Affiliation
Institute of Advanced Medical Sciences, Department of Cell Biology, Associate Professor
Title
Associate Professor
External link
Hashiguchi Masaaki
Degree
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Ph.D ( 2000.3 The University of Tokyo )
Research Interests
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IgE
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IgA
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innate lymphoid cells
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mucosal immunity
Research Areas
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Life Science / Immunology
Education
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The University of Tokyo
2000.3
Research History
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Nippon Medical School Institute for Advanced Medical Sciences Associate Professor
2021.4
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Dokkyo Medical University Associate Professor
2020.4 - 2021.3
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Dokkyo Medical University School of Medicine Associate Professor
2012.4 - 2020.3
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Dokkyo Medical University School of Medicine Assistant Professor
2010.4 - 2012.3
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Tokyo Medical and Dental University Graduate School of Medical and Dental Sciences Assistant Professor
2003.9 - 2010.3
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Medical Collage of Georgia, Institute of Molecular Medicine and Genetics, Postdoctral fellow
2000.6 - 2003.8
Papers
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Inhibition of IL-33 signaling ameliorate hepatic fibrosis with decreasing MCP-1 in a mouse model of diabetes and non-alcoholic steatohepatitis; comparison for luseogliflozin, an SGLT2 inhibitor Reviewed
Sho Wakamatsu, Teruo Jojima, Masaaki Hashiguchi, Haruka Kishi, Takafumi Niitani, Shintaro Sakurai, Toshie Iijima, Takahiko Kogai, Takuya Tomaru, Isao Usui, Yoshimasa Aso
Journal of Diabetes and its Complications 38 ( 1 ) 108650 - 108650 2024.1
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Hidefumi Kojima, Yuji Kashiwakura, Yumiko Kanno, Masaaki Hashiguchi, Tetsuji Kobata
Scandinavian Journal of Immunology 93 ( 6 ) e13020 2021.1
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IL-21 and IL-5 coordinately induce surface IgA+ cells Reviewed
Masaaki Hashiguchi, Yuji Kashiwakura, Yumiko Kanno, Hidefumi Kojima, Tetsuji Kobata
Immunology Letters 224 21 - 27 2020.8
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Yuji Kashiwakura, Hidefumi Kojima, Yumiko Kanno, Masaaki Hashiguchi, Tetsuji Kobata
Clinical & Experimental Immunology 2020.6
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Peyer’s patches contain abundant isotype-switched B cells with activated phenotypes and are inductive sites for T-independent anti-DNA IgA. Reviewed
Hashiguchi M, Kashiwakura Y, Kojima H, Kanno Y, Kobata T
Immunology Letters 211 53 - 59 2019
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Tumor necrosis factor superfamily member (TNFSF) 13 (APRIL) and TNFSF13B (BAFF) downregulate homeostatic immunoglobulin production in the intestines Reviewed
Masaaki Hashiguchi, Yuji Kashiwakura, Yumiko Kanno, Hidefumi Kojima, Tetsuji Kobata
Cellular Immunology 323 41 - 48 2018.1
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Masahiko Itoh, Derek C. Radisky, Masaaki Hashiguchi, Hiroyuki Sugimoto
Oncotarget 8 ( 54 ) 92157 - 92170 2017
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Peyer's patch innate lymphoid cells regulate commensal bacteria expansion Reviewed
Masaaki Hashiguchi, Yuji Kashiwakura, Hidefumi Kojima, Ayano Kobayashi, Yumiko Kanno, Tetsuji Kobata
Immunology Letters 165 ( 1 ) 1 - 9 2015.5
