研究者業績

須藤 明

Akira Suto

基本情報

所属
千葉大学 国際高等研究基幹 / 大学院医学研究院 アレルギー・臨床免疫学 准教授
学位
医学博士(2003年3月 千葉大学)

J-GLOBAL ID
201901000960979899
researchmap会員ID
B000348879

論文

 107
  • Hiroki Furuya, Yosuke Toda, Arifumi Iwata, Mizuki Kanai, Kodai Kato, Takashi Kumagai, Takahiro Kageyama, Shigeru Tanaka, Lisa Fujimura, Akemi Sakamoto, Masahiko Hatano, Akira Suto, Kotaro Suzuki, Hiroshi Nakajima
    Nature communications 15(1) 5610-5610 2024年7月5日  
    Group 2 innate lymphoid cells (ILC2s) are a subset of innate lymphocytes that produce type 2 cytokines, including IL-4, IL-5, and IL-13. GATA3 is a critical transcription factor for ILC2 development at multiple stages. However, when and how GATA3 is induced to the levels required for ILC2 development remains unclear. Herein, we identify ILC2-specific GATA3-related tandem super-enhancers (G3SE) that induce high GATA3 in ILC2-committed precursors. G3SE-deficient mice exhibit ILC2 deficiency in the bone marrow, lung, liver, and small intestine with minimal impact on other ILC lineages or Th2 cells. Single-cell RNA-sequencing and subsequent flow cytometry analysis show that GATA3 induction mechanism, which is required for entering the ILC2 stage, is lost in IL-17RB+PD-1- late ILC2-committed precursor stage in G3SE-deficient mice. Cnot6l, part of the CCR4-NOT deadenylase complex, is a possible GATA3 target during ILC2 development. Our findings implicate a stage-specific regulatory mechanism for GATA3 expression during ILC2 development.
  • Takashi Kumagai, Arifumi Iwata, Hiroki Furuya, Kodai Kato, Atsushi Okabe, Yosuke Toda, Mizuki Kanai, Lisa Fujimura, Akemi Sakamoto, Takahiro Kageyama, Shigeru Tanaka, Akira Suto, Masahiko Hatano, Atsushi Kaneda, Hiroshi Nakajima
    Proceedings of the National Academy of Sciences of the United States of America 121(27) e2320727121 2024年7月2日  
    Asthma is a widespread airway disorder where GATA3-dependent Type-2 helper T (Th2) cells and group 2 innate lymphoid cells (ILC2s) play vital roles. Asthma-associated single nucleotide polymorphisms (SNPs) are enriched in a region located 926-970 kb downstream from GATA3 in the 10p14 (hG900). However, it is unknown how hG900 affects the pathogenesis of allergic airway inflammation. To investigate the roles of the asthma-associated GATA3 enhancer region in experimental allergic airway inflammation, we first examined the correlation between GATA3 expression and the activation of the hG900 region was analyzed by flow cytometry and ChIP-qPCR. We found that The activation of enhancers in the hG900 region was strongly correlated to the levels of GATA3 in human peripheral T cell subsets. We next generated mice lacking the mG900 region (mG900KO mice) were generated by the CRISPR-Cas9 system, and the development and function of helper T cells and ILCs in mG900KO mice were analyzed in steady-state conditions and allergic airway inflammation induced by papain or house dust mite (HDM). The deletion of the mG900 did not affect the development of lymphocytes in steady-state conditions or allergic airway inflammation induced by papain. However, mG900KO mice exhibited reduced allergic inflammation and Th2 differentiation in the HDM-induced allergic airway inflammation. The analysis of the chromatin conformation around Gata3 by circular chromosome conformation capture coupled to high-throughput sequencing (4C-seq) revealed that the mG900 region interacted with the transcription start site of Gata3 with an influencing chromatin conformation in Th2 cells. These findings indicate that the mG900 region plays a pivotal role in Th2 differentiation and thus enhances allergic airway inflammation.
