myeloperoxidase (MPO) activity and serum haptoglobin level. Histological study of DSS-treated WT intestine revealed disruption of mucosal epithelium and massive infiltration of inflammatory cells, while the organ from IFN-γ–/– mice remained virtually normal in appearance. Enzyme-linked immunosorbent assay (ELISA) analyses indicated abundant production of three chemokines, i.e. monokine induced by interferon-γ (MIG), interferon-inducible protein 10 (IP-10) and monocyte chemoattractant protein-1 (MCP-1), in the DSS-irritated intestine of WT but not of IFN-γ–/– mice. The present results demonstrate clearly that IFN-γ plays indispensable roles in the initiation of DSS colitis, and some chemokines are produced in an IFN-γ-dependent fashion. [ABSTRACT FROM AUTHOR]

Published

2006

17. Low concentration of interleukin-1beta induces FLICE-inhibitory protein-mediated beta-cell proliferation in human pancreatic islets.

Author

Maedler K, Schumann DM, Sauter N, Ellingsgaard H, Bosco D, Baertschiger R, Iwakura Y, Oberholzer J, Wollheim CB, Gauthier BR, Donath MY, Maedler, Kathrin, Schumann, Desiree M, Sauter, Nadine, Ellingsgaard, Helga, Bosco, Domenico, Baertschiger, Reto, Iwakura, Yoichiro, Oberholzer, José, and Wollheim, Claes B

Subjects

*ANIMAL experimentation, *CELL physiology, *CELLULAR signal transduction, *GLYCOPROTEINS, *INTERLEUKIN-1, *ISLANDS of Langerhans, *RESEARCH methodology, *MICE, *PROTEINS, *TISSUE culture, *GLUCOSE intolerance

Abstract

High glucose concentrations have a dual effect on beta-cell turnover, inducing proliferation in the short-term and apoptosis in the long-term. Hyperglycemia leads to beta-cell production of interleuking (IL)-1beta in human pancreatic islets. Fas, a death receptor regulated by IL-1beta, is involved in glucose-induced beta-cell apoptosis. Fas engagement can be switched from death signal to induction of proliferation when the caspase 8 inhibitor, FLICE-inhibitory protein (FLIP), is active. Here, we show that IL-1beta at low concentrations may participate in the mitogenic actions of glucose through the Fas-FLIP pathway. Thus, exposure of human islets to low IL-1beta concentrations (0.01-0.02 ng/ml) stimulated proliferation and decreased apoptosis, whereas increasing amounts of IL-1beta (2-5 ng/ml) had the reverse effects. A similarly bimodal induction of FLIP, pancreatic duodenal homeobox (PDX)-1, and Pax4 mRNA expression, as well as glucose-stimulated insulin secretion, was observed. In contrast, Fas induction by IL-1beta was monophasic. Low IL-1beta also induced the IL-1 receptor antagonist (IL-1Ra), suppression of which by RNA interference abrogated the beneficial effects of low IL-1beta. The Fas antagonistic antibody ZB4 and small interfering RNA to FLIP prevented low IL-1beta-stimulated beta-cell proliferation. Consistent with our in vitro results, IL-1beta knockout mice displayed glucose intolerance along with a decrease in islet Fas, FLIP, Pax4, and PDX-1 transcripts. These findings indicate that low IL-1beta levels positively influence beta-cell function and turnover through the Fas-FLIP pathway and that IL-1Ra production prevents harmful effects of high IL-1beta concentrations. [ABSTRACT FROM AUTHOR]

Published

2006

18. Interleukin-1-dependent sequential chemokine expression and inflammatory cell infiltration in ischemia-reperfusion injury.