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IL-33 activates eosinophils of visceral adipose tissue both directly and via innate lymphoid cells Reviewed
Masaaki Hashiguchi, Yuji Kashiwakura, Hidefumi Kojima, Ayano Kobayashi, Yumiko Kanno, Tetsuji Kobata
European Journal of Immunology 45 ( 3 ) 876 - 885 2015.3
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NF kappa B attenuates IL-5 production and upregulates T-box transcription factors in Th2-like T cells Reviewed
Masaaki Hashiguchi, Ayano Kobayashi, Yuji Kashiwakura, Hidefumi Kojima, Yumiko Kanno, Akira Kurosu, Shogo Tokudome, Tetsuji Kobata
CYTOTECHNOLOGY 66 ( 3 ) 373 - 382 2014.5
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CD2-mediated regulation of peripheral CD4(+) CD25(+) regulatory T-cell apoptosis accompanied by down-regulation of Bim Reviewed
Yuji Kashiwakura, Daisuke Sakurai, Yumiko Kanno, Masaaki Hashiguchi, Ayano Kobayashi, Akira Kurosu, Shogo Tokudome, Tetsuji Kobata, Hidefumi Kojima
IMMUNOLOGY 139 ( 1 ) 48 - 60 2013.5
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Intact B7-H3 signaling promotes allograft prolongation through preferential suppression of Th1 effector responses Reviewed
Takuya Ueno, Melissa Y. Yeung, Martina McGrath, Sunmi Yang, Nadia Zaman, Benjamin Snawder, Robert F. Padera, Ciara N. Magee, Rostic Gorbatov, Masaaki Hashiguchi, Miyuki Azuma, Gordon J. Freeman, Mohamed H. Sayegh, Nader Najafian
European Jounal of Immunology 42 ( 9 ) 2343 - 2353 2012.9
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Antibodies Against B7-DC with Differential Binding Properties Exert Opposite Effects Reviewed
Patcharee Ritprajak, Masaaki Hashiguchi, Hisaya Akiba, Hideo Yagita, Ko Okumura, Miyuki Azuma
Hybridoma 31 ( 1 ) 40 - 47 2012.2
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Hashiguchi M, Inamochi Y, Nagai S, Otsuki N, Piao J, Kobori H, Kanno Y, Kojima H, Kobata T, Azuma M
Open Journal of Immunology 2 ( 1 ) 9 - 16 2012
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Naive CD4+ T cells of Peye's patches produce more IL-6 than those of spleen in response to antigenic stimulation Reviewed
Masaaki Hashiguchi, Satoshi Hachimura, Akio Ametani, Takehito Sato, Hidefumi Kojima, Yoshihiro Kumagai, Sonoko Habu, Tetsuji Kobata, Shuichi Kaminogawa
IMMUNOLOGY LETTERS 141 ( 1 ) 109 - 115 2011.12
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Immunoregulatory Molecule B7-H1 (CD274) Contributes to Skin Carcinogenesis Reviewed
Yujia Cao, Lu Zhang, Pacharee Ritprajak, Fumihiko Tsushima, Pornpan Youngnak-Piboonratanakit, Yosuke Kamimura, Masaaki Hashiguchi, Miyuki Azuma
Cancer Research 71 ( 14 ) 4737 - 4741 2011.7
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B7-H1 Overexpression Regulates Epithelial-Mesenchymal Transition and Accelerates Carcinogenesis in Skin Reviewed
Yujia Cao, Lu Zhang, Yosuke Kamimura, Patcharee Ritprajak, Masaaki Hashiguchi, Sachiko Hirose, Miyuki Azuma
Cancer Research 71 ( 4 ) 1235 - 1243 2011.2
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Enhancement of effector CD8+T-cell function by tumour-associated B7-H3 and modulation of its counter-receptor triggering receptor expressed on myeloid cell-like transcript 2 at tumour sites Reviewed
Hiroko Kobori, Masaaki Hashiguchi, Jinhua Piao, Moriyuki Kato, Patcharee Ritprajak, Miyuki Azuma
Immunology 130 ( 3 ) 363 - 373 2010.7
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Keratinocyte-associated B7-H1 directly regulates cutaneous effector CD8+ T cell responses Reviewed
Patcharee Ritprajak, Masaaki Hashiguchi, Fumihiko Tsushima, Narumon Chalermsarp, Miyuki Azuma
Journal of Immunology 184 ( 9 ) 4918 - 4925 2010.5
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Possible involvement of soluble B7-H4 in T cell-mediated inflammatory immune responses Reviewed
