Your search keyword '"Kashiwakura, Jun-ichi"' showing total 36 results

1. STAP‐2 negatively regulates BCR‐mediated B cell activation by recruiting tyrosine‐protein kinase CSK to LYN.

Author

Kashiwakura, Jun‐ichi, Kawahara, Shoya, Inagaki, Iori, Inui, Kyosuke, Saitoh, Kodai, Kagohashi, Kota, Sasaki, Yuto, Kobayashi, Fuki, Kitai, Yuichi, Muromoto, Ryuta, Oritani, Kenji, and Matsuda, Tadashi

Subjects

*B cells, *B cell receptors, *ANTIBODY formation, *IMMUNE response

Abstract

Although signal‐transducing adaptor protein‐2 (STAP‐2) acts in certain immune responses, its role in B cell receptor (BCR)‐mediated signals remains unknown. In this study, we have revealed that BCR‐mediated signals, cytokine production and antibody production were increased in STAP‐2 knockout (KO) mice compared with wild‐type (WT) mice. Phosphorylation of tyrosine‐protein kinase LYN Y508 was reduced in STAP‐2 KO B cells after BCR stimulation. Mechanistic analysis revealed that STAP‐2 directly binds to LYN, dependently of STAP‐2 Y250 phosphorylation by LYN. Furthermore, phosphorylation of STAP‐2 enhanced interactions between LYN and tyrosine‐protein kinase CSK, resulting in enhanced CSK‐mediated LYN Y508 phosphorylation. These results suggest that STAP‐2 is crucial for controlling BCR‐mediated signals and antibody production by enhanced CSK‐mediated feedback regulation of LYN. [ABSTRACT FROM AUTHOR]

Published

2023

2. Signal-transducing adaptor protein-2 has a nonredundant role for IL-33-triggered mast cell activation.

Author

Kashiwakura, Jun-ichi, Koizumi, Nao, Saitoh, Kodai, Kagohashi, Kota, Sasaki, Yuto, Kobayashi, Fuki, Kawahara, Shoya, Yamauchi, Yukie, Kitai, Yuichi, Muromoto, Ryuta, Oritani, Kenji, and Matsuda, Tadashi

Subjects

*CELL physiology, *CELLULAR signal transduction, *ADAPTOR proteins, *CYTOKINES, *PHOSPHORYLATION, *MAST cells

Abstract

Signal-transducing adaptor protein (STAP)-2 is one of the STAP family adaptor proteins and ubiquitously expressed in a variety types of cells. Although STAP-2 is required for modification of FcεRI signal transduction in mast cells, other involvement of STAP-2 in mast cell functions is unknown, yet. In the present study, we mainly investigated functional roles of STAP-2 in IL-33-induced mast cell activation. In STAP-2-deficient, but not STAP-1-deficient, mast cells, IL-33-induced IL-6 and TNF-α production was significantly decreased compared with that of wild-type mast cells. In addition, STAP-2-deficiency greatly reduced TLR4-mediated mast cell activation and cytokine production. For the mechanisms, STAP-2 directly binds to IKKα after IL-33 stimulation, leading to elevated NF-κB activity. In conclusion, STAP-2, but not STAP-1, participates in IL-33-induced mast cells activation. [Display omitted] • We sought to investigate role of STAP-2 for IL-33-mediated mast cell activation. • STAP-2, but not STAP-1, is required for IL-33-induced full mast cell activation. • STAP-2 affects NF-κB signal pathway without its phosphorylation after IL-33 stimulation. [ABSTRACT FROM AUTHOR]

Published

2021

3. Propolis suppresses cytokine production in activated basophils and basophil-mediated skin and intestinal allergic inflammation in mice.

Author

Kashiwakura, Jun-ichi, Yoshihara, Mari, Saitoh, Kodai, Kagohashi, Kota, Sasaki, Yuto, Kobayashi, Fuki, Inagaki, Iori, Kitai, Yuichi, Muromoto, Ryuta, and Matsuda, Tadashi

Subjects

*PROPOLIS, *BASOPHILS, *CYTOKINES, *INTESTINES, *LABORATORY mice

Abstract

Propolis is a resinous mixture produced by honey bees that contains cinnamic acid derivatives and flavonoids. Although propolis has been reported to inhibit mast cell functions and mast cell-dependent allergic responses, the effect of propolis on basophil biology remains unknown. This study aimed to investigate the inhibitory effect of propolis on FcεRI-mediated basophil activation. To determine the inhibitory effect of propolis on basophil activation in vitro , cytokine production and FcεRI signal transduction were analyzed by ELISA and western blotting, respectively. To investigate the inhibitory effect of propolis in vivo , IgE-CAI and a food allergy mouse model were employed. Propolis treatment resulted in the suppression of IgE/antigen-induced production of IL-4, IL-6 and IL-13 in basophils. Phosphorylation of FcεRI signaling molecules Lyn, Akt and ERK was inhibited in basophils treated with propolis. While propolis did not affect the basophil population in the treated mice, propolis did inhibit IgE-CAI. Finally, ovalbumin-induced intestinal anaphylaxis, which involves basophils and basophil-derived IL-4, was attenuated in mice prophylactically treated with propolis. Taken together, these results demonstrate the ability of propolis to suppress IgE-dependent basophil activation and basophil-dependent allergic inflammation. Therefore, prophylactic treatment with propolis may be useful for protection against food allergic reactions in sensitive individuals. [ABSTRACT FROM AUTHOR]

Published

2021

4. Higher PGD2 production by synovial mast cells from rheumatoid arthritis patients compared with osteoarthritis patients via miR-199a-3p/prostaglandin synthetase 2 axis.

Author

Mishima, Shintaro, Kashiwakura, Jun-ichi, Toyoshima, Shota, Sasaki-Sakamoto, Tomomi, Sano, Yutaka, Nakanishi, Kazuyoshi, Matsumoto, Kenji, and Okayama, Yoshimichi

Subjects

*PROSTAGLANDINS, *RHEUMATOID arthritis, *MAST cells, *OSTEOARTHRITIS, *MICRORNA

Abstract

We previously reported that synovial mast cells (MCs) from patients with rheumatoid arthritis (RA) produced TNF-α in response to immune complexes via FcγRI and FcγRIIA. However, the specific functions of synovial MCs in RA remain unclear. This study aimed to elucidate those functions. Synovial tissues and fluid were obtained from RA and osteoarthritis (OA) patients undergoing joint replacement surgery. Synovium-derived, cultured MCs were generated by culturing dispersed synovial cells with stem cell factor. We performed microarray-based screening of mRNA and microRNA (miRNA), followed by quantitative RT-PCR-based verification. Synovial MCs from RA patients showed significantly higher prostaglandin systhetase (PTGS)1 and PTGS2 expression compared with OA patients' MCs, and they produced significantly more prostaglandin D2 (PGD2) following aggregation of FcγRI. PGD2 induced IL-8 production by human group 2 innate lymphoid cells, suggesting that PGD2-producing MCs induce neutrophil recruitment into the synovium of RA patients. PTGS2 mRNA expression in RA patients' MCs correlated inversely with miRNA-199a-3p expression, which down-regulated PTGS2. RA patients' synovial fluid contained significantly more PGD2 compared with OA patients' fluid. Synovial MCs might regulate inflammation in RA through hyper-production of PGD2 following FcRγ aggregation. Our findings indicate functional heterogeneity of human MCs among diseases. [ABSTRACT FROM AUTHOR]

Published

2021

5. Expression of signal-transducing adaptor protein-1 attenuates experimental autoimmune hepatitis via down-regulating activation and homeostasis of invariant natural killer T cells.