  • Shunjiro Kurihara, Kotaro Suzuki, Masaya Yokota, Takashi Ito, Yuki Hayashi, Ryo Kikuchi, Takahiro Kageyama, Kazuyuki Meguro, Shigeru Tanaka, Arifumi Iwata, Yoshiyuki Goto, Akira Suto, Hiroshi Nakajima
    Biomolecules 14(1) 89-89 2024年1月10日  査読有り
  • 林 佑紀, 岩田 有史, 前澤 裕子, 岩本 太郎, 古田 俊介, 須藤 明, 鈴木 浩太郎, 中島 裕史
    アレルギー 72(8) 1066-1066 2023年9月  
  • Junichi Ishikawa, Akira Suto, Kazuya Abe, Yuki Hayashi, Kensuke Suga, Shigeru Tanaka, Takahiro Kageyama, Arifumi Iwata, Kazumasa Suzuki, Kotaro Suzuki, Hiroshi Nakajima
    Frontiers in Immunology 14 2023年8月18日  
    Murine IL-17-producing γδT (γδT17) cells are divided into two subsets: natural γδT17 (nγδT17) cells, whose development is restricted to the fetal thymus, and inducible γδT17 cells, which require antigen exposure for their IL-17 production and are presumed to develop from Rorc+Il17a-CCR9+ immature γδT17 cells in the adult thymus and whose T cell receptor (TCR) is biased toward Vγ4. Although IL-23 is known to be involved in developing γδT17 cells, the roles of other cytokines, such as IL-21, which is involved in developing Th17 cells like IL-23, in the development, maintenance, and pathophysiology of γδT17 cells remain unknown. Here, we show that IL-21 is dispensable for the fetal thymic development of nγδT17 cells but is required for the peripheral maintenance of Vγ4+nγδT17 cells. Upon stimulation with γδTCR, IL-1 plus IL-21 induces the proliferation of Vγ4+nγδT17 cells via STAT3 as effectively as IL-1 plus IL-23. Using bone marrow chimeric mice, we demonstrated that immature γδT17 cells are produced de novo in the adult mice from donor adult bone marrow cells and that IL-21 is dispensable for their development. Instead, IL-21 is required to expand newly induced Vγ4+γδT17 cells in the periphery upon immunization. Finally, using adoptive transfer experiments of γδT17 cells, we found that IL-21 receptors on γδT17 cells are involved in maintaining Vγ4+γδT17 cells, subsequent infiltration of Th17 cells into the spinal cord, and exacerbation of experimental autoimmune encephalomyelitis. Collectively, IL-21 plays a vital role in the maintenance and pathogenesis of Vγ4+γδT17 cells.
  • Shigeru Tanaka, Keishi Etori, Koto Hattori, Jun Tamura, Kei Ikeda, Takahiro Kageyama, Kazuyuki Meguro, Taro Iwamoto, Arifumi Iwata, Shunsuke Furuta, Akira Suto, Kotaro Suzuki, Hiroshi Nakajima
    Modern rheumatology 2023年7月31日  
    OBJECTIVE: Predicting the efficacy of biological disease-modifying anti-rhematic drugs (bDMARDs) is challenging. In this study, we aimed to explore markers that predict the efficacy of abatacept in rheumatoid arthritis (RA) patients. METHODS: Thirty RA patients receiving abatacept were recruited, and peripheral blood mononuclear cells (PBMCs) from the participants were subjected to DNA microarray analysis. The expression of CCR4, which was selected by the result of DNA microarray, was determined by flow cytometry in 16 newly diagnosed treatment-naïve RA patients. CCR4 expression on each helper T cell subset was also measured. RESULTS: CCR4 was upregulated in the abatacept responder. The expression levels of CCR4 were significantly correlated with the improvement of clinical disease activity index (CDAI). CCR4 expression was predominantly observed in CD4+ T cells in PBMCs. The percentage of CCR4-expressing CD4+ T cells was significantly higher in RA patients than in healthy individuals. Interestingly, Th17 and Treg cells expressed high levels of CCR4 compared to non-Th17-related helper T cells. CONCLUSION: CCR4 is a Th17- and Treg-related gene, and the high CCR4 expression in peripheral blood samples may predict the efficacy of abatacept in RA.
  • Kazuma Iida, Kensuke Suga, Kotaro Suzuki, Shunjiro Kurihara, Yoko Yabe, Takahiro Kageyama, Kazuyuki Meguro, Shigeru Tanaka, Arifumi Iwata, Akira Suto, Hiroshi Nakajima
    Biochemical and Biophysical Research Communications 664 9-19 2023年7月  
  • Kensuke Suga, Akira Suto, Shigeru Tanaka, Yutaka Sugawara, Takahiro Kageyama, Junichi Ishikawa, Yoshie Sanayama, Kei Ikeda, Shunsuke Furuta, Shin-Ichiro Kagami, Arifumi Iwata, Koichi Hirose, Kotaro Suzuki, Osamu Ohara, Hiroshi Nakajima
    JCI Insight 8(10) 2023年5月22日  
  • Tadamichi Kasuya, Shigeru Tanaka, Jun Tamura, Keishi Etori, Jumpei Shoda, Koto Hattori, Yusuke Endo, Masayuki Kitajima, Takahiro Kageyama, Taro Iwamoto, Masaya Yokota, Arifumi Iwata, Akira Suto, Kotaro Suzuki, Harumi Suzuki, Steven F. Ziegler, Hiroshi Nakajima
    Scientific Reports 13(1) 2023年1月30日  
    Abstract Epithelial cells control a variety of immune cells by secreting cytokines to maintain tissue homeostasis on mucosal surfaces. Regulatory T (Treg) cells are essential for immune homeostasis and for preventing tissue inflammation; however, the precise molecular mechanisms by which epithelial cell-derived cytokines function on Treg cells in the epithelial tissues are not well understood. Here, we show that peripheral Treg cells preferentially respond to thymic stromal lymphoprotein (TSLP). Although TSLP does not affect thymic Treg differentiation, TSLP receptor-deficient induced Treg cells derived from naïve CD4+ T cells are less activated in an adoptive transfer model of colitis. Mechanistically, TSLP activates induced Treg cells partially through mTORC1 activation and fatty acid uptake. Thus, TSLP modulates the activation status of induced Treg through the enhanced uptake of fatty acids to maintain homeostasis in the large intestine.