Yosuke Kamimura, Hiroko Kobori, Jinhua Piao, Masaaki Hashiguchi, Koichiro Matsumoto, Sachiko Hirose, Miyuki Azuma
Biochemical and Biophysical Research Communications 389 ( 2 ) 349 - 353 2009.11
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Enhancement of T-cell-mediated anti-tumour immunity via the ectopically expressed glucocorticoid-induced tumour necrosis factor receptor-related receptor ligand (GITRL) on tumours Reviewed
Jinhua Piao, Yosuke Kamimura, Hideyuki Iwai, Yujia Cao, Keisuke Kikuchi, Masaaki Hashiguchi, Taro Masunaga, Hongsi Jiang, Kouichi Tamura, Shimon Sakaguchi, Miyuki Azuma
Immunology 127 ( 4 ) 489 - 499 2009.8
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Tim-3 mediates phagocytosis of apoptotic cells and cross-presentation Reviewed
Masafumi Nakayama, Hisaya Akiba, Kazuyoshi Takeda, Yuko Kojima, Masaaki Hashiguchi, Miyuki Azuma, Hideo Yagita, Ko Okumura
Blood 113 ( 16 ) 3821 - 3830 2009.4
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The Glucocorticoid-Induced TNF Receptor-Related Protein (GITR)-GITR Ligand Pathway Acts As a Mediator of Cutaneous Dendritic Cell Migration and Promotes T Cell-Mediated Acquired Immunity Reviewed
Yosuke Kamimura, Hideyuki Iwai, Jinhua Piao, Masaaki Hashiguchi, Miyuki Azuma
J. Immunol. 182 ( 5 ) 2708 - 2716 2009.3
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Triggering receptor expressed on myeloid cell-like transcript 2 (TLT-2) is a counter-receptor for B7-H3 and enhances T cell responses Reviewed
Masaaki Hashiguchi, Hiroko Kobori, Patcharee Ritprajak, Yosuke Kamimura, Haruo Kozono, Miyuki Azuma
Proc. Natl. Acad. Sci. USA 105 ( 30 ) 10495 - 10500 2008.7
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Topical application of cream-emulsified CD86 siRNA ameliorates allergic skin disease by targeting cutaneous dendritic cells Reviewed
Patcharee Ritprajak, Masaaki Hashiguchi, Miyuki Azuma
MOLECULAR THERAPY 16 ( 7 ) 1323 - 1330 2008.7
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GITR ligand-costimulation activates effector and regulatory functions of CD4(+) T cells Reviewed
Hanna Igarashi, Yujia Cao, Hideyuki Iwai, Jinhua Piao, Yosuke Kamimura, Masaaki Hashiguchi, Teruo Amagasa, Miyuki Azuma
BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS 369 ( 4 ) 1134 - 1138 2008.5
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Expression and function of the B and T lymphocyte attenuator (BTLA/CD272) on human T cells Reviewed
N Otsuki, Y Kamimura, M Hashiguchi, M Azuma
BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS 344 ( 4 ) 1121 - 1127 2006.6
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IkB-alpha-specific transcript regulation by the C-terminal end of c-Rel Reviewed
K Iwai, BR Lee, M Hashiguchi, A Fukushima, M Iwashima
FEBS LETTERS 579 ( 1 ) 141 - 144 2005.1
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CD4(-)c-kit(-)CD3 epsilon-IL-2R alpha(+) Peyer's patch cells are a novel cell subset which secrete IL-5 in response to IL-2: implications for their role in IgA production Reviewed
M Kuraoka, M Hashiguchi, S Hachimura, S Kaminogawa
EUROPEAN JOURNAL OF IMMUNOLOGY 34 ( 7 ) 1920 - 1929 2004.7
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Costimulation via glucocorticoid-induced TNF receptor in both conventional and CD25(+) regulatory CD4(+) T cells Reviewed
F Kanamaru, P Youngnak, M Hashiguchi, T Nishioka, T Takahashi, S Sakaguchi, Ishikawa, I, M Azuma
JOURNAL OF IMMUNOLOGY 172 ( 12 ) 7306 - 7314 2004.6
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CD11b(+) Peyer's patch dendritic cells secrete IL-6 and induce IgA secretion from naive B cells Reviewed
A Sato, M Hashiguchi, E Toda, A Iwasaki, S Hachimura, S Kaminogawa
JOURNAL OF IMMUNOLOGY 171 ( 7 ) 3684 - 3690 2003.10