Author

Kashiwakura, Jun-ichi, Saitoh, Kodai, Ihara, Takeru, Sasaki, Yuto, Kagohashi, Kota, Enohara, Shiyo, Morioka, Yuka, Watarai, Hiroshi, Muromoto, Ryuta, Kitai, Yuichi, Iwabuchi, Kazuya, Oritani, Kenji, and Matsuda, Tadashi

Subjects

*CYTOTOXIC T cells, *CHRONIC active hepatitis, *MITOGEN-activated protein kinases, *ALANINE aminotransferase, *HOMEOSTASIS, *ADAPTOR proteins

Abstract

Objective: Signal-transducing adaptor protein (STAP) family members function as adaptor molecules and are involved in several events during immune responses. Notably however, the biological functions of STAP-1 in other cells are not known. We aimed to investigate the functions of STAP-1 in invariant natural killer T (iNKT) cells and iNKT cell-dependent hepatitis. Methods: We employed concanavalin A (Con A)-induced hepatitis and α-galactosylceramide (α-GalCer)-induced hepatitis mouse models, both are models of iNKT cell-dependent autoimmune hepatitis, and STAP-1 overexpressing 2E10 cells to investigate the role of STAP-1 in iNKT cell activation in vivo an in vitro, respectively. Results: After Con A- or α-GalCer-injection, hepatocyte necrotic areas and plasma alanine aminotransferase elevation were more severe in STAP-1 knockout (S1KO) mice and milder in lymphocyte-specific STAP-1 transgenic (S1Tg) mice, as compared to wild-type (WT) mice. Two events that may be related to Con A-induced and/or α-GalCer-induced hepatitis were influenced by STAP-1 manipulation. One is that iNKT cell populations in the livers and spleens were increased in S1KO mice and were decreased in S1Tg mice. The other is that Con A-induced interleukin-4 and interferon-γ production was attenuated by STAP-1 overexpression. These effects of STAP-1 were confirmed using 2E10 cells overexpressing STAP-1 that showed impairment of interleukin-4 and interferon-γ production as well as phosphorylation of Akt and mitogen-activated protein kinases in response to Con A stimulation. Conclusions: These results conclude that STAP-1 regulates iNKT cell maintenance/activation, and is involved in the pathogenesis of autoimmune hepatitis. [ABSTRACT FROM AUTHOR]

Published

2020

6. The basophil‐IL‐4‐mast cell axis is required for food allergy.

Author

Kashiwakura, Jun‐Ichi, Ando, Tomoaki, Karasuyama, Hajime, Kubo, Masato, Matsumoto, Kenji, Matsuda, Tadashi, and Kawakami, Toshiaki

Subjects

*FOOD allergy, *OVALBUMINS, *MAST cell disease, *MEDICAL sciences, *THYMIC stromal lymphopoietin

Abstract

Keywords: basophil; food allergy; IgE; IL-4; mast cell Despite this assumption and the fact that basophils express the SB 2 sb -type Fc RI-like mast cells, their role in food allergy is less well characterized than that of mast cells. In previous studies using mice sensitized epicutaneously with OVA, basophil-depleted mice were shown to not produce OVA-specific IgE and to be protected from oral OVA challenge-induced anaphylaxis.[[3]] Attenuation of food allergy signs was also observed in basophil-depleted mice in an intradermal OVA + TSLP (thymic stromal lymphopoietin)-sensitization/OVA gavage model.[5] However, the role of basophils in the effector phase of food allergy has not been assessed. Basophil, food allergy, IgE, IL-4, mast cell. [Extracted from the article]

Published

2019

7. STAP-2 positively regulates FcεRI-mediated basophil activation and basophil-dependent allergic inflammatory reactions.

Author

Kashiwakura, Jun-ichi, Yamashita, Shinsuke, Yoshihara, Mari, Inui, Kyosuke, Saitoh, Kodai, Sekine, Yuichi, Muromoto, Ryuta, Kitai, Yuichi, Oritani, Kenji, and Matsuda, Tadashi

Subjects

*BASOPHILS, *ALLERGIES, *ONTOGENY, *IMMUNOREGULATION, *ANTIALLERGIC agents, *CELLULAR control mechanisms, *IMMUNOGLOBULIN E, *MAST cells

Abstract

Basophils are an important cell type in the regulation of Th2 immune responses. Recently, we revealed that signal-transducing adaptor protein-2 (STAP-2) negatively regulates mast cell activation via FcεRI. However, the role of STAP-2 in basophil maturation and activation remained unclear. In this study, we demonstrated the normal development of basophils in STAP-2-deficient (STAP-2−/−) mice. We also demonstrated in vitro normal basophil differentiation and FcεRI expression in STAP-2−/− mice, suggesting that STAP-2 is dispensable for basophil maturation. Using bone marrow-derived cultured basophils (BMBs), we showed that degranulation and cytokine production of STAP-2−/− BMBs were lower than those of wild-type (WT) BMBs upon stimulation with IgE/Ag. In accordance with the reduction of degranulation and cytokine production, phosphorylation of several signal molecules such as Lyn, PLC-γ2 and Erk was reduced in STAP-2−/− BMBs after stimulation via FcεRI. Finally, it was observed that IgE-dependent chronic allergic inflammation of STAP-2−/− mice was significantly inhibited compared with WT mice. Taken together, we conclude that STAP-2 is an adaptor molecule that positively regulates FcεRI-mediated basophil activation and basophil-dependent allergic inflammatory reactions. [ABSTRACT FROM AUTHOR]

Published

2019

8. Crystal structures of murine and human Histamine-Releasing Factor (HRF/TCTP) and a model for HRF dimerisation in mast cell activation.

Author

Doré, Katy A., Kashiwakura, Jun-ichi, McDonnell, James M., Gould, Hannah J., Kawakami, Toshiaki, Sutton, Brian J., and Davies, Anna M.

Subjects

*CRYSTAL structure, *HISTAMINE release, *DIMERIZATION, *MAST cell disease, *LABORATORY mice

Abstract

In allergic disease, mast cell activation is conventionally triggered by allergen-mediated cross-linking of receptor-bound IgE on the cell surface. In addition to its diverse range of intracellular roles in apoptosis, cell proliferation and cancer, Histamine-Releasing Factor (HRF) also activates mast cells and basophils. A subset of IgE antibodies bind HRF through their Fab regions, and two IgE binding sites on HRF have been mapped. HRF can form dimers, and a disulphide-linked dimer is critical for activity. The current model for the activity of HRF in mast cell activation involves cross-linking of receptor-bound IgE by dimeric HRF, mediated by HRF/Fab interactions. HRF crystal and solution structures have provided little insight into either the formation of disulphide-linked HRF dimers or the ability of HRF to activate mast cells. We report the first crystal structure of murine HRF (mHRF) to 4.0 Å resolution, revealing a conserved fold. We also solved the structure of human HRF (hHRF) in two new crystal forms, one at the highest resolution (1.4 Å) yet reported. The high resolution hHRF structure reveals a disulphide-linked dimer, in which the two molecules are closely associated, and provides a model for the role of both human and murine HRF in mast cell activation. [ABSTRACT FROM AUTHOR]

Published

2018

9. Interleukin-33 Synergistically Enhances Immune Complex-Induced Tumor Necrosis Factor Alpha and Interleukin-8 Production in Cultured Human Synovium-Derived Mast Cells.

Author

Kashiwakura, Jun-ichi, Yanagisawa, Masahiko, Lee, Hyunho, Okamura, Yuki, Sasaki-Sakamoto, Tomomi, Saito, Shu, Tokuhashi, Yasuaki, Ra, Chisei, and Okayama, Yoshimichi

Subjects

*MAST cells, *TUMOR necrosis factors, *INTERLEUKINS, *CELL culture, *RHEUMATOID arthritis, *IMMUNOGLOBULIN G

Abstract

Background: Substantial evidence suggests that human synovial mast cells (MCs) are involved in the pathogenesis of rheumatoid arthritis (RA). Interleukin (IL)-33 is believed to play an important role in the pathogenesis of RA. We recently reported that FcγRI is responsible for producing abundant tumor necrosis factor alpha (TNF-α) from cultured synovium-derived MCs (SyMCs) in response to aggregated immunoglobulin G (IgG). However, whether or not IL-33 affects immune complex (IC)-induced synovial MC activation remains unknown. This study sought to evaluate the effect of IL-33 on IC-induced synovial MC activation. Methods: Cultured SyMCs were generated by culturing synovial cells with stem cell factor. ST2 expression was analyzed using FACS and immunohistochemical techniques. Mediators released from the MCs were measured using EIAs or ELISAs. Results: SyMCs obtained from patients with RA or osteoarthritis (OA) expressed ST2 on their surfaces. We confirmed the expression of ST2 in MCs using immunofluorescence staining in joint tissue obtained from RA patients. IC-triggered histamine release was not enhanced by IL-33. However, IL-33 synergistically enhanced IC-induced IL-8 and TNF-α production in SyMCs. Conclusions: ICs and IL-33 may exacerbate inflammation associated with RA by abundantly producing TNF-α and IL-8 from SyMCs. Copyright © 2013 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2013

10. Significantly High Levels of Anti-dsDNA Immunoglobulin E in Sera and the Ability of dsDNA to Induce the Degranulation of Basophils from Chronic Urticaria Patients.