  • Jumpei Shoda, Shigeru Tanaka, Keishi Etori, Koto Hattori, Tadamichi Kasuya, Kei Ikeda, Yuko Maezawa, Akira Suto, Kotaro Suzuki, Junichi Nakamura, Yoshiro Maezawa, Minoru Takemoto, Christer Betsholtz, Koutaro Yokote, Seiji Ohtori, Hiroshi Nakajima
    Arthritis Research & Therapy 24(1) 2022年12月  
    Abstract Objectives Methotrexate (MTX) is an anchor drug for the treatment of rheumatoid arthritis (RA). However, the precise mechanisms by which MTX stalls RA progression and alleviates the ensuing disease effects remain unknown. The aim of the present study was to identify novel therapeutic target molecules, the expression patterns of which are affected by MTX in patients with RA. Methods CD4+ T cells from 28 treatment-naïve patients with RA before and 3 months after the initiation of MTX treatment were subjected to DNA microarray analyses. The expression levels of semaphorin 3G, a differentially expressed gene, and its receptor, neuropilin-2, were evaluated in the RA synovium and collagen-induced arthritis synovium. Collagen-induced arthritis and collagen antibody-induced arthritis were induced in semaphorin3G-deficient mice and control mice, and the clinical score, histological score, and serum cytokines were assessed. The migration and proliferation of semaphorin 3G-stimulated bone marrow-derived macrophages were analyzed in vitro. The effect of local semaphorin 3G administration on the clinical score and number of infiltrating macrophages during collagen antibody-induced arthritis was evaluated. Results Semaphorin 3G expression in CD4+ T cells was downregulated by MTX treatment in RA patients. It was determined that semaphorin 3G is expressed in RA but not in the osteoarthritis synovium; its receptor neuropilin-2 is primarily expressed on activated macrophages. Semaphorin3G deficiency ameliorated collagen-induced arthritis and collagen antibody-induced arthritis. Semaphorin 3G stimulation enhanced the migration and proliferation of bone marrow-derived macrophages. Local administration of semaphorin 3G deteriorated collagen antibody-induced arthritis and increased the number of infiltrating macrophages. Conclusions Upregulation of semaphorin 3G in the RA synovium is a novel mechanism that exacerbates joint inflammation, leading to further deterioration, through macrophage accumulation.
  • 戸田 陽介, 古矢 裕樹, 金井 瑞希, 影山 貴弘, 田中 繁, 須藤 明, 鈴木 浩太郎, 中島 裕史
    日本臨床免疫学会総会プログラム・抄録集 50回 69-69 2022年10月  
  • Yusuke Yokoyama, Tomohiro Tamachi, Arifumi Iwata, Yuko Maezawa, Kazuyuki Meguro, Masaya Yokota, Hiroaki Takatori, Akira Suto, Kotaro Suzuki, Koichi Hirose, Noritaka Yamaguchi, Hiroaki Honda, Hiroshi Nakajima
    Biochemical and Biophysical Research Communications 2022年9月  
  • 戸田 陽介, 古矢 裕樹, 岩田 有史, 金井 瑞希, 影山 貴弘, 田中 繁, 須藤 明, 中島 裕史
    アレルギー 71(6-7) 795-795 2022年8月  
  • 前澤 裕子, 林 佑紀, 岩田 有史, 井田 友明, 高山 明日香, 影山 貴弘, 田中 繁, 岩本 太郎, 横田 雅也, 池田 啓, 須藤 明, 中島 裕史
    アレルギー 71(6-7) 877-877 2022年8月  
  • 田村 潤, 高山 明日香, 井田 友明, 岩本 太郎, 古田 俊介, 池田 啓, 前澤 裕子, 須藤 明, 鈴木 浩太郎, 中島 裕史
    アレルギー 71(6-7) 878-878 2022年8月  
  • 田村 潤, 高山 明日香, 井田 友明, 岩本 太郎, 古田 俊介, 池田 啓, 前澤 裕子, 須藤 明, 鈴木 浩太郎, 中島 裕史
    アレルギー 71(6-7) 878-878 2022年8月  
  • Kazumasa Suzuki, Kotaro Suzuki, Yoko Yabe, Kazuma Iida, Junichi Ishikawa, Sohei Makita, Takahiro Kageyama, Taro Iwamoto, Shigeru Tanaka, Masaya Yokota, Arifumi Iwata, Akira Suto, Hiroshi Nakajima
    The Journal of investigative dermatology 2021年11月11日  
    Recent studies have identified NF-κB1 as a new disease susceptibility gene for psoriasis. Although accumulating evidence has shown the importance of NF-κB signaling in various cell types in the pathogenesis of psoriasis, it remains unclear how NF-κB1 contributes to the pathogenesis of psoriasis. In this study, we examined psoriasis-like skin diseases induced by topical administration of imiquimod in Nf-κb1‒deficient (Nf-κb1-/-) mice and littermate wild-type (WT) mice. Compared with WT mice, Nf-κb1-/- mice exhibited attenuated skin inflammation. The numbers of Vγ4+Vδ4+γδT17 cells, which cause skin inflammation in this model, were significantly reduced in the skin and draining lymph nodes in imiquimod-treated Nf-κb1-/- mice. Nf-κb1 is preferentially phosphorylated in Vγ4+Vδ4+γδT17 cells in WT mice. In vitro proliferation of Vγ4+Vδ4+γδT17 cells but not conventional CD4+ T cells was significantly impaired in Nf-κb1-/- mice compared with that in WT mice. RNA-sequencing analyses revealed that the expression of E2 factor target genes was decreased in Vγ4+Vδ4+γδT cells by the absence of NF-κB1. Consistently, the cell cycle progression of Vγ4+Vδ4+γδT cells was reduced in Nf-κb1-/- mice compared with that in WT mice. These results suggest that Nf-κb1 plays a crucial role in the pathogenesis of imiquimod-induced psoriasis-like skin inflammation by promoting the proliferation of Vγ4+Vδ4+γδT17 cells.