Author

Furuichi K, Wada T, Iwata Y, Kokubo S, Hara A, Yamahana J, Sugaya T, Iwakura Y, Matsushima K, Asano M, Yokoyama H, and Kaneko S

Abstract

OBJECTIVE: Ischemia-reperfusion injury is known to cause organ failure, but the mechanisms of pathogenesis remain unclear. Inflammation is a factor in tissue destruction in ischemia reperfusion injury, and interleukin (IL)-1 is a key promoter of inflammation. DESIGN: Prospective, randomized, and controlled study. SETTING: University laboratory. SUBJECTS: Male mice 6-8 wks of age, in which genes for IL-1alpha and IL-1beta (IL-1alpha/beta deficient) and IL-1 receptor antagonist (IL-1RA deficient) are deleted by homologous recombination, and wild-type controls on a Balb/c background. INTERVENTIONS: In this study, the role of IL-1 on inflammatory cascades, including chemokine expression, inflammatory cell infiltration, and tissue destruction, was investigated in 45 mins of unilateral renal ischemic injury using IL-1alpha/beta-deficient mice and IL-1RA-deficient mice. In addition, the effects of IL-1 on chemokine expression in cultured tubular epithelial cells were investigated. MEASUREMENTS AND MAIN RESULTS: In vivo study revealed that the number of interstitial infiltrated neutrophils and macrophages, which accompanied the increase of the serum levels of keratinocyte-derived chemokine (KC) and macrophage inflammatory protein (MIP)-1alpha, respectively, significantly increased in IL-1RA-deficient mice. The number of interstitial infiltrated neutrophils correlated well with serum levels of KC at 24 hrs after reperfusion, whereas the number of interstitial infiltrated macrophages correlated well with the serum levels of MIP-1alpha and monocyte chemoattractant protein (MCP)-1 at 24 and 48 hrs after reperfusion, respectively. Likewise, in vitro study revealed that stimulation of tubular epithelial cells by IL-1beta and/or H2O2 sequentially induced KC, MIP-1alpha, and MCP-1 in both protein and messenger RNA levels, which is consistent with in vivo results. CONCLUSION: IL-1-dependent inflammatory cascades, followed by inflammatory cell infiltration and subsequent tissue destruction, may affect pathogenesis of renal ischemia-reperfusion injury. [ABSTRACT FROM AUTHOR]

Published

2006

19. Endogenous interleukin (IL)-1 alpha and IL-1 beta are crucial for host defense against disseminated candidiasis.

Author

Vonk AG, Netea MG, van Krieken JH, Iwakura Y, van der Meer JWM, and Kullberg BJ

Abstract

Background. Interleukin (IL)-1 alpha and IL-1 beta are protective proinflammatory cytokines involved in host defense against Candida albicans. It is, however, unknown whether they provide protection through similar mechanisms. We investigated the effect of endogenous IL-1 alpha and IL-1 beta on disseminated C. albicans infection. Methods. Mice deficient in the genes encoding IL-1 alpha (IL-1 alpha (-/-)), IL-1 beta (IL-1 beta (-/-)), or both molecules (IL-1 alpha (-/-) beta (-/-)) were used. Survival and C. albicans outgrowth in the kidneys was assessed after intravenous injection of C. albicans.Results. Both mortality and C. albicans outgrowth in the kidneys were significantly increased in IL-1 alpha (-/-) and IL-1 beta (-/-) mice, compared with those in control mice, with the IL-1 alpha (-/-) beta (-/-) mice being most susceptible to disseminated candidiasis. The host defense mechanisms triggered by IL-1 alpha and IL-1 beta differed from one another. IL-1 beta (-/-) mice showed decreased recruitment of granulocytes in response to an intraperitoneal C. albicans challenge, and generation of superoxide production was diminished in IL-1 beta (-/-) granulocytes. IL-1 alpha (-/-) mice had a reduced capacity to damage C. albicans pseudohyphae. Protective type 1 responses were deficient in both IL-1 alpha (-/-) and IL-1 beta (-/-) mice, as assessed by production of interferon- gamma by splenocytes in response to heat-killed C. albicans.Conclusion. Although IL-1 alpha and IL-1 beta have differential effects on the various arms of host defense, both cytokines are essential for mounting a protective host response against invasive C. albicans infection. Copyright © 2006 Infectious Diseases Society of America [ABSTRACT FROM AUTHOR]

Published

2006

20. CD28-dependent differentiation into the effector/memory phenotype is essential for induction of arthritis in interleukin-1 receptor antagonist-deficient mice.