Author

Kashiwakura, Jun-ichi, Hayama, Koremasa, Fujisawa, Daisuke, Sasaki-Sakamoto, Tomomi, Terui, Tadashi, Ra, Chisei, and Okayama, Yoshimichi

Subjects

*IMMUNOGLOBULIN E, *BASOPHILS, *URTICARIA, *DNA, *AUTOIMMUNE diseases, *BLOOD serum analysis, *ENZYME-linked immunosorbent assay

Abstract

Background: Chronic urticaria (CU) appears to be of autoimmune origin in about half of all patients, since several autoreactive immunoglobulin Gs (IgGs), such as anti-FcεRIα and anti-IgE, are detected in the sera of such patients. However, whether autoreactive IgE is associated with CU remains unclear. In this study, we attempted to identify autoreactive IgE antibodies in sera from patients with CU. Methods: Sera were collected from 67 normal subjects, 85 patients with CU and 28 patients with atopic dermatitis (AD). An autologous serum skin test (ASST) was performed on 27 of the CU patients. Autoreactive IgE and IgG levels against self-antigens were measured using enzyme-linked immunosorbent assays. The basophils were activated with dsDNA, and the CD63 expression level was examined using a fluorescence-activated cell sorter. Results: The anti-dsDNA IgE levels were significantly higher in patients with CU and AD than in normal subjects, but no differences in the anti-dsDNA IgG levels were seen. The levels of thioredoxin-, peroxiredoxin- and thyroglobulin-reactive IgE and IgG were not significantly higher in the CU patients than in the other 2 groups. There was no significant difference in the levels of anti-dsDNA IgE between ASST-positive and ASST-negative patients. The basophils from 2 out of 9 CU patients exhibited degranulation in response to dsDNA. Conclusions: Our data suggest that anti-dsDNA IgE is involved in the pathogenesis of some cases of CU. Copyright © 2013 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2013

11. Activation of human synovial mast cells from rheumatoid arthritis or osteoarthritis patients in response to aggregated IgG through Fcγ receptor I and Fcγ receptor II.

Author

Lee, Hyunho, Kashiwakura, Jun-Ichi, Matsuda, Akira, Watanabe, Yasuo, Sakamoto-Sasaki, Tomomi, Matsumoto, Kenji, Hashimoto, Noriko, Saito, Shu, Ohmori, Kazumitsu, Nagaoka, Masahiro, Tokuhashi, Yasuaki, Ra, Chisei, and Okayama, Yoshimichi

Abstract

Objective Substantial evidence suggests that human synovial mast cells (MCs) are involved in the pathogenesis of rheumatoid arthritis (RA). A plausible pathway for the activation of synovial MCs is through IgG receptors, given the prevalence of circulating IgG isotype autoantibodies and synovial immune complexes in patients with RA. However, IgG receptor expression on human synovial MCs remains uncharacterized. The aim of this study was to identify which IgG receptor(s) on synovial MCs are responsible for MC activation in immune complexes. Methods Synovial tissue specimens were obtained from patients with RA or patients with osteoarthritis (OA) who were undergoing joint replacement surgery, and synovial MCs were enzymatically dispersed. Cultured synovium-derived MCs were generated by culturing synovial cells with stem cell factor, and receptor expression was analyzed using fluorescence-activated cell sorting. Mediators released from MCs were measured using enzyme immunoassays or enzyme-linked immunosorbent assays. Results Primary synovial MCs and cultured synovium-derived MCs obtained from both patients with RA and patients with OA expressed Fcε receptor I (FcεRI), FcγRI, and FcγRII but not FcγRIII. Cultured synovium-derived MCs induced degranulation and the production of prostaglandin D2 and tumor necrosis factor α (TNFα) through FcγRI. The aggregation of FcγRII caused histamine release from cultured MCs but not from primary MCs. Histamine release induced by aggregated IgG was significantly inhibited by neutralizing anti-FcγRI monoclonal antibody and anti-FcγRII monoclonal antibody. Conclusion With regard to the FcR expression profile, synovial MCs from patients with RA and patients with OA were similar. FcγRI was responsible for producing abundant TNFα from synovial MCs in response to aggregated IgG. Immune complexes may activate synovial MCs through FcγRI and FcγRII. [ABSTRACT FROM AUTHOR]

Published

2013

12. Activation of human synovial mast cells from rheumatoid arthritis or osteoarthritis patients in response to aggregated IgG through Fcγ receptor I and Fcγ receptor II.

Author

Lee, Hyunho, Kashiwakura, Jun‐Ichi, Matsuda, Akira, Watanabe, Yasuo, Sakamoto‐Sasaki, Tomomi, Matsumoto, Kenji, Hashimoto, Noriko, Saito, Shu, Ohmori, Kazumitsu, Nagaoka, Masahiro, Tokuhashi, Yasuaki, Ra, Chisei, and Okayama, Yoshimichi

Subjects

*MAST cell physiology, *CELL receptors, *ENZYME-linked immunosorbent assay, *FLOW cytometry, *IMMUNOGLOBULINS, *IMMUNOHISTOCHEMISTRY, *OSTEOARTHRITIS, *RESEARCH funding, *RHEUMATOID arthritis, *U-statistics, *CELL physiology

Abstract

Objective Substantial evidence suggests that human synovial mast cells (MCs) are involved in the pathogenesis of rheumatoid arthritis (RA). A plausible pathway for the activation of synovial MCs is through IgG receptors, given the prevalence of circulating IgG isotype autoantibodies and synovial immune complexes in patients with RA. However, IgG receptor expression on human synovial MCs remains uncharacterized. The aim of this study was to identify which IgG receptor(s) on synovial MCs are responsible for MC activation in immune complexes. Methods Synovial tissue specimens were obtained from patients with RA or patients with osteoarthritis (OA) who were undergoing joint replacement surgery, and synovial MCs were enzymatically dispersed. Cultured synovium-derived MCs were generated by culturing synovial cells with stem cell factor, and receptor expression was analyzed using fluorescence-activated cell sorting. Mediators released from MCs were measured using enzyme immunoassays or enzyme-linked immunosorbent assays. Results Primary synovial MCs and cultured synovium-derived MCs obtained from both patients with RA and patients with OA expressed Fcε receptor I (FcεRI), FcγRI, and FcγRII but not FcγRIII. Cultured synovium-derived MCs induced degranulation and the production of prostaglandin D2 and tumor necrosis factor α (TNFα) through FcγRI. The aggregation of FcγRII caused histamine release from cultured MCs but not from primary MCs. Histamine release induced by aggregated IgG was significantly inhibited by neutralizing anti-FcγRI monoclonal antibody and anti-FcγRII monoclonal antibody. Conclusion With regard to the FcR expression profile, synovial MCs from patients with RA and patients with OA were similar. FcγRI was responsible for producing abundant TNFα from synovial MCs in response to aggregated IgG. Immune complexes may activate synovial MCs through FcγRI and FcγRII. [ABSTRACT FROM AUTHOR]

Published

2013

13. Histamine-releasing factor has a proinflammatory role in mouse models of asthma and allergy.

Author

Kashiwakura, Jun-ichi, Ando, Tomoaki, Matsumoto, Kenji, Kimura, Miho, Kitaura, Jiro, Matho, Michael H., Zajonc, Dirk M., Ozeki, Tomomitsu, Ra, Chisei, MacDonald, Susan M., Siraganian, Reuben P., Broide, David H., Kawakami, Yuko, and Kawakami, Toshiaki

Subjects

*MAST cells, *BASOPHILS, *ASTHMA, *HISTAMINE, *TUMOR proteins

Abstract

IgE-mediated activation of mast cells and basophils underlies allergic diseases such as asthma. Histamine-releasing factor (HRF; also known as translationally controlled tumor protein [TCTP] and fortilin) has been implicated in late-phase allergic reactions (LPRs) and chronic allergic inflammation, but its functions during asthma are not well understood. Here, we identified a subset of IgE and IgG antibodies as HRF-interacting molecules in vitro. HRF was able to dimerize and bind to Igs via interactions of its N-terminal and internal regions with the Fab region of Igs. Therefore, HRF together with HRF-reactive IgE was able to activate mast cells in vitro. In mouse models of asthma and allergy, Ig-interacting HRF peptides that were shown to block HRF/Ig interactions in vitro inhibited IgE/HRF-induced mast cell activation and in vivo cutaneous anaphylaxis and airway inflammation. Intranasally administered HRF recruited inflammatory immune cells to the lung in naive mice in a mast cell-- and Fc receptor--dependent manner. These results indicate that HRF has a proinflammatory role in asthma and skin immediate hypersensitivity, leading us to suggest HRF as a potential therapeutic target. [ABSTRACT FROM AUTHOR]

Published

2012

14. Phospholipase C-β3 Regulates FcɛRI-Mediated Mast Cell Activation by Recruiting the Protein Phosphatase SHP-1

Author

Xiao, Wenbin, Kashiwakura, Jun-ichi, Hong, Hong, Yasudo, Hiroki, Ando, Tomoaki, Maeda-Yamamoto, Mari, Wu, Dianqing, Kawakami, Yuko, and Kawakami, Toshiaki