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Decrease in expression of alpha(5)beta(1) integrin during neuronal differentiation of cortical progenitor cells Reviewed
N Yoshida, S Hishiyama, M Yamaguchi, M Hashiguchi, Y Miyamoto, S Kaminogawa, T Hisatsune
Exp. Cell Res. 287 ( 2 ) 262 - 271 2003.7
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Splenic dendritic cells from antigen-fed mice induced antigen-specific T cell unresponsiveness in vivo Reviewed
M Hibi, S Hachimura, T Somaya, E Toda, M Hashiguchi, T Takayama, K Sasaki, T Senga, S Hashizume, S Kaminogawa
Cytotechnology 43 ( 1-3 ) 41 - 48 2003
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Suppressive effect of dietary raffinose on T-helper 2 cell-mediated immunity Reviewed
T Nagura, S Hachimura, M Hashiguchi, Y Ueda, T Kanno, H Kikuchi, K Sayama, S Kaminogawa
British Journal of Nutrition 88 ( 4 ) 421 - 426 2002.10
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Murine Peyer's patch dendritic cells prime naive CD4(+) T cells to produce interferon-gamma Reviewed
A Sato, M Hashiguchi, S Hachimura, S Kaminogawa
CYTOTECHNOLOGY 40 ( 1-3 ) 31 - 38 2002
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Genetic background determines sensitivity to the inhibitory function of NO on T cell proliferation and the amounts of NO production mediated through IFN-gamma Reviewed
A Ozaki, A Fukushima, K Fukata, S Sakamoto, T Taniguchi, M Hashiguch, H Ueno
Microbiology and Immunology 46 ( 8 ) 555 - 563 2002
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Serum IgE response to orally ingested antigen: A novel IgE response model with allergen-specific T-cell receptor transgenic mice Reviewed
Kan Shida, Satoshi Hachimura, Akio Ametani, Mina Ishimori, Mei Ling, Masaaki Hashiguchi, Yoshihiro Ueda, Takehito Sato, Yoshihiro Kumagai, Kotaro Takamizawa, Sonoko Habu, Shuichi Kaminogawa
Journal of Allergy and Clinical Immunology 105 ( 4 ) 788 - 795 2000
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Th2 polarization by higher doses of oral administration of antigen Reviewed
Masaaki Hashiguchi, Satoshi Hachimura, Akio Ametani, Shuichi Kaminogawa
Cytotechnology 33 ( 1/3 ) 237 - 245 2000
Books
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Topical application of siRNA targeting cutaneous dendritic cells in allergic skin disease
Azuma M, Ritprajak P, Hashiguchi M( Role: Joint authorMethods in Molecular Biology (Clifton, N.J.) 623 373 - 381)
2010
Misc.
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B7 family molecules and the recently found function
Clinical immunology & allergology 47 ( 6 ) 696 - 701 2007.6
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The role dendritic cells play in the cytokine response in Peyer's patches
A.Sato, M. Hashiguchi, S. Hachimura, S. Kaminogawa
12 331 - 335 2001
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腸管免疫応答の特性
上野川 修一, 八村敏志, 後藤真生, 好田 正, 橋口昌章, 上野川修一
日本農芸化学会誌 73 ( 5 ) 523 - 527 1999
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上野川 修一, 橋口昌章, 八村敏志, 上野川修一
臨床免疫 30 ( 11 ) 1524 - 1531 1998
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T細胞抗原レセプタートランスジェニックマウスを用いた経口投与抗原に対するパイエル板リンパ球の応答の解析 : 食品
橋口 昌章, 八村 敏志, 飴谷 章夫, 佐藤 健人, 熊谷 善博, 垣生 園子, 上野川 修一
日本農芸化学会誌 70 187 - 187 1996.3
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T細胞抗原レセプタートランスジェニックマウスを用いた経口投与抗原に対するT細胞応答の解析 : 食品
八村 敏志, 橋口 昌章, 植田 祥啓, 飴谷 章夫, 佐藤 健人, 熊谷 善博, 垣生 園子, 上野川 修一
日本農芸化学会誌 70 187 - 187 1996.3
Research Projects
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パイエル板Tfhによる抗体産生制御:対立遺伝子排除の破綻とアレルギーの抑制
Grant number:22K05481 2022.4 - 2025.3
日本学術振興会 科学研究費助成事業 基盤研究(C)
橋口 昌章, 岩井 佳子
Grant amount:\4160000 ( Direct Cost: \3200000 、 Indirect Cost:\960000 )
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Does IL-21 produced in Peyer's patch regulate the affinity of IgA and food allergy?