Author

Kotani M, Hirata K, Ogawa S, Habiro K, Ishida Y, Tanuma S, Horai R, Iwakura Y, Kishimoto H, and Abe R

Abstract

OBJECTIVE: Interleukin-1 receptor antagonist (IL-1Ra)-deficient mice on a BALB/c background spontaneously develop a chronic inflammatory polyarthropathy closely resembling that of rheumatoid arthritis in humans. To elucidate the role of CD28 costimulatory signals in the development of this disease, we studied IL-1Ra/CD28-double-deficient mice. METHODS: We crossed IL-1Ra-deficient mice with CD28-deficient mice and observed the incidence and severity of arthritis. To investigate functions of IL-1Ra/CD28-double-deficient T cells, cells were stimulated with CD3 monoclonal antibody or allogeneic antigen-presenting cells (APCs) and their proliferative responses and levels of cytokine production were measured. RESULTS: Disease severity was lower in IL-1Ra/CD28-double-deficient mice than in mice that were deficient only in IL-1Ra, although incidence of arthritis was not affected by the presence or absence of CD28. When pathogenic IL-1Ra-KO T cells were transferred into nude mice, severe arthritis developed. Even though T cells from double-deficient mice showed the same diminished proliferative capacity as was seen in T cells from CD28-single-deficient animals, nude mice into which double-deficient T cells were transferred never developed arthritis. CONCLUSION: These findings indicate that IL-1Ra/CD28-double-deficient T cells can be activated by IL-1Ra-deficient activated APCs, resulting in induction of arthritis; however, these T cells did not induce the disease under normal conditions, because they did not differentiate into effector/memory phenotype. [ABSTRACT FROM AUTHOR]

Published

2006

21. IL-18 gene therapy develops Th1-type immune responses in Leishmania major-infected BALB/c mice: is the effect mediated by the CpG signaling TLR9?

Author

Li, Y., Ishii, K., Hisaeda, H., Hamano, S., Zhang, M., Nakanishi, K., Yoshimoto, T., Hemmi, H., Takeda, K., Akira, S., Iwakura, Y., and Himeno, K.

Subjects

*CYTOKINES, *LEISHMANIA, *GENE expression, *MICE, *LABORATORY animals, *PLASMIDS, *GENETIC vectors, *GENE therapy

Abstract

IL-18 regulates either Th1 or Th2 responses depending on the cytokine microenvironment. Administration of recombinant IL-18 (rIL-18) alone does not promote Th1 response, but rather induces Th2 response and exacerbates Leishmania major infection in susceptible BALB/c mice. Here, we treated BALB/c mice with an IL-18-expressing plasmid by using a gene gun weekly after L. major infection. This gene therapy resulted in improved pathogenic process and preferential induction of Th1 responses by inducing the expression of IL-12 p40, but treatment with rIL-18 did not. Notably, simultaneous administration of rIL-18 with an empty plasmid vector rendered BALB/c mice resistant to the infection, despite the fact that treatment with either rIL-18 alone or the plasmid vector alone did not influence the susceptibility. The synergistic role of the vector with rIL-18 was found to depend on CpG motifs, which enhanced expression of proinflammatory cytokines, especially IL-12, from APCs through Toll-like receptor (TLR) 9 ligation. Treatment with methylated plasmid vector in which CpG was disrupted could no longer prevent the disease development in coadministration with rIL-18. Taken together, IL-18 gene therapy was shown to develop Th1-type protective immunity in L. major-infected BALB/c mice without the requirement of exogenous IL-12, probably via CpG-TLR9 signaling pathway.Gene Therapy (2004) 11, 941-948. doi:10.1038/sj.gt.3302240 Published online 26 February 2004 [ABSTRACT FROM AUTHOR]

Published

2004

22. Ex vivo whole-embryo culture of caspase-8-deficient embryos normalize their aberrant phenotypes in the developing neural tube and heart.