Subjects

*PHOSPHOLIPASE C, *MAST cells, *CELLULAR control mechanisms, *PHOSPHOPROTEIN phosphatases, *IMMUNOGLOBULIN E, *ALLERGIES, *ANAPHYLAXIS, *INFLAMMATION

Abstract

Summary: Mast cells are major effectors in high-affinity IgE receptor (FcɛRI)-dependent allergic reactions. Here we show that phospholipase C (PLC)-β3 is crucial for FcɛRI-mediated mast cell activation. Plcb3−/− mice showed blunted FcɛRI-dependent late-phase, but not acute, anaphylactic responses and airway inflammation. Accordingly, FcɛRI stimulation of Plcb3−/− mast cells exhibited reduced cytokine production but normal degranulation. Reduced cytokine production in Plcb3−/− cells could be accounted for by increased activity of the negative regulatory Src family kinase Lyn and reduced activities of the positive regulatory protein kinases MAPKs. Mechanistically, PLC-β3 constitutively interacts with FcɛRI, Lyn, and SHP-1 (protein phosphatase). SHP-1 probably recognizes its substrates Lyn and MAPKs via the recently described kinase tyrosine-based inhibitory motif, KTIM. Consistent with PLC-β3- and SHP-1-mediated repression of Lyn activity by dephosphorylation at Tyr396, FcɛRI-mediated phenotypes were similar in Plcb3−/− and SHP-1 mutant mast cells. Thus, we have defined a PLC-β3- and SHP-1-mediated signaling pathway for FcɛRI-mediated cytokine production. [ABSTRACT FROM AUTHOR]

Published

2011

15. JNK1 controls mast cell degranulation and IL-1β production in inflammatory arthritis.

Author

Guma, Monica, Kashiwakura, Jun-ichi, Crain, Brian, Kawakami, Yuko, Beutler, Bruce, Firestein, Gary S., Kawakami, Toshiaki, Karin, Michael, and Corr, Maripat

Subjects

*RHEUMATOID arthritis, *AUTOIMMUNE diseases, *BLOOD hyperviscosity syndrome, *RHEUMATISM, *ARTHRITIS

Abstract

Rheumatoid arthritis (RA) is a chronic inflammatory disease marked by bone and cartilage destruction. Current biologic therapies are beneficial in only a portion of patients; hence small molecules targeting key pathogenic signaling cascades represent alternative therapeutic strategies. Here we show that c-Jun N-terminal kinase (iNK) 1, but not JNK2, is critical for joint swelling and destruction in a serum transfer model of arthritis. The proinflammatory function of JNK1 requires bone marrow-derived cells, particularly mast cells. Without JNK1, mast cells fail to degranulate efficiently and release less lL-1γ after stimulation via Fcγ receptors (FcγRs). Pharmacologic JNK inhibition effectively prevents arthritis onset and abrogates joint swelling in established disease. Hence, JNK1 controls mast cell degranulation and FcγR-triggered lL-1β production, in addition to regulating cytokine and matrix metalloproteinase biosynthesis, and is an attractive therapeutic target in inflammatory arthritis. [ABSTRACT FROM AUTHOR]

Published

2010

16. Polyclonal IgE Induces Mast Cell Survival and Cytokine Production.

Author

Kashiwakura, Jun-ichi, Kawakami, Yuko, Yuki, Keisuke, Zajonc, Dirk M., Hasegawa, Shunji, Tomimori, Yoshiaki, Caplan, Benjamin, Saito, Hirohisa, Furue, Masutaka, Oettgen, Hans C., Okayama, Yoshimichi, and Kawakami, Toshiaki

Subjects

*IMMUNOGLOBULIN E, *MAST cells, *CYTOKINES, *ALLERGIES, *MONOCLONAL antibodies, *LABORATORY mice, *ATOPIC dermatitis

Abstract

Background: Ag-dependent activation of IgE-bearing mast cells is a critical first step in immediate hypersensitivity and other allergic responses. Recent studies have revealed Ag-independent effects of monoclonal mouse IgE molecules on mast cell survival and activation. However, no studies have been performed on the effects of polyclonal IgE molecules. Here, we tested whether polyclonal mouse and human IgE molecules affect survival and cytokine production in mast cells. Methods: Mast cells were cultured in the presence of polyclonal mouse and human IgE molecules, and cell survival and cytokine production were analyzed. Results: Polyclonal mouse IgE molecules in sera from mice with atopic dermatitis-like allergic skin inflammaion, enhanced survival and cytokine production in mast cell cultures. Similar to the effects of monoclonal IgE, he polyclonal IgE effects were mediated by the high-affinity IgE receptor, FcεRI. Human polyclonal IgE molecules present in sera from atopic dermatitis patients were also capable of activating mast cells, and inducing IL8 production in human cord blood-derived mast cells. Conclusions: These results imply that polyclonal IgE in atopic dermatitis and other atopic conditions might modulate mast cell number and function, thus amplifying the allergic response. [ABSTRACT FROM AUTHOR]

Published

2009

17. Correction: Expression of signal-transducing adaptor protein-1 attenuates experimental autoimmune hepatitis via down-regulating activation and homeostasis of invariant natural killer T cells.

Author

Kashiwakura, Jun-ichi, Saitoh, Kodai, Ihara, Takeru, Sasaki, Yuto, Kagohashi, Kota, Enohara, Shiyo, Morioka, Yuka, Watarai, Hiroshi, Muromoto, Ryuta, Kitai, Yuichi, Iwabuchi, Kazuya, Oritani, Kenji, and Matsuda, Tadashi

Subjects

*CYTOTOXIC T cells, *CHRONIC active hepatitis, *HOMEOSTASIS

Abstract

The following information is missing from the Funding statement: This work was supported in part by JSPS KAKENHI Grants 19H03364 (T.M.) & 16K09872 (K.O.). Reference 1 Kashiwakura J-i, Saitoh K, Ihara T, Sasaki Y, Kagohashi K, Enohara S, et al. (2020) Expression of signal-transducing adaptor protein-1 attenuates experimental autoimmune hepatitis via down-regulating activation and homeostasis of invariant natural killer T cells. [Extracted from the article]

Published

2021

18. Positive interactions between STAP-1 and BCR-ABL influence chronic myeloid leukemia cell proliferation and survival.

Author

Ishiura, Marie, Kitai, Yuichi, Kashiwakura, Jun-ichi, Muromoto, Ryuta, Toda, Jun, Ichii, Michiko, Oritani, Kenji, and Matsuda, Tadashi

Subjects

*CHRONIC myeloid leukemia, *CELL proliferation, *SCAFFOLD proteins, *ADAPTOR proteins, *MOLECULAR interactions

Abstract

Chronic myeloid leukemia (CML) is a clonal disease characterized by the presence of the Philadelphia chromosome and its oncogenic product, BCR-ABL, which activates multiple pathways involved in cell survival, growth promotion, and disease progression. We recently reported that signal-transducing adaptor protein 1 (STAP-1) is upregulated in CML stem cells (LSCs) and functions to reduce the apoptosis of CML LSCs by upregulating the STAT5-downstream anti-apoptotic genes. In this study, we demonstrate the detailed molecular interactions among BCR-ABL, STAP-1, and signal transducer and activator of transcription 5 (STAT5). Studies with deletion mutants have revealed that STAP-1 interacts with BCR-ABL and STAT5a through its SH2 and PH domains, respectively, suggesting the possible role of STAP-1 as a scaffold protein. Furthermore, the binding of STAP-1 to BCR-ABL stabilizes the BCR-ABL protein in CML cells. Since STAP-1 is highly expressed in CML cells, we also analyzed the STAP-1 promoter activity using a luciferase reporter construct and found that NFATc1 is involved in activating the STAP-1 promoter and inducing STAP-1 mRNA expression. Our results demonstrate that STAP-1 contributes to the BCR-ABL/STAT5 and BCR-ABL/Ca2+/NFAT signals to induce proliferation and STAP-1 mRNA expression in CML cells, respectively. • STAP-1 interacts with BCR-ABL and STAT5a through its SH2 and PH domains, respectively. • STAP-1 stabilizes BCR-ABL protein in CML cells. • NFATc1 is involved in the induction of STAP-1 mRNA expression in CML cells. [ABSTRACT FROM AUTHOR]

Published

2021

19. STAP-2 interacts with Pyk2 and enhances Pyk2 activity in T-cells.

Author

Saitoh, Kodai, Tsuchiya, Takuya, Kashiwakura, Jun-ichi, Muromoto, Ryuta, Kitai, Yuichi, Sekine, Yuichi, Oritani, Kenji, and Matsuda, Tadashi