Grant number:18K05478 2018.4 - 2021.3
Japan Society for the Promotion of Science Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)
Hashiguchi Masaaki
Grant amount:\4290000 ( Direct Cost: \3300000 、 Indirect Cost:\990000 )
IgA is at least partly induced in Peyer’s patches (PPs), which are secondary lymphoid tissues and scatteredly located in the small intestine (SI). However, the precise mechanisms have not been clarified yet. Establishing hybridomas from naive murine PPs revealed the major specificity against double stranded DNA in IgA. The IgA was induced by the intestinal microbes and in PPs, but was independent of CD4+ T cells. IgA positively regulate intestinal bacteria via an antigen-independent manner. TGF-beta induced IgA secretion from naive B cells, but was not enough for the induction of surface IgA. The additional IL-21 and IL-5 upregulate surface IgA+ B cell frequency. The blocking of IL-21R signaling abrogated GC B cell frequency and IgA+ B cells in PPs. PPs were required for oral antigen-specific IgA in the intestine. These results suggest that PPs are required for anti-dsDNA and anti-diet protein IgAs, and that IL-21 and IL-5 coordinately induce IgA.
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Peyer's patch immune cells regulates intestinal bacteria: basic research for the manipulation of intestinal bacteria by foods
Grant number:15K07438 2015.10 - 2018.3
Japan Society for the Promotion of Science Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)
HASHIGUCHI Masaaki, KOBAYASHI Ayano, TASAKU Yumi
Grant amount:\4550000 ( Direct Cost: \3500000 、 Indirect Cost:\1050000 )
Anatomical containment of commensal bacteria in the intestinal mucosa is promoted by innate lymphoid cells (ILCs). We show that Peyer’s patch (PP) ILCs robustly produce IL-22 in the absence of exogenous stimuli. In vivo depletion of ILCs rather than T cells altered the composition of and allowed the proliferation of bacteria in PPs. Collectively, our results show that ILCs restrain commensal bacteria in the PPs.
Intestinal immunoglobulins (Igs) protect against microbes. We have investigated the roles of APRIL (TNFSF13) and BAFF (TNFSF13B) in intestinal Ig induction. PPs are, at least in part, an inductive site for Igs, including IgA. Our results demonstrate that APRIL and BAFF in vivo lowered the frequency of isotype-switched B cells in PPs. These results indicate that APRIL and BAFF paradoxically downregulate homeostatic Ig production in the intestines. -
Functional study of IL-5-producing cells in food allergy using GFP marking system
Grant number:24580196 2012.4 - 2015.3
Japan Society for the Promotion of Science Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)
MASAAKI Hashiguchi, KOBAYASHI Ayano
Grant amount:\5330000 ( Direct Cost: \4100000 、 Indirect Cost:\1230000 )
Eosinophils are multifunctional leukocytes involved in parasite elimination, evocation of allergic reactions, and regulation of adipose tissue. IL-5 is required for eosinophil survival; however, the in vivo mechanisms of eosinophil regulation are not fully understood. A transgenic (tg) mouse model with Il5 promoter-driven EGFP expression was established for detecting the IL-5-producing cells in vivo. The first part of the results demonstrate that innate lymphoid cells (ILCs) activate eosinophils in GAT. The blockage of IL-33R, on the other hand, did not impair EGFP+ ILC numbers but did impair eosinophil numbers in vivo. IL-33 was found to expand eosinophil numbers in CD90+ cell-depleted mice. The latter part of findings demonstrate that IL-33 directly activates eosinophils in GAT, and together with our other findings described above, our findings show that IL-33 has dual pathways via which it activates eosinophils in vivo: a direct activation pathway and a group 2 ILC-mediated pathway.