Author

Sakamaki, K, Inoue, T, Asano, M, Sudo, K, Kazama, H, Sakagami, J, Sakata, S, Ozaki, M, Nakamura, S, Toyokuni, S, Osumi, N, Iwakura, Y, and Yonehara, S

Subjects

*CYSTEINE proteinases, *EXPERIMENTAL embryology, *NEURAL tube defects, *HEART abnormalities

Abstract

Caspase-8 plays the role of initiator in the caspase cascade and is a key molecule in death receptor-induced apoptotic pathways. To investigate the physiological roles of caspase-8 in vivo, we have generated caspase-8-deficient mice by gene targeting. The first signs of abnormality in homozygous mutant embryos were observed in extraembryonic tissue, the yolk sac. By embryonic day (E) 10.5, the yolk sac vasculature had begun to form inappropriately, and subsequently the mutant embryos displayed a variety of defects in the developing heart and neural tube. As a result, all mutant embryos died at E11.5. Importantly, homozygous mutant neural and heart defects were rescued by ex vivo whole-embryo culture during E10.5–E11.5, suggesting that these defects are most likely secondary to a lack of physiological caspase-8 activity. Taken together, these results suggest that caspase-8 is indispensable for embryonic development.Cell Death and Differentiation (2002) 9, 1196–1206. doi:10.1038/sj.cdd.4401090 [ABSTRACT FROM AUTHOR]

Published

2002

23. Caspase-2 deficiency prevents programmed germ cell death resulting from cytokine insufficiency but not meiotic defects caused by loss of ataxia telangiectasia-mutated (Atm) gene function.

Author

Morita, Y, Maravei, D V, Bergeron, L, Wang, S, Perez, G I, Tsutsumi, O, Taketani, Y, Asano, M, Horai, R, Korsmeyer, S J, Iwakura, Y, Yuan, J, and Tilly, J L

Subjects

*APOPTOSIS, *CYTOKINES, *ATAXIA telangiectasia, *GERM cells

Abstract

It is well established that programmed cell death claims up to two-thirds of the oocytes produced during gametogenesis in the developing fetal ovaries. However, the mechanisms underlying prenatal germ cell loss in females remain poorly understood. Herein we report that caspase-11 null female mice are born with a reduced number of oocyte-containing primordial follicles. This phenotype is likely due to failed cytokine processing known to occur in caspase-11 mutants since neonatal female mice lacking both interleukin (IL)-1α and IL-1β also exhibit a reduced endowment of primordial follicles. In addition, germ cell death in wild-type fetal ovaries cultured ex vivo is suppressed by either cytokine, likely via ligand activation of type 1 IL-1 receptors expressed in fetal germ cells. Normal oocyte endowment can be restored in caspase-11 null female mice by simultaneous inactivation of the gene encoding the cell death executioner enzyme, caspase-2. However, caspase-2 deficiency cannot overcome gametogenic failure resulting from meiotic recombination defects in ataxia telangiectasia-mutated (Atm) null female mice. Thus, genetically distinct mechanisms exist for developmental deletion of oocytes via programmed cell death, one of which probably functions as a meiotic quality-control checkpoint that cannot be overridden. [ABSTRACT FROM AUTHOR]

Published

2001

24. O036 IL-17-producing gamma-delta T cells are crucial for the development of autoimmune arthritis in IL-1 receptor antagonist-deficient mice

Author

Akitsu, A., Ishigame, H., Kakuta, S., Saijo, S., and Iwakura, Y.

Subjects

*INTERLEUKIN-17, *T cells, *RHEUMATOID arthritis treatment, *INTERLEUKIN-1 receptors, *AUTOIMMUNE diseases, *MONOCLONAL antibodies, *LABORATORY mice