Subjects

*SPACE-time adaptive signal processing, *CYTOKINES, *CELL communication, *CHEMOTAXIS, *TOLL-like receptors, *PHOSPHORYLATION

Abstract

STAP-2 is an adaptor molecule regulating several signaling pathways, including TLRs and cytokine/chemokine receptors in immune cells. We previously reported that STAP-2 enhances SDF-1α-induced Vav1/Rac1-mediated T-cell chemotaxis. However, the detailed mechanisms of STAP-2 involvement in enhancing T-cell chemotaxis remain unknown. In the present study, we demonstrate that STAP-2 directly interacts with Pyk2, which is a key molecule in the regulation of SDF-1α/CXCR4-mediated T-cell chemotaxis, and increases phosphorylation of Pyk2. Pyk2 itself can induce STAP-2 Y250 phosphorylation, and this phosphorylation is critical for maximal interactions between STAP-2 and Pyk2. Finally, SDF-1α-induced T-cell chemotaxis is inhibited by treatment with Pyk2 siRNA or AG17, an inhibitor of Pyk2, in Jurkat cells overexpressing STAP-2. Taken together, the Pyk2/STAP-2 interaction is a novel mechanism to regulate SDF-1α-dependent T-cell chemotaxis. [ABSTRACT FROM AUTHOR]

Published

2017

20. Regulation of NFKBIZ gene promoter activity by STAT3, C/EBPβ, and STAT1.

Author

Muromoto, Ryuta, Sato, Ami, Komori, Yuki, Nariya, Kota, Kitai, Yuichi, Kashiwakura, Jun-ichi, and Matsuda, Tadashi

Subjects

*STAT proteins, *GENETIC regulation, *TRANSCRIPTION factors, *GENETIC transcription regulation, *BINDING sites

Abstract

Interleukin-17A (IL-17A) is a cytokine that affects the functions of non-immune cells, including keratinocytes, and thereby amplifies immune responses. An IκB family protein IκB-ζ, encoded by the NFKBIZ gene, mediates IL-17A-induced inflammatory cellular responses. Previously we reported that a transcription factor STAT3 mediates the transcriptional induction of NFKBIZ through its binding to the specific binding site existing in the NFKBIZ promoter. However, it remains unclear how other transcription factors regulate NFKBIZ transcription. Here, we investigated the NFKBIZ promoter regulation by transcription factors C/EBPβ and STAT1 and revealed opposing roles of C/EBPβ and STAT1 in NFKBIZ transcription. We found that siRNA-mediated knockdown of C/EBPβ attenuates IL-17A-induced upregulation of NFKBIZ in the HaCaT cell line. A putative C/EBP-binding site is located adjacent to the STAT-binding site in the NFKBIZ promoter, the deletion of which abolished C/EBPβ-driven promoter activation in transient NFKBIZ promoter-luciferase assay. Deleting the STAT-binding site also led to a reduction in C/EBPβ-driven promoter activation, suggesting a cooperative action between C/EBP- and STAT-binding sites. Furthermore, Co-overexpression of STAT1 suppressed both C/EBPβ- and STAT3-driven NFKBIZ promoter activation independently of its tyrosine 701 phosphorylation. siRNA-mediated STAT1 knockdown augmented IκB-ζ induction in IL-17A-treated HaCaT cells, with enhanced expression of an IκB-ζ target gene DEFB4A. Together, these results indicate that both C/EBPβ and STAT3 are transcription factors that coordinately induce NFKBIZ promoter activation, indicating that STAT1 has an inhibitory role. Thus, these could be a fine-tuning mechanism of IL-17A-IκB-ζ-mediated cellular responses. • NFKBIZ promoter regulation by transcription factors was investigated. • C/EBPβ and STAT3 induced NFKBIZ promoter activation. • STAT1 suppressed C/EBPβ- and STAT3-driven NFKBIZ promoter activation. • These could be a fine-tuning mechanism of IκB-ζ-induced cellular responses. [ABSTRACT FROM AUTHOR]

Published

2022

21. novel intramolecular negative regulation of mouse Jak3 activity by tyrosine 820.

Author

Sekine, Yuichi, Kikkawa, Kazuna, Witthuhn, Bruce A, Kashiwakura, Jun-ichi, Muromoto, Ryuta, Kitai, Yuichi, Fujimuro, Masahiro, Oritani, Kenji, and Matsuda, Tadashi

Subjects

*KINASES, *TYROSINE, *CYTOKINE receptors, *MICE, *STAT proteins, *CELL growth

Abstract

Jak3, a member of the Janus kinase family, is essential for the cytokine receptor common gamma chain (γc)-mediated signaling. During activation of Jak3, tyrosine residues are phosphorylated and potentially regulate its kinase activity. We identified a novel tyrosine phosphorylation site within mouse Jak3, Y820, which is conserved in human Jak3, Y824. IL-2-induced tyrosine phosphorylation of Jak3 Y824 in human T cell line HuT78 cells was detected by using a phosphospecific, pY824, antibody. Mutation of mouse Jak3 Y820 to alanine (Y820A) showed increased autophosphorylation of Jak3 and enhanced signal transducer and activator of transcription 5 (STAT5) tyrosine phosphorylation and transcriptional activation. Stably expressed Jak3 Y820A in F7 cells, an IL-2 responsive mouse pro-B cell line Ba/F3, exhibited enhanced IL-2-dependent cell growth. Mechanistic studies demonstrated that interaction between Jak3 and STAT5 increased in Jak3 Y820A compared to wild-type Jak3. These data suggest that Jak3 Y820 plays a role in negative regulation of Jak3-mediated STAT5 signaling cascade upon IL-2-stimulation. We speculate that this occurs through an interaction promoted by the tyrosine phosphorylated Y820 or a conformational change by Y820 mutation with either the STAT directly or with the recruitment of molecules such as phosphatases via a SH2 interaction. Additional studies will focus on these interactions as Jak3 plays a crucial role in disease and health. [ABSTRACT FROM AUTHOR]

Published

2022

22. Human CD300C Delivers an Fc Receptor-γ-dependent Activating Signal in Mast Cells and Monocytes and Differs from CD300A in Ligand Recognition.

Author

Takahashi, Mariko, Izawa, Kumi, Kashiwakura, Jun-ichi, Yamanishi, Yoshinori, Enomoto, Yutaka, Kaitani, Ayako, Maehara, Akie, Isobe, Masamichi, Ito, Shinichi, Matsukawa, Toshihiro, Nakahara, Fumio, Oki, Toshihiko, Kajikawa, Masunori, Ra, Chisei, Okayama, Yoshimichi, Kitamura, Toshio, and Kitaura, Jiro

Subjects

*MONOCYTES, *MAST cells, *IMMUNOGLOBULINS, *CHEMOKINES, *CYTOKINES

Abstract

D300C is highly homologous with an inhibitory receptor CD300A in an immunoglobulin-like domain among the human CD300 family of paired immune receptors. To clarify the precise expression and function of CD300C, we generated antibodies discriminating between CD300A and CD300C, which recognized a unique epitope involving amino acid residues CD300A(F56-L57) and CD300C(L63-R64). Notably, CD300C was highly expressed in human monocytes and mast cells. Cross-linking of CD300C by its specific antibody caused cytokine/ chemokine production of human monocytes and mast cells. Fc receptor γ was indispensable for both efficient surface expression and activating functions of CD300C. To identify a ligand for CD300A or CD300C, we used reporter cell lines expressing a chimera receptor harboring extracellular CD300A or CD300C and intracellular CD3ζ, in which its unknown ligand induced GFP expression. Our results indicated that phosphatidylethanolamine (PE) among the lipids tested and apoptotic cells were possible ligands for both CD300C and CD300A. PE and apoptotic cells more strongly inducedGFPexpression in the reporter cells through binding to extracellular CD300A as compared with CD300C. Differential recognition of PE by extracellular CD300A and CD300C depended on different amino acid residues CD300A(F56-L57) and CD300C(L63-R64). Interestingly, GFP expression induced by extracellular CD300C-PE binding in the reporter cells was dampened by co-expression of full-length CD300A, indicating the predominance of CD300A over CD300C in PE recognition/signaling. PE consistently failed to stimulate cytokine production in monocytes expressing CD300C with CD300A. In conclusion, specific engagement of CD300C led to Fc receptor γ-dependent activation of mast cells and monocytes. [ABSTRACT FROM AUTHOR]