  • 須賀 謙介, 須藤 明, 影山 貴弘, 田中 繁, 岩本 太郎, 岩田 有史, 池田 啓, 鈴木 浩太郎, 中島 裕史
    日本臨床免疫学会総会プログラム・抄録集 49回 71-71 2021年10月  
  • Akihiko Kubota, Akira Suto, Kensuke Suga, Arifumi Iwata, Shigeru Tanaka, Kotaro Suzuki, Yoshio Kobayashi, Hiroshi Nakajima
    Journal of Molecular and Cellular Cardiology 159 48-61 2021年10月  
  • Manami Kato, Kei Ikeda, Takahiro Sugiyama, Shigeru Tanaka, Kazuma Iida, Kensuke Suga, Nozomi Nishimura, Norihiro Mimura, Tadamichi Kasuya, Takashi Kumagai, Hiroki Furuya, Taro Iwamoto, Arifumi Iwata, Shunsuke Furuta, Akira Suto, Kotaro Suzuki, Eiryo Kawakami, Hiroshi Nakajima
    PLOS ONE 16(5) e0252116-e0252116 2021年5月21日  
    <sec id="sec001"> <title>Objectives</title> We aimed to explore the associations of musculoskeletal inflammation patterns with peripheral blood innate lymphoid cell (ILC) populations, serum cytokines/chemokines, and treatment response to methotrexate in patients with rheumatoid arthritis (RA) and spondyloarthritis (SpA). </sec> <sec id="sec002"> <title>Methods</title> We enrolled 100 patients with either RA or SpA and performed ultrasound to evaluate power Doppler signals for synovitis (52 joint regions), tenosynovitis (20 tendons), and enthesitis (44 sites). We performed clustering analysis using unsupervised random forest based on the multi-axis ultrasound information and classified the patients into groups. We identified and counted ILC1-3 populations in the peripheral blood by flow cytometry and also measured the serum levels of 20 cytokines/chemokines. We also determined ACR20 response at 3 months in 38 patients who began treatment with methotrexate after study assessment. </sec> <sec id="sec003"> <title>Results</title> Synovitis was more prevalent and severe in RA than in SpA, whereas tenosynovitis and enthesitis were comparable between RA and SpA. Patients were classified into two groups which represented synovitis-dominant and synovitis-nondominant inflammation patterns. While peripheral ILC counts were not significantly different between RA and SpA, they were significantly higher in the synovitis-nondominant group than in the synovitis-dominant group (ILC1-3: p = 0.0007, p = 0.0061, and p = 0.0002, respectively). On the other hand, clustering of patients based on serum cytokines/chemokines did not clearly correspond either to clinical diagnoses or to synovitis-dominant/nondominant patterns. The synovitis-dominant pattern was the most significant factor that predicted clinical response to methotrexate (p = 0.0065). </sec> <sec id="sec004"> <title>Conclusions</title> Musculoskeletal inflammation patterns determined by ultrasound are associated with peripheral ILC counts and could predict treatment response to methotrexate. </sec>
  • Masashi Fukuta, Kotaro Suzuki, Shotaro Kojima, Yoko Yabe, Kazumasa Suzuki, Kazuma Iida, Hiroyuki Yamada, Shinichi Makino, Arifumi Iwata, Shigeru Tanaka, Taro Iwamoto, Akira Suto, Daiki Nakagomi, Hidefumi Wakashin, Yuko Maezawa, Yoshiro Maezawa, Minoru Takemoto, Katsuhiko Asanuma, Hiroshi Nakajima
    Lupus Science & Medicine 8(1) e000426-e000426 2021年5月  
    <sec><title>Objective</title>Recently, podocytes have been recognised not only as a physical barrier to prevent urinary protein loss but also as producers of proinflammatory cytokines. However, the roles of podocytes in the pathogenesis of lupus nephritis (LN) remain largely unknown. This study aims to determine the roles of suppressor of cytokine signalling (SOCS) family members expressed in glomeruli in the regulation of LN. </sec><sec><title>Methods</title>We investigated the expression of SOCS family members in glomeruli in murine lupus model induced by repeated epicutaneous administration of the TLR7/8 agonist imiquimod. We also investigated the roles of SOCS3 expressed in podocytes in the imiquimod-induced glomerulonephritis and systemic autoimmunity by using podocyte-specific SOCS3-deficient mice (podocin-Cre x SOCS3fl/fl mice (SOCS3-cKO mice)). Finally, we investigated the expression of proinflammatory cytokines and chemokines in SOCS3-deficient podocyte cell lines. </sec><sec><title>Results</title>qPCR analysis revealed that among SOCS family members, SOCS3 was preferentially induced in glomeruli on epicutaneous administration of imiquimod and that interleukin 6 (IL-6) induced SOCS3 expression in podocyte cell lines. SOCS3-cKO mice exhibited severe glomerulonephritis, high levels of serum creatinine and urine albumin and decreased survival rate compared with control SOCS3-WT mice. Levels of anti-double-strand DNA antibody, SOCS (GC) formation and the numbers of follicular helper T (Tfh) cells and GC B cells in the spleen were higher in SOCS3-cKO mice than those in SOCS3-WT mice. Serum IL-6 levels and expression of IL-6 mRNA in glomeruli were also elevated in SOCS3-cKO mice. IL-6-induced IL-6 expression was enhanced in SOCS3-deficient podocyte cell lines compared with that in SOCS3-sufficient podocyte cell lines. </sec><sec><title>Conclusion</title>SOCS3 expressed in podocytes plays protective roles for the development of glomerulonephritis and inhibits autoantibody production in the imiquimod-induced lupus model presumably by suppressing IL-6 production of podocytes. </sec>