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Regulatory roles of HIF-1a and glycolysis in autoimmunity
Grant number:24591454 2012.4 - 2015.3
Japan Society for the Promotion of Science Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)
KOBATA Tetsuji, HASHIGUCHI Masaaki, KASHIWAKURA Yuji
Grant amount:\5200000 ( Direct Cost: \4000000 、 Indirect Cost:\1200000 )
In order to understand the pathophysiology of HIF-1α/RAG-2–deficient chimeric mice, which develop autoimmunity resembling human systemic erythematosus, we analyzed mice with conditional knock-outs in HIF-1α in B cells and revealed that autoantibody production is regulated by HIF-1α in the very early stages of B cell development and/or HIF-1α in cells other than B cells. Although HIF-1α/RAG-2–deficient chimeric mice have increased regulatory T cells, we found that regulatory T cells less depend on glycolysis and need CD2-mediated down-regulation of pro-apoptotic Bim for their survival.
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T細胞に依存しない新たな補助シグナル分子機能の解明
Grant number:22021016 2010 - 2011
日本学術振興会 科学研究費助成事業 特定領域研究
東 みゆき, 橋口 昌章, 大野 建州, 神村 洋介, 長谷 英徳
Grant amount:\7700000 ( Direct Cost: \7700000 )
T細胞補助シグナル分子研究は、T細胞上に発現される補助シグナル分子受容体と抗原提示細胞上に発現されるリガンド分子による抗原特異的適応免疫応答に焦点が当たってきたが、本研究では、免疫細胞ではなく組織細胞上に発現される補助シグナル分子リガンドとランゲルハンス細胞あるいはミエロイド系細胞に発現誘導される補助シグナル分子受容体との結合によるT細胞非依存性の免疫応答への関与に注目し検討することで、補助シグナル分子の新たな機能的役割を明らかにすることを目的とした。
プロジェクト1:角化上皮細胞に発現誘導される免疫抑制補助シグナル分子B7-H1(CD274)の機能を明確にする目的で、B7-H1トランスジェニックマウス(Tg)を作成した。化学発癌物質メチルコラントレンにより誘導される早期皮膚炎症と発癌を検討したところ、皮膚炎症はB7-H1:PD-1経路依存性に抑制されたが、上皮発癌率は有意に増加した。B7-H1過剰発現上皮細胞では、上皮間葉移行に関連する接着分子カドヘリンや転写因子発現に変化がおきており、B7-H1による内因性のシグナルが上皮細胞に悪性転化に至る変化を与えた可能性が示された。
プロジェクト2:我々が報告したB7-H3の新規受容体Tlt-2は、T細胞におけるTlt2の発現と機能的関与は少なく、マクロファージなどのミエロイド細胞上に恒常的な発現が認められることから、Tlt2の機能を明確にする目的で、Tlt-2欠損マウスの作出に取り組んだ。Tlt-2欠損マウスにいて、胸腺、脾臓、リンパ節、骨髄、腹腔内細胞における免疫細胞構成比に明らかな違いは認められなかった。ヒトにおいては、Tlt-2とB7-H3は結合しないという論文が発表されたが、我々はヒトにおいてもTlt-2とB7-H3は結合し、この結合はマウスと同様T細胞機能増強に働くことを新たに示した。 -
Immune regulation of oral disease by co-signal molecule B7-H3 and the novel receptor.
Grant number:21592385 2009 - 2011
Japan Society for the Promotion of Science Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)
HASHIGUCHI Masaaki, AZUMA Miyuki
Grant amount:\4420000 ( Direct Cost: \3400000 、 Indirect Cost:\1020000 )
Co-signal molecules play important roles in positively or negatively regulate cell responses. We previously reported that new cosignal ligand murine B7-H3 and the receptor TLT-2 enhance T cell responses. Here we investigate the precise mechanisms and found, in human system, B7-H3 upregulate T cell responses through the ligation with TLT-2, too. We also clarified TLT-2 upregulates anti-tumor immunity through the enhancement of cytotoxicity by CD8^+T cells. These suggest that B7-H3.TLT-2 enhances anti-tumor immunity and imply that strong or continuous B7-H3.TLT-2 signaling lowers TLT-2.