Published

2013

23. CD47 promotes T-cell lymphoma metastasis by up-regulating AKAP13-mediated RhoA activation.

Author

Kitai, Yuichi, Ishiura, Marie, Saitoh, Kodai, Matsumoto, Naoki, Owashi, Kimiya, Yamada, Shunsuke, Muromoto, Ryuta, Kashiwakura, Jun-ichi, Oritani, Kenji, and Matsuda, Tadashi

Subjects

*T-cell lymphoma, *GUANINE nucleotide exchange factors, *METASTASIS, *THERAPEUTICS, *MEMBRANE proteins

Abstract

CD47, a 50 kDa transmembrane protein, facilitates integrin-mediated cell adhesion and inhibits cell engulfment by phagocytes. Since CD47 blocking promotes engulfment of cancer cells by macrophages, it is important to clarify the mechanism of CD47 signaling in order to develop treatments for diseases involving CD47-overexpressing cancer cells, including breast cancer and lymphoma. Here, we show that CD47 plays an essential role in T-cell lymphoma metastasis by up-regulating basal RhoA activity independent of its anti-phagocytic function. CD47 interacts with AKAP13, a RhoA-specific guanine nucleotide exchange factor (GEF), and facilitates AKAP13-mediated RhoA activation. Our study shows that CD47 has a novel function on the AKAP13-RhoA axis and suggests that CD47–AKAP13 interaction would be a novel target for T-cell lymphoma treatment. [ABSTRACT FROM AUTHOR]

Published

2021

24. Graft-versus-host disease develops in mice transplanted with lymphocyte-depleted bone marrow cells from signal-transducing adaptor protein-2 transgenic mice.

Author

Saito, Hideaki, Ichii, Michiko, Toda, Jun, Kitai, Yuichi, Muromoto, Ryuta, Kashiwakura, Jun-ichi, Saitoh, Kodai, Tanimura, Akira, Yokota, Takafumi, Shibayama, Hirohiko, Matsuda, Tadashi, Oritani, Kenji, Kanakura, Yuzuru, and Hosen, Naoki

Subjects

*BONE marrow cells, *TRANSGENIC mice, *GRAFT versus host disease, *HEMATOPOIETIC stem cell transplantation, *HEMATOPOIETIC system, *PROGENITOR cells

Abstract

Graft-versus-host disease (GVHD) is the most frequent complication after allogeneic hematopoietic stem cell transplantation (HSCT), and is one of the major causes of non-relapse mortality. Transferred mature lymphocytes are thought to be responsible for GVHD based on the findings that mice transplanted with lymphocyte-depleted bone marrow (BM) cells from MHC-mismatched donors do not develop GVHD. However, we found that overexpression of signal-transducing adaptor protein (STAP)-2 in lymphoid cells could induce GVHD after lymphocyte-depleted BM transplantation. To examine the function of STAP-2, which has been shown to play an important role in development and function of lymphocytes, in GVHD, we transplanted BM cells from STAP-2 deficient, or Lck promoter/IgH enhancer-driven STAP-2 transgenic (Tg) mice into MHC-mismatched recipients. Unexpectedly, mice transplanted with lymphocyte-depleted BM cells from STAP-2 Tg mice developed severe acute GVHD with extensive colitis and atrophy of thymus, while no obvious GVHD developed in mice transplanted with the wild type or STAP-2 deficient graft. Furthermore, mice transplanted with lymphocyte-depleted BM cells from the syngeneic STAP-2 Tg mice developed modest GVHD with colitis and atrophy of thymus. These results suggest that STAP-2 overexpression may enhance survival of allo-, and even auto-, reactive lymphocytes derived from engrafted hematopoietic progenitor cells in lethally irradiated mice, and that clarification of the mechanism may help understanding induction of immune tolerance after HSCT. • GVHD was induced by STAP-2 overexpression in allogeneic lymphocyte-depleted BMT. • Even in syngeneic transplantation, GVHD was induced by STAP-2 overexpression. • STAP-2 plays an important role in GVHD. [ABSTRACT FROM AUTHOR]

Published

2021

25. Dimethyl fumarate dampens IL-17-ACT1-TBK1 axis-mediated phosphorylation of Regnase-1 and suppresses IL-17–induced IκB-ζ expression.

Author

Ohgakiuchi, Yui, Saino, Yuka, Muromoto, Ryuta, Komori, Yuki, Sato, Ami, Hirashima, Koki, Kitai, Yuichi, Kashiwakura, Jun-ichi, Oritani, Kenji, and Matsuda, Tadashi

Subjects

*NF-kappa B, *SMALL interfering RNA, *SMALL molecules, *GLYCOPYRROLATE, *PHOSPHORYLATION, *DIMETHYLFORMAMIDE, *DIMETHYL fumarate

Abstract

The signaling elicited by the cytokine interleukin-17A (IL-17) is important for antimicrobial defense responses, whereas excessive IL-17 production leads to autoimmune diseases such as psoriasis and multiple sclerosis. IL-17–induced stabilization of mRNAs has been recognized as a unique and important feature of IL-17 signaling. Previously, we demonstrated that IL-17 signaling protein ACT1 is required to counteract constitutive inhibitor of nuclear factor kappa B zeta (IκB-ζ) mRNA degradation by the ribonuclease Regnase-1. However, information about the mechanism of mRNA stabilization in IL-17–stimulated cells remains insufficient. In the present study, we aimed to clarify the mechanism in more detail and identify an agent that can inhibit IL-17–induced mRNA stabilization. Experiments using small interfering RNA and an inhibitor of TANK-binding kinase 1 (TBK1) revealed that TBK1 was required for IκB-ζ mRNA stabilization through Regnase-1 phosphorylation. Intriguingly, this TBK1-mediated phosphorylation of Regnase-1 was suppressed by the addition of dimethyl fumarate (DMF), an electrophilic small molecule that has been used to treat IL-17–related autoimmune diseases. Confocal microscopic observation of the cellular localization of ACT1 revealed that DMF treatment resulted in the disappearance of ACT1 nuclear dots and perinuclear accumulation of ACT1. These results suggested that DMF is a small molecule that compromises IL-17–induced activation of the ACT1-TBK1 pathway, thereby inhibiting IL-17–induced mRNA stabilization. • IL-17–induced IκB-ζ mRNA stabilization was mediated by Regnase-1 phosphorylation. • Regnase-1 phosphorylation occurred via the ACT1-TBK1 pathway. • DMF treatment suppressed Regnase-1 phosphorylation. • DMF treatment affected the subcellular localization of ACT1. • DMF appears to inhibit IL-17–induced mRNA stabilization. [ABSTRACT FROM AUTHOR]

Published

2020

26. Differentiation between control subjects and patients with chronic spontaneous urticaria based on the ability of anti-IgE autoantibodies (AAbs) to induce FcεRI crosslinking, as compared to anti-FcεRIα AAbs.

Author

Izaki, Satoshi, Toyoshima, Shota, Endo, Takahiro, Kanegae, Kazuko, Nunomura, Satoshi, Kashiwakura, Jun-ichi, Sasaki-Sakamoto, Tomomi, Nakamura, Ryosuke, Akiyama, Haruyo, Ra, Chisei, Hayama, Koremasa, Terui, Tadashi, and Okayama, Yoshimichi

Subjects

*URTICARIA, *IMMUNOGLOBULIN E, *AUTOANTIBODIES, *HISTAMINE

Abstract

The reported prevalences of IgG autoantibodies (AAbs) to FcεRIα and IgE in sera from patients with chronic spontaneous urticaria (CSU) have varied, and these AAbs are also often observed in healthy control subjects. Regarding the histamine release activity of purified IgG from patients with CSU, the number of examined patients has been small. Thus, we sought to determine the prevalence and FcεRI crosslinking ability of these AAbs in a large number of patients with CSU and non-atopic control (NC) subjects. We compared the concentrations of anti-IgE and anti-FcεRIα AAbs and the abilities of these AAbs to cause FcεRI aggregation in patients with CSU (n = 134) and NC subjects (n = 55) using ELISA and an in vitro elicitation test, respectively. The concentration of anti-IgE AAbs was significantly different between the NC subjects and the CSU patients (P < 0.0001, cutoff value: 0.558 μg/mL), whereas the concentration of anti-FcεRIα AAbs was not. A significant difference in the duration of illness was noted between patients with lower and those with higher concentrations of anti-IgE AAbs relative to the cutoff value. The abilities of anti-IgE AAbs, but not anti-FcεRIα AAbs, to induce FcεRI crosslinking were significantly higher in CSU patients than in NC subjects (P = 0.0106). In the Japanese population of CSU patients studied, the ability of the anti-IgE AAbs to induce FcεRI crosslinking differed significantly between NC subjects and CSU patients, suggesting the involvement of anti-IgE AAbs in the pathogenesis of CSU in the Japanese population. Image 1 [ABSTRACT FROM AUTHOR]