  • Sohei Makita, Hiroaki Takatori, Ayako Matsuki, Hirotoshi Kawashima, Arifumi Iwata, Shigeru Tanaka, Daiki Nakagomi, Yoshihiro Oya, Ryutaro Matsumura, Tomohiro Tamachi, Akira Suto, Kotaro Suzuki, Koichi Hirose, Hiroshi Nakajima
    The Journal of investigative dermatology 2020年10月14日  
    T-bet and signal transducer and activator of transcription (STAT) 6 are critical factors for helper T-cell differentiation in humans and mice. Additionally, polymorphisms in TBX21 (T-bet) and STAT6 are associated with the susceptibility of allergic diseases. However, precise mechanisms of the reciprocal regulation between T-bet and STAT6 in allergy remain unclear. To determine the reciprocal regulation in vivo, we investigated the phenotype of T-bet/STAT6 double-deficient (T-bet-/- STAT6-/-) mice. Unexpectedly, T-bet-/- STAT6-/- mice but not T-bet-/- mice or STAT6-/- mice spontaneously developed severe dermatitis. Not only eosinophils and mast cells but also CD4+ T cells infiltrated into the skin of T-bet-/- STAT6-/- mice. Adoptive transfer of CD4+ T cells of T-bet-/- STAT6-/- mice into severe combined immunodeficient mice induced the accumulation of eosinophils and mast cells in the skin, whereas depletion of CD4+ T cells ameliorated the dermatitis in T-bet-/- STAT6-/- mice. Comprehensive transcriptome analyses revealed that IL-9 expression was enhanced in T-bet-/- STAT6-/- CD4+ T cells. Indeed, IL-9 neutralization ameliorated the dermatitis in T-bet-/- STAT6-/- mice. T-bet-/- STAT6-/- CD4+ T cells expressed functional thymic stromal lymphopoietin receptors and produced large amounts of IL-9 on thymic stromal lymphopoietin stimulation. These results indicate that T-bet and STAT6 coordinately suppress atopic dermatitis-like skin inflammation, possibly by inhibiting thymic stromal lymphopoietin-dependent IL-9 production in CD4+ T cells.
  • Sohei Makita, Hiroaki Takatori, Arifumi Iwata, Shigeru Tanaka, Shunsuke Furuta, Kei Ikeda, Akira Suto, Kotaro Suzuki, Silvia B. V. Ramos, Hiroshi Nakajima
    Frontiers in Immunology 11 2020年6月23日  
  • Aiko Saku, Shunsuke Furuta, Manami Kato, Hiroki Furuya, Kazumasa Suzuki, Masashi Fukuta, Kenichi Suehiro, Sohei Makita, Tomohiro Tamachi, Kei Ikeda, Hiroaki Takatori, Yuko Maezawa, Akira Suto, Kotaro Suzuki, Koichi Hirose, Hiroshi Nakajima
    Clinical rheumatology 39(4) 1091-1099 2020年4月  
    OBJECTIVE: Musculoskeletal ultrasound (US) is more sensitive than physical examination in detecting synovitis and helps physicians to understand its pathophysiology. In this study, we aimed to determine if the experience in musculoskeletal US scanning is independently associated with improved physical examination skills to detect synovitis. METHOD: Seventy patients with rheumatoid arthritis and twenty-three physicians were enrolled. Patients were first assessed by multiple physicians with a range of clinical/sonographic experience for the swelling of the wrist, metacarpophalangeal and proximal interphalangeal (PIP) joints and next underwent US assessment performed by another physician experienced in musculoskeletal US. We then calculated the positive/negative predictive values (PPV/NPV) of joint swelling to identify US-detected synovial hypertrophy. Finally, the factors independently associated with the accuracy of clinical assessment were identified by using multivariate analyses. RESULTS: One thousand five hundred forty joints were assessed 6116 times in total for swelling. Overall, PPV and NPV of joint swelling were 51.7% and 88.3%, respectively. Multivariate analyses identified wrist joint, tenderness, male and greater patients' age as the factors significantly associated with higher PPV. In addition, there was a trend that longer experience in rheumatology clinical practice was associated with higher PPV (p = 0.058). On the other hand, longer experience in musculoskeletal US, PIP joint and positive rheumatoid factor were identified as the significant factors for higher NPV, while wrist joint, tenderness, presence of osteophyte and obesity as those for lower NPV. CONCLUSION: Our data suggest that the experience in musculoskeletal US improves physical examination skills particularly to avoid overestimation.Key Points• Physicians with longer US experience are less likely to overestimate synovitis by physical examination.• Musculoskeletal US is a useful tool for rheumatologists to improve their physical examination skill.• Presence of osteophytes, joint tenderness and obesity influence the accuracy of physical examination of joints.