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Analyses of Regulatory Mechanisms in Oral Immune Responses and Development of a New Immunotherapy Targeting Dendritic Cells
Grant number:20249075 2008 - 2010
Japan Society for the Promotion of Science Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (A)
AZUMA Miyuki, HASHIGUCHI Masaaki, HASE Hidenori
Grant amount:\48490000 ( Direct Cost: \37300000 、 Indirect Cost:\11190000 )
Migrating dendritic cells (DC) from oral mucosa into regional lymph nodes were divided into four subsets similar to cutaneous migrating DCs. CD207-CD11c^<hi> F1-DCs that migrated quickly, expressed the highest levels of co-signal molecules, whereas CD207+CD11c^<int/lo> F3-DCs that migrated at the later time point were further divided into both CD103+CD207+ submucosal DCs and CD103- Langerhans cells (LCs) and the latter expressed the lowest co-signal molecules, suggest tolerogenic properties. We demonstrated that using mouse skin allergic models, silencing of CD86 co-signal molecule in skin DCs by RNA interference efficiently inhibited both early innate immune responses at the local site and adaptive immune responses in the secondary lymphoid tissues.
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機能T細胞のマルチイメージング化による歯周疾患の免疫病態解析手法の確立
Grant number:20659293 2008 - 2009
日本学術振興会 科学研究費助成事業 挑戦的萌芽研究
東 みゆき, 橋口 昌章
Grant amount:\3000000 ( Direct Cost: \3000000 )
『機能T細胞のマルチイメージング化による歯周疾患の免疫病態解析手法の確立』
(2010/04/05神村)
様々な免疫疾患の病態発生において新しいT細胞サブセットであるTh17と制御性T細胞(Treg)の関与が明確になってきている。これらの細胞分化はナイーブCD4^+T細胞が抗原刺激を受ける際の微小環境により決定される。本研究では、歯周病におけるT細胞サブセットの動きを生体において可視化することで、真の病態解明に迫ろうというのが当初の目的であった。当初の戦略としては、Th17に特異的に発現する転写因子ROR(gamma)tおよびTh17細胞の産生するサイトカインであるIL-17、またはTreg分化のマスター遺伝子である転写因子Foxp3に注目し、これらのプロモーターにレポーターとしてeGFP,RFP,あるいはLuciferaseを発現させることでTh17およびTregの可視化を行うべく、ウイルスベクターを作成し、T細胞に遺伝子導入し発現確認を行う予定であった。しかしながら、先んじてL.MatthiasらによりTh17、F.JasonらによりTregのレポーターマウスの樹立が報告され、これからトランスジェニックマウスを樹立するよりも、共同研究としてすでに樹立されたマウスを入手する方が得策と考え、マウス歯周病モデルの樹立を先行させることに計画を変更した。全ゲノム解読が既に完了しているヒト歯周病患者由来のPorphyromonas gingivalis菌株であるTDC60の提供を受け、マウス歯肉に塗布感染させ、歯周病の発症実験を行った。病態評価のために、マイクロCTによる歯槽骨吸収、歯肉の免疫組織染色、歯肉で発現している炎症関連分子のリアルタイムPCR、血清・唾液・歯肉溝滲出液中のPG菌特異的な抗体価の測定などの評価系を立ち上げ、ほぼ完了した。マウスの歯周病モデルは、Th17とTregの機能や動態解析のみならず、様々な分子や細胞の歯周病への関与を検討していく上で、今後有益であると考えられる。 -
Triggering receptor expressed on myeloid cell-like transcript 2(TLT-2)is a counter-receptor for B7-H3 and enhances T cell responses
Grant number:19592168 2007 - 2008
Japan Society for the Promotion of Science Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)
HASHIGUCHI Masaaki, AZUMA Miyuki
Grant amount:\4290000 ( Direct Cost: \3300000 、 Indirect Cost:\990000 )
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周囲環境により変化する多機能性ミエロイド細胞の癌治療への応用
Grant number:18015017 2006 - 2007
日本学術振興会 科学研究費助成事業 特定領域研究
東 みゆき, 橋口 昌章
Grant amount:\5600000 ( Direct Cost: \5600000 )
マウス扁平上皮癌NRS1モデルにおいて増加するCD11b^+Gr-1^+のミエロイド細胞は,末梢血および脾臓,リンパ節に集積し.この細胞は,未刺激ではアロ抗原提示能を持たず担がんマウスT細胞の増殖反応をIFN-γ産生依存性に抑制すること、in vitroでGM-CSF+IL-4存在下の培養後は,抗原提示能力を有する樹状細胞に分化できることを明らかにしてきた。しかしながら、in vitroで分化させたこの細胞を移入することにより癌の縮小効果が得られるかどうか詳細な検討を続けたところ,残念ながら,担癌状態においては,抗原提示能としての能力を発揮できないことが明らかになった.