Abstract

Introduction: A high proportion of IL-17-producing gamma-delta T (gd17) cells was detected in joints of Il1rn −/− mice, a model of rheumatoid arthritis, whose development depends on IL-17 and T cells. However, their pathogenic roles are not well understood. Methods: We assessed the effect of gdT cell or CD4+T cell depletion in Il1rn −/− mice using a monoclonal antibodies. Then, we examined the pathogenic activity of gd17 cells by adoptive transfer. Results: To clarify the roles of gdT cells and CD4+ T cells in the development of arthritis, gdT cells or CD4+ T cells were depleted in Il1rn −/− miceusing antibodies. The development of disease was suppressed in both cases, suggesting both gdT cells and CD4+ T cells were involved in the pathogenesis. Then, the pathogenic role of gd17 cells in the absence of Th17 cells was examined. We generated mice with gd17 cells, but without Th17 cells, by adoptively transferring Il17 −/− Il1rn −/−-CD4+ T cells into nu/nu mice in which gd17 cells are present. We found that these mice still developed arthritis and that only gdT cells produced IL-17. To corroborate that the development of arthritis in this transfer system is dependent on IL-17, we adoptively transferred Il17 −/− Il1rn −/−-CD4+ T cells into Il17 −/−-nu/nu mice. The development of arthritis was significantly suppressed in Il17 −/−-nu/nu mice transferred with Il17 −/− Il1rn −/−-CD4+ T cells compared with Il17 +/+-nu/nu mice transferred with Il17 −/− Il1rn −/−-CD4+ T cells, suggesting that extrathymic gd17 cells are also important for the development of arthritis. Interestingly, Il1rn −/− mice on the nu/nu mice background, in which only gd17 cells but not thymus-derived T cells are present, also developed arthritis. Thus, gd17 cells alone can induce arthritis without involvement of CD4+ T cells only in Il1rn −/− background mice in which excess IL-1 signaling is introduced. In contrast, a combination of CD4+ T cells and gd17 cells was required for the development of arthritis when scid/scid mice were used as recipients. These observations suggest that gd17 cells are required for the amplification of inflammation and CD4+ T cells direct the tissue specificity. Conclusion: These results indicate that gdT cell-derived IL-17 plays an important role in the pathogenesis of arthritis in Il1rn −/−mice. [Copyright &y& Elsevier]

Published

2012

25. O040 A novel role of Dectin-1 signaling in promoting intestinal inflammation

Author

Tang, C., Kamiya, T., Kadoki, M., and Iwakura, Y.

Subjects

*INTESTINAL diseases, *INFLAMMATION, *CELLULAR signal transduction, *DENDRITIC cells, *IMMUNE system, *INFLAMMATORY bowel diseases, *CYTOKINES

Abstract

Introduction: Dectin-1, which was first reported as a dentritic cell-specific type II C-type lectin family member, is the receptor for β-1,3 or −1,6-linked glucans (β-glucans), an important cell wall components of fungi and yeasts. Dysregulated response of mucosal immune system toward intraluminal bacteria results in the human inflammatory bowel disease (IBD). Beta-glucan is thought to promote the mucosal immunity in intestines, but the roles of Dectin-1 in mucosal immune system are still unknown. Methods: To investigate the potential role of Dectin-1 in development of IBD, we administrated Decint-1 deficient (clec7a −/−) mice with dextran sulfate sodium (DSS) to induce the acute ulcerative colitis and found that clec7a −/− mice were significantly resistant to DSS-induced colitis compared to wild-type (WT) mice, associated with lower production of TNF-α and reduced numbers of neutrophils and macrophages in lamina propria of colon. Results: Pre-treatment of dectin-1 antagonist ligand Laminarin could suppress the acute intestinal inflammation induced by DSS. Metagenome analysis using bacterial 16s rRNA genes revealed significantly change of the microflora in small intestine and colon of clec7a −/− mice compared to WT mice, and administration of intestinal bacteria of clec7a −/− mice in SPF condition to germ-free WT mice also showed resistant to DSS-induced colitis. Conclusion: These new findings identify Dectin-1 as novel factor in promotion of acute colitis by directly inducing proinflammatory cytokines and by regulating the balance of intestinal microbiota. Blockade of Dectin-1 signaling suggests new therapeutic strategies for inflammatory bowel diseases. [ABSTRACT FROM AUTHOR]

Published

2012

26. P1773 The role of interleukin-1 during Pseudomonas aeruginosa bacteraemia in compromised host

Author

Horino, T., Matsumoto, T., Uramatsu, M., Tanabe, M., Tateda, K., Miyazaki, S., Aramaki, Y., Iwakura, Y., and Yamaguchi, K.

Published

2007

27. Tu-W24:7 Interleukin-1 alpha deficiency inhibits atherogenesis in hypercholesterolemic mice: The role of macrophage IL-1 alpha

Author

Kamari, Y., Werman-Venkert, R., Shaish, A., Harari, A., Gonen, A., Grossman, E., Iwakura, Y., Dinarrelo, C.A., Apte, R.N., and Harats, D.

Published

2006