  • Ken-Ichi Suehiro, Akira Suto, Kensuke Suga, Hiroki Furuya, Arifumi Iwata, Taro Iwamoto, Shigeru Tanaka, Takahiro Kageyama, Kotaro Suzuki, Koichi Hirose, Véronique Lefebvre, Hiroshi Nakajima
    Cellular & Molecular Immunology 2020年3月9日  査読有り
  • Kono K, Hirose K, Makita S, Kageyama T, Tamachi T, Saku A, Suto A, Suzuki K, Nakajima H
    Clinical and experimental allergy : journal of the British Society for Allergy and Clinical Immunology 49(11) 1523-1526 2019年11月  査読有り
  • 中島 裕史, 田中 繁, 須藤 明
    日本臨床免疫学会総会プログラム・抄録集 47回 56-56 2019年10月  
  • Saku A, Hirose K, Ito T, Iwata A, Sato T, Kaji H, Tamachi T, Suto A, Goto Y, Domino SE, Narimatsu H, Kiyono H, Nakajima H
    The Journal of allergy and clinical immunology 144(3) 698-709.e9 2019年9月  査読有り
  • Saku A, Hirose K, Kageyama T, Kono K, Nakamura K, Yokota M, Maezawa Y, Suto A, Nakajima H
    Allergology international : official journal of the Japanese Society of Allergology 2019年6月  査読有り
  • Kubota A, Suto A, Suzuki K, Kobayashi Y, Nakajima H
    Journal of molecular and cellular cardiology 131 41-52 2019年6月  査読有り
  • Saku A, Hirose K, Kageyama T, Kono K, Nakamura K, Yokota M, Maezawa Y, Suto A, Nakajima H
    Allergology international : official journal of the Japanese Society of Allergology 69(1) 132-135 2019年6月  査読有り
  • 末廣 健一, 須藤 明, 田中 繁, 玉地 智宏, 鈴木 浩太郎, 中島 裕史
    アレルギー 68(4-5) 497-497 2019年5月  
  • 福田 匡志, 鈴木 浩太郎, 田中 繁, 鈴木 一正, 岩田 有史, 古田 俊介, 玉地 智宏, 池田 啓, 前澤 裕子, 須藤 明, 中島 裕史
    日本リウマチ学会総会・学術集会プログラム・抄録集 63回 647-647 2019年3月  
  • Kato M, Ikeda K, Kageyama T, Kasuya T, Kumagai T, Furuya H, Furuta S, Tamachi T, Suto A, Suzuki K, Nakajima H
    Journal of clinical rheumatology : practical reports on rheumatic & musculoskeletal diseases 27(8S) S574-S577 2019年1月  査読有り
  • Tanaka S, Suto A, Iwamoto T, Kageyama T, Tamachi T, Takatori H, Suzuki K, Hirose K, Ohara O, Lefebvre V, Nakajima H
    The Journal of experimental medicine 215(10) 2509-2519 2018年10月  査読有り
  • Makita S, Takatori H, Tamachi T, Suto A, Suzuki K, Nakajima H
    Allergology international : official journal of the Japanese Society of Allergology 67S S51-S53 2018年9月  査読有り
  • 久保田 暁彦, 須藤 明, 鈴木 浩太郎, 小林 欣夫, 中島 裕史
    日本結合組織学会学術大会プログラム・抄録集 50回 90-90 2018年6月  
  • 河野 健太, 廣瀬 晃一, 牧田 荘平, 影山 貴弘, 玉地 智宏, 須藤 明, 中島 裕史
    アレルギー 67(4-5) 573-573 2018年5月  
  • Yoshihisa Kobayashi, Arifumi Iwata, Kotaro Suzuki, Akira Suto, Saki Kawashima, Yukari Saito, Takayoshi Owada, Midori Kobayashi, Norihiko Watanabe, Hiroshi Nakajima
    Proceedings of the National Academy of Sciences of the United States of America 110(13) 5121-5126 2018年4月24日  査読有り
    Although innate immune responses are necessary for the initiation of acquired immune responses and the subsequent successful elimination of pathogens, excessive responses occasionally result in lethal endotoxic shock accompanied by a cytokine storm. B and T lymphocyte attenuator (BTLA), a coinhibitory receptor with similarities to cytotoxic T-lymphocyte antigen (CTLA)-4 and programmed death (PD)-1, is expressed in not only B and T cells but also dendritic cells (DCs) and macrophages (Mφs). Recently, several studies have reported that BTLA-deficient (BTLA-/-) mice show enhanced pathogen clearance compared withWTmice in early phase of infections. However, the roles of BTLA expressed on innate cells in overwhelming and uncontrolled immune responses remain unclear. Here, we found that BTLA-/- mice were highly susceptible to LPS-induced endotoxic shock. LPS-induced TNF-α and IL-12 production in DCs and Mφs