Published

2019

27. Histamine-releasing factor enhances food allergy.

Author

Jun-ichi Kashiwakura, Tomoaki Ando, Takao Fujisawa, Mizuho Nagao, Kenji Matsumoto, Naoka Itoh-Nagato, Hirotaka Yamashita, Naoki Inagaki, Minato Baba, Yu Kawakami, Yuko Kawakami, Toshiaki Kawakami, Shih Han Tsai, Kiyoshi Takeda, Tsutomu Iwata, Naoki Shimojo, Ando, Tomoaki, Kashiwakura, Jun-Ichi, Itoh-Nagato, Naoka, and Yamashita, Hirotaka

Subjects

*HISTAMINE, *FOOD allergy, *IMMUNOGLOBULIN E, *MAST cell disease, *IMMUNOTHERAPY, *INFLAMMATION, *GENETICS

Abstract

Food allergy occurs due to IgE- and mast cell-dependent intestinal inflammation. Previously, we showed that histamine-releasing factor (HRF), a multifunctional protein secreted during allergy, interacts with a subset of IgE molecules and that the HRF dimer activates mast cells in an HRF-reactive IgE-dependent manner. In this study, we investigated whether HRF plays any role in food allergy. Specifically, we determined that prophylactic and therapeutic administration of HRF inhibitors that block HRF-IgE interactions reduces the incidence of diarrhea and mastocytosis in a murine model of food allergy. Food allergy-associated intestinal inflammation was accompanied by increased secretion of the HRF dimer into the intestine in response to proinflammatory, Th2, and epithelial-derived cytokines and HRF-reactive IgE levels at the elicitation phase. Consistent with these data, patients with egg allergy had higher blood levels of HRF-reactive IgE compared with individuals that were not hypersensitive. Successful oral immunotherapy in egg-allergy patients and food-allergic mice reduced HRF-reactive IgE levels, thereby suggesting a pathological role for HRF in food allergy. Together, these results suggest that antigen and HRF dimer amplify intestinal inflammation by synergistically activating mast cells and indicate that HRF has potential as a therapeutic target in food allergy. [ABSTRACT FROM AUTHOR]

Published

2017

28. The dual regulation of substance P-mediated inflammation via human synovial mast cells in rheumatoid arthritis.

Author

Okamura, Yuki, Mishima, Shintaro, Kashiwakura, Jun-ichi, Sasaki-Sakamoto, Tomomi, Toyoshima, Shota, Kuroda, Kazumichi, Saito, Shu, Tokuhashi, Yasuaki, and Okayama, Yoshimichi

Subjects

*RHEUMATOID arthritis, *INFLAMMATION, *SYNOVIAL fluid, *MAST cells, *OSTEOARTHRITIS

Abstract

Background Neural pathways are thought to be directly involved in the pathogenesis of rheumatoid arthritis (RA). Although synovial mast cells (MCs) are activated by substance P (SP), the role of MCs in neural pathways in RA remains unknown. The aims of this study were to investigate 1) whether tachykinins are produced by synovial MCs and whether production differs in RA and osteoarthritis (OA) patients, and 2) what is the responsible receptor for SP in synovial MCs. Methods Synovial tissues were obtained from patients with RA or OA undergoing joint replacement surgery. Cultured synovium-derived MCs were generated by culturing dispersed synovial cells with stem cell factor. SP expression was investigated using immunofluorescence and enzyme immunoassays. Mas-related gene X2 (MrgX2) expression was reduced in human MCs using a lentiviral shRNA silencing technique. Results SP expression was localized around the cell membrane in 41% (median) of the MCs in synovium from RA but in only 7% of that from OA, suggesting the activation of MCs. Synovial MCs expressed tachykinin (TAC) 1 mRNA, the expression of which was upregulated by the aggregation of FcɛRI or the addition of aggregated IgG. However, the released SP appeared to be rapidly degraded by MC chymase. Synovial MCs were activated with SP through MrgX2 to release histamine without producing proinflammatory cytokines. Conclusions Activated synovial MCs may rapidly degrade SP, which may downregulate the SP-mediated activation of synoviocytes in RA. On the other hand, SP activates MCs to induce inflammatory mediators, suggesting the dual regulation of SP-mediated inflammation by MCs in RA. [ABSTRACT FROM AUTHOR]

Published

2017

29. Biochanin A enhances RORγ activity through STAT3-mediated recruitment of NCOA1.

Author

Takahashi, Miki, Muromoto, Ryuta, Kojima, Hiroyuki, Takeuchi, Shinji, Kitai, Yuichi, Kashiwakura, Jun-ichi, and Matsuda, Tadashi

Subjects

*BIOCHANIN A, *STAT proteins, *AUTOIMMUNITY, *INTERLEUKIN-17, *STEROID receptor coactivators

Abstract

Interleukin (IL)-17-producing T cells play important roles in autoimmunity, chronic inflammation and host protection against extracellular bacteria and fungi. The retinoic acid receptor-related orphan receptors (ROR) α and γ are key regulators of the IL-17-producing phenotype. We previously showed that the isoflavone biochanin A enhanced ROR-mediated transcriptional activity. Here, we investigated the possible mechanisms underlying this ROR activation. Biochanin A-treated murine thymoma EL4 and primary splenocytes demonstrated enhanced induction of IL-17. Biochanin A also induced tyrosine-phosphorylation of signal transducer and activator of transcription 3 (STAT3) in these cells. Stable knockdown of either RORγ or STAT3 in EL4 cells canceled biochanin A-induced upregulation of IL-17 expression. Importantly, biochanin A enhanced complex formation between RORγ and STAT3 or nuclear-receptor coactivator 1 (NCOA1). Furthermore, the biochanin A-induced RORγ-NCOA1 complex was disrupted by a dominant negative mutant of STAT3 or by the STAT3 specific inhibitor Stattic. These results suggest that biochanin A activates RORγ-dependent IL-17 transcription through the enhancement of STAT3 phosphorylation and STAT3-mediated recruitment of NCOA1 to RORγ. [ABSTRACT FROM AUTHOR]

Published

2017

30. Expression of Mas-related gene X2 on skin mast cells is upregulated in the patients with severe chronic spontaneous urticaria.

Author

Hayama, Koremasa, Fujisawa, Daisuke, Kashiwakura, Jun-ichi, Kita, Hirohito, Kikukawa, Yusuke, Fujitani, Yashushi, Sasaki-sakamoto, Tomomi, Kuroda, Kazumichi, Nunomura, Satoshi, Ra, Chisei, Okayama, Yoshimichi, and Terui, Tadashi

Subjects

*URTICARIA, *CHRONIC diseases, *GENE expression, *MAST cells, *SEVERITY of illness index, *GENETICS

Published

2016

31. Interleukin-17A expression in human synovial mast cells in rheumatoid arthritis and osteoarthritis.

Author

Kan, Jun-ichiro, Mishima, Shintaro, Kashiwakura, Jun-ichi, Sasaki-Sakamoto, Tomomi, Okayama, Yoshimichi, Seki, Masayuki, Saito, Shu, Tokuhashi, Yasuaki, and Ra, Chisei

Subjects

*INTERLEUKIN-17, *MAST cells, *SYNOVIAL membranes

Abstract

Background Interleukin (IL)-17A plays a pivotal role in the pathogenesis of rheumatoid arthritis (RA). The expression of IL-17A in synovial mast cells (MCs) in RA and osteoarthritis (OA) has been reported, but the frequencies of IL-17A expression in synovial MCs have varied. The aim of this study was to investigate whether IL-17A expression is upregulated in human synovial MCs in RA and to elucidate the mechanism of IL-17A expression in synovial MCs. Methods Synovial tissues were obtained from patients with RA or OA undergoing joint replacement surgery, and synovial MCs were enzymatically dispersed. Synovium-derived cultured MCs were generated by culturing synovial cells with stem cell factor. IL-17A expression was investigated using immunofluorescence in synovial tissues. IL-17A mRNA expression and its production from MCs were examined using RT-PCR and ELISA, respectively. Results The number of IL-17A-positive (+) synovial MCs and the percentage of IL-17A + MCs among all the IL-17A + cells from RA patients were not significantly increased compared with those from OA subjects. The synovium-derived cultured MCs spontaneously released small amounts of IL-17A. Neither IgE- nor IgG-dependent stimulation increased IL-17A production from the MCs. IL-33, tumor necrosis factor-α, C5a, lipopolysaccharide or IL-23 plus IL-1β did not affect IL-17A production in MCs. Conclusions The synovial MCs are not a main source of IL-17A in RA. [ABSTRACT FROM AUTHOR]