was significantly enhanced in BTLA -/- mice. BTLA-/- DCs also produced high levels of TNF-α on stimulation with Pam3CSK4 but not poly(I:C) or CpG, suggesting that BTLA functions as an inhibitory molecule on Toll-like receptor signaling at cell surface but not endosome. Moreover, BTLA-/- DCs showed enhanced MyD88- and toll/IL-1R domain-containing adaptor inducing IFN (TRIF)-dependent signaling on LPS stimulation, which is associated with impaired accumulation of Src homology 2-containing protein tyrosine phosphatase in lipid rafts. Finally, we found that an agonistic anti-BTLA antibody rescued mice from LPS-induced endotoxic shock, even if the antibody was given to mice that had developed a sign of endotoxic shock. These results suggest that BTLA directly inhibits LPS responses in DCs and Mφs and that agonistic agents for BTLA might have therapeutic potential for LPS-induced endotoxic shock. © PNAS 2013.
  • Hosokawa J, Suzuki K, Meguro K, Tanaka S, Maezawa Y, Suto A, Fujimura L, Sakamoto A, Clevers H, Ohara O, Nakajima H
    The Journal of allergy and clinical immunology 140(1) 288-+ 2017年7月  査読有り
  • 横山 裕亮, 玉地 智宏, 岩田 有史, 前澤 裕子, 目黒 和行, 横田 雅也, 高取 宏昌, 須藤 明, 鈴木 浩太郎, 廣瀬 晃一, 中島 裕史, 本田 浩章
    アレルギー 66(4-5) 606-606 2017年5月  
  • Matsuki A, Takatori H, Makita S, Yokota M, Tamachi T, Suto A, Suzuki K, Hirose K, Nakajima H
    The Journal of allergy and clinical immunology 139(4) 1355-1367.e6 2017年4月  
  • Ayako Matsuki, Hiroaki Takatori, Sohei Makita, Masaya Yokota, Tomohiro Tamachi, Akira Suto, Kotaro Suzuki, Koichi Hirose, Hiroshi Nakajima
    JOURNAL OF ALLERGY AND CLINICAL IMMUNOLOGY 139(4) 1355-+ 2017年4月  査読有り
    Background: Innate lymphoid cells (ILCs) are emerging subsets of immune cells that produce large amounts of cytokines upon cytokine and/or alarmin stimulation. Recent studies have shown that T-bet plays pivotal roles in the development of ILC3s and type 1 ILCs; however, the roles of T-bet in lung type 2 innate lymphoid cells (ILC2s) remain unknown. Objective: We sought to determine the role of T-bet in ILC2-mediated airway inflammation. Methods: The expression of T-bet in lung ILCs (defined as Thy1.2(+) Lin(-) cells) was examined. The roles of T-bet in the development of lung ILC2s and airway inflammation induced by IL-33 administration were examined by using T-bet-deficient (T-bet(-/-)) mice. Gene expression profiles of T-bet(-/-) lung ILCs were analyzed by RNA sequencing. Results: T-bet was expressed in lung ILC2s (defined as Thy1.2(+) Lin(-) cells expressing ST2 or CD25) and IFN-gamma enhanced its expression. Although the development of lung ILC2s at steady-state conditions was normal in T-bet(-/-) mice, IL-33-induced accumulation of lung ILC2s and eosinophilic airway inflammation were exacerbated in T-bet(-/-) mice. The exacerbated accumulation of ILC2s and eosinophilic airway inflammation by the absence of T-bet were evident even in a RAG2(-/-) background, suggesting that T-bet expressed in non-T/non-B population is involved in the suppression of IL-33-induced eosinophilic airway inflammation. Transcriptome analysis revealed that IL-9 expression in IL-33-stimulated lung ILCs was upregulated in T-bet(-/-) mice compared with that in wild-type mice. Importantly, neutralization of IL-9 markedly attenuated IL-33-induced accumulation of lung ILC2s and eosinophilic inflammation in T-bet(-/-) mice. Conclusions: T-bet suppresses IL-9 production from lung ILC2s and thereby inhibits IL-33-induced eosinophilic airway inflammation.
  • Yokota M, Tamachi T, Yokoyama Y, Maezawa Y, Takatori H, Suto A, Suzuki K, Hirose K, Takeda K, Nakajima H
    Allergy 72(7) 1043-1053 2017年  査読有り
  • Kageyama Takahiro, Suto Akira, Iwamoto Taro, Tanaka Shigeru, Suehiro Kenichi, Yokoyama Yusuke, Saku Aiko, Furuta Shunsuke, Ikeda Kei, Suzuki Kotaro
    ImmunoHorizons 1(8) 176 2017年  査読有り
  • 玉地 智宏, 横田 雅也, 横山 裕亮, 前澤 裕子, 須藤 明, 鈴木 浩太郎, 廣瀬 晃一, 中島 裕史
    アレルギー 65(4-5) 601-601 2016年5月  
  • Meguro K, Nakagomi D, Suzuki K, Hosokawa J, Fukuta T, Yokota M, Maezawa Y, Suto A, Nakajima H
    The Journal of investigative dermatology 136(3) 649-657 2016年3月  
  • Kazuyuki Meguro, Daiki Nakagomi, Kotaro Suzuki, Junichi Hosokawa, Tadashi Fukuta, Masaya Yokota, Yuko Maezawa, Akira Suto, Hiroshi Nakajima
    JOURNAL OF INVESTIGATIVE DERMATOLOGY 136(3) 649-657 2016年3月  査読有り
    Numerous studies have clarified the immunological mechanisms of contact hypersensitivity (CHS). In addition, we have recently shown that M2 macrophages play key roles in the development of CHS by producing matrix metalloproteinase-12 (MMP-12). However, regulatory mechanisms of the elicitation phase in CHS remain largely unknown. To determine the roles of suppressor of cytokine signaling (SOCS) family members in M2 macrophages in the regulation of CHS, we investigated the expression of SOCS family members in M2 macrophages at the inflammatory sites of CHS. Transcriptome analysis revealed that among SOCS family members, SOCS3 was highly expressed in M2 macrophages at the site of CHS, and SOCS3 induction was reduced by IFN-g neutralization. 2,4-Dinitrofluorobenzeneeinduced CHS was significantly enhanced and prolonged in mice lacking SOCS3 expression in monocytes/macrophages (SOCS3D/D mice) compared with that in control mice. Importantly, expression of MMP-12 in M2 macrophages was significantly increased in SOCS3D/D mice at the site of CHS, and deletion of the MMP-12 gene reduced the exacerbated CHS in SOCS3D/D mice. Finally, IFN-g inhibited IL-4-induced MMP-12 expression in a SOCS3-dependent manner. Taken together, these results suggest that SOCS3 expressed in M2 macrophages is involved in the attenuation and/or resolution of CHS, presumably by suppressing MMP-12 production.
  • Kazuyuki Meguro, Kotaro Suzuki, Junichi Hosokawa, Yoshie Sanayama, Shigeru Tanaka, Shunsuke Furuta, Kei Ikeda, Hiroaki Takatori, Akira Suto, Akemi Sakamoto, Osamu Ohara, Hiroshi Nakajima
    ARTHRITIS & RHEUMATOLOGY 67(10) 2651-2660 2015年10月  査読有り
    Objective. We have previously shown that expression of the Bcl-3 gene, a member of the IkB family, is down-regulated in CD4+ T cells from patients with rheumatoid arthritis (RA) following tocilizumab therapy. The objective of this study was to examine the role of Bcl-3 in the pathogenesis of RA. Methods. DNA microarray analysis was used to compare the signal intensity of Bcl-3 in CD41+ T cells from untreated RA patients and healthy controls. We examined the roles of interleukin-6 (IL-6)/ STAT-3 signaling in the induction of Bcl-3. In addition, we analyzed the gene expression profiles of Bcl-3-transduced CD4+ T cells by RNA sequencing. The effects of enforced expression as well as gene silencing of Bcl-3 on the development of follicular helper T (Tfh) cells were evaluated. Finally, we examined correlations between the signal intensities of Bcl-3 and Tfh cell-related genes in CD4+ T cells from untreated RA patients. Results. Bcl-3 levels were significantly higher in RA patients than in healthy controls. IL-6 induced Bcl-3 expression in CD41 T cells in a STAT-3-dependent manner. Transcriptome analysis revealed that the expression of Bcl-6, a master regulator of Tfh cell differentiation, was significantly up-regulated by the enforced Bcl-3 expression. The enforced Bcl-3 expression increased, but Bcl-3 silencing decreased, the numbers of IL-21-producing Tfh-like cells. Bcl-3 levels in CD4+ T cells from RA patients correlated positively with the levels of Tfh cell-related genes CXCR5, inducible costimulator, and achaete-scute homolog 2. Conclusion. Bcl-3 is involved in the development of Tfh cells and the pathogenesis of RA, presumably by inducing IL-21 production.
  • Akira Suto, Shigeru Tanaka, Hiroshi Nakajima
    ONCOTARGET 6(24) 19952-19953 2015年8月  査読有り

MISC

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共同研究・競争的資金等の研究課題

 22