Published

2016

32. Gene Expression Profiling of Human Mast Cell Subtypes: An In Silico Study.

Author

Saito, Hirohisa, Matsumoto, Kenji, Okumura, Shigeru, Kashiwakura, Jun-ichi, Oboki, Keisuke, Yokoi, Hidenori, Kambe, Naotomo, Ohta, Ken, and Okayama, Yoshimichi

Subjects

*GENE expression, *MAST cells, *GRANULOCYTES, *GENETIC transcription, *CELL populations, *BASOPHILS

Abstract

Background: Human mast cells (MCs) were classified into at least two subtypes, i.e., tryptase- and chymase-positive MCs (MCTC) and tryptase-only-positive MCs (MCT). However, differences in global molecular expression between these subtypes are unknown. Methods: We analyzed public microarray data of MC subtypes derived from various tissues and those of peripheral blood granulocytes by using hierarchical clustering methods to understand the global gene expression profiles. Results: All the transcripts subjected to this clustering analysis were classified into two large clusters, i.e., MC-preferential or granulocyte-preferential. In the original works, MCs from tonsil, lung and skin had been cultured for more than several weeks to obtain highly viable and pure cell populations, and these MCs retained their typical profiles such as intensities of chymase protein expression. Most of the transcripts were commonly expressed by these MC subtypes. However, tonsil-derived MCs and skin-derived MCs but not lung-derived MCs expressed high levels of chymase (CMA1) as expected for the properties of MCTC and MCT. These CMA1-high MCs and CMA1-low MCs respectively expressed distinct sets of transcripts as small gene clusters as well as CMA-1 even after being cultured in the absence of a tissue environment. Conclusions: The MC lineage seems to be far from the granulocyte lineages including basophils. CMA1-high MCs (MCTC) and CMA1-low MCs (MCT) can be regarded as differentiated MC subtypes. As such, importance of data analysis studies will be increasing along with the accumulation of global molecular data in the public database. [ABSTRACT FROM AUTHOR]

Published

2006

33. Human mast cell activation through Fc receptors and Toll-like receptors.

Author

Okayama, Yoshimichi, Okumura, Shigeru, Tomita, Hisashi, Katayama, Hiroko, Yuki, Keisuke, Kagaya, Shinji, Kashiwakura, Jun-ichi, and Saito, Hirohisa

Subjects

*IMMUNITY, *BASOPHILS, *GLYCOPROTEINS, *GENETIC regulation, *IMMUNOLOGIC diseases, *IMMUNE system

Abstract

Mast cells express high-affinity IgE receptors (FcℇRI) on their surface and can be activated to secrete a variety of biologically active mediators by cross-linking of receptor-bound IgE. Recent studies in animal models indicate that mouse mast cells may play a protective role in host defense against bacteria through the production of tumor necrosis factor-α, mainly as a result of Toll-like receptor (TLR) 4- or CD48-mediated activation. Moreover, several recent observations in animal models have indicated that mast cells may also play a pivotal role in coordinating the early phases of autoimmune diseases, particularly those involving auto-antibodies. We recently identified functional TLR4 and FcγRI on human mast cells, in which their expression had been upregulated by interferon-γ. We compared each of the receptor-mediated gene expression profiles with the FcℇRI-mediated gene expression profile using high-density oligonucleotide probe arrays and discovered that human mast cells may modulate the immune system in a receptor-specific manner. [ABSTRACT FROM AUTHOR]

Published

2004

34. The mechanism of Tyk2 deficiency-induced immunosuppression in mice involves robust IL-10 production in macrophages.

Author

Hirashima, Koki, Muromoto, Ryuta, Minoguchi, Hiroya, Matsumoto, Tomohiro, Kitai, Yuichi, Kashiwakura, Jun-ichi, Shimoda, Kazuya, Oritani, Kenji, and Matsuda, Tadashi

Subjects

*INTERFERON gamma, *PROTEIN kinase inhibitors, *CUTIBACTERIUM acnes, *MICE, *PROTEIN-tyrosine kinases, *TYPE I interferons

Abstract

• Heat-killed P. acnes -induced peritonitis was reduced in Tyk2 KO mice independently of IFNs. • Tyk2 KO macrophages produced a greater amount of IL-10 than WT macrophages. • The enhanced IL-10 production was correlated to an enhanced activation of PGE 2 -PKA signaling. • These data provide an additional explanation for the immunosuppression seen in Tyk2 KO mice. Macrophages are highly plastic in their pro-inflammatory/anti-inflammatory roles. Type I and II interferons (IFNs) are known to modulate macrophage activation. Tyrosine kinase 2 (Tyk2) has an intimate relationship with type I and II IFN signaling. Animal studies have shown that Tyk2 knock-out (KO) in mice is associated with reduced inflammatory responses in various mouse models of diseases. To investigate the role of Tyk2 in inflammation in more detail, we intraperitoneally injected heat-killed Propionibacterium acnes (P. acnes) to Tyk2 KO mice. P. acnes –induced acute peritoneal inflammation, assessed by neutrophil infiltration, was reduced in Tyk2 KO mice. The reduction was accompanied with diminished productions of inflammatory cytokines and an enhanced production of anti-inflammatory IL-10. Unexpectedly, pre-treatment of wild-type mice with the neutralizing antibodies for IFNs did not affect P. acnes -induced neutrophil infiltration. A neutralizing antibody for the IL-10 receptor in Tyk2 KO mice restored P. acnes -induced peritoneal inflammation. Enhanced production of IL-10 from Tyk2 KO peritoneal cells was suppressed by either the cyclooxygenase inhibitor diclofenac or protein kinase A inhibitor H-89. The level of prostaglandin E 2 (PGE 2) in the steady-state peritoneal cavity in Tyk2 KO mice was higher than that in wild-type mice. Tyk2 KO macrophages showed an enhanced CREB phosphorylation induced by P. acnes plus PGE 2. Taken together, these results showed that Tyk2 deficiency potentiates the PGE 2 -protein kinase A-IL-10 pathway in macrophages, and thereby contributes to potentiation of the immunosuppressive phenotype. [ABSTRACT FROM AUTHOR]

Published

2020

35. Characterization of human decidual mast cells and establishment of a culture system.

Author

Matsuno, Takayuki, Toyoshima, Shota, Sakamoto-Sasaki, Tomomi, Kashiwakura, Jun-ichi, Matsuda, Akira, Watanabe, Yasuo, Azuma, Hiromitsu, Kawana, Kei, Yamamoto, Tatsuo, and Okayama, Yoshimichi

Subjects

*MAST cells, *PLACENTA, *STEM cell factor, *HISTAMINE, *TRYPTASE

Abstract

Abstract Background Although rodent decidual mast cells (MCs) reportedly play an important role in implantation and placenta formation, the characterization of human decidual MCs has been not well clarified. The aims of this study were to investigate the distribution and characteristics of MCs in human decidua and to establish a culture system for decidua-derived MCs. Methods Decidual tissues were obtained from patients who underwent a legal elective abortion (6th week to 9th week of pregnancy), and decidual MCs were enzymatically dispersed. Cultured decidua-derived MCs were generated by culturing decidual cells with stem cell factor. An ultrastructural analysis of primary decidual MCs and cultured decidua-derived MCs was performed using a transmission electron microscope. Receptor and protease expression was analyzed using FACS. Histamine released from MCs was measured using enzyme immune assays. Results A larger proportion of tryptase positive(+) MCs in decidua was present on the maternal side. Both enzymatically dispersed decidual MCs and cultured decidua-derived MCs showed an FcεRIα+Kit+tryptase+chymase+ phenotype. Their granules contenting particles exhibited variable amounts of electron-lucent space separating electron-dense particles. Both enzymatically dispersed decidual MCs and cultured decidua-derived MCs released comparable amounts of histamine following FcεRI aggregation. Conclusions The isolation method for MCs from decidua during early pregnancy and the culture system for decidua-derived MCs may enable the roles of decidual MC during pregnancy to be explored. [ABSTRACT FROM AUTHOR]

Published

2018

36. Characterization of human decidual mast cells and establishment of culture system.

Author

Matsuno, Takayuki, Okayama, Yoshimichi, Yamazaki, Motomi, Kashiwakura, Jun-ichi, Sakamoto, Tomomi, Toyoshima, Shota, Azuma, Hiromitsu, Murase, Takayuki, Chishima, Fumihisa, and Yamamoto, Tatsuo

Subjects

*MAST cells, *CELL culture, *INTERLEUKIN-6, *IMMUNOHISTOCHEMISTRY, *HISTAMINE

Published

2016