このミエロイド細胞はGr-1およびCD11bの発現パターンが幅広く、ヘテロな細胞集団であり、実際にどの表現型を有する細胞分画が抑制機能を担っているのかを明らかにするために,Gr-1およびCD11bの発現強度別に詳細な細胞分画に分けその機能を検討した.評価系として、OVA特異的TCRトランスジェニックマウスOT-1 CD8 T細胞のペプチドパルス骨髄由来樹状細胞に対する抗原特異的増殖反応およびIFN-γ産生を指標にした。
担癌マウスにおいて最も顕著に増加するGr-1^<hi>CD11b^<hi>分画は増殖抑制活性を示さず,Gr-1^<lo>CD11b^<hi>、Gr-1^<lo>CD11b^<lo>およびGr-1-CD11b^<lo>に増殖抑制活性があることが明らかとなった。IFN-γの産生は,むしろ増強された。さらに、Gr-1^<lo>CD11b^<lo>に含まれるF4/80陽性分画には強い抑制活性は認められなかった。抑制活性は抗IFN-γ中和抗体もしくはiNOS阻害剤(L-NAME)の添加で部分的に解除されたが、抗IL-10中和抗体、抗TGF-β中和抗体、IDO阻害剤(1-MT)の添加では影響を受けなかった。 -
The Regulation of Oral Mucosa Immunity by Immune Co-inhibitory Molecules
Grant number:16591884 2004 - 2005
Japan Society for the Promotion of Science Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (C)
HASHIGUCHI Masaaki, AZUMA Miyuki
Grant amount:\2900000 ( Direct Cost: \2900000 )
Mucosal tissues including oral cavity are distinguished from the others in the point of immune responses. On the other hand, co-signal molecules are known to function positively or negatively. That is why these molecules are important for the regulation of immune responses. In this research, we aimed to control the unique immune responses of mucosa by a modulation of co-inhibitory molecules on keratinocytes, with a further desire of developing a mucosa vaccination system.
Genetically engineered animals are powerful tools for examine in vivo immune responses. We made a construct for the expression of a co-inhibitory molecule, B7-H1 (PD-L1) specifically on keratinocyte under the control of keratin 14 (K14) promoter and using this we established a K14-B7-H1 transgenic mouse. Keratinocytes from this transgenic mouse showed the higher level of B7-H1 but the other cells tested not. On the contact hypersensitivity model with painting DNFB on the belly and ears, K14-B7-H1 transgenic mice showed smaller swellings of ears when a relatively lower dose was administered and showed larger swellings when a relative higher dose was administered. As described previously, B7-H1 is known to be a co-inhibitory molecule. From this points, we had expected the smaller swellings despite of the dosages, but a higher dose induced larger swellings, which suggest that immune responses at mucosa are distinct where B7-H1 is involved. The further investigation is to be accomplished. -
RNA干渉による口腔粘膜の炎症制御に関する研究
Grant number:16659517 2004 - 2005
日本学術振興会 科学研究費助成事業 萌芽研究
東 みゆき, 橋口 昌章
Grant amount:\3100000 ( Direct Cost: \3100000 )
口腔粘膜上皮を構成している細胞には,角化上皮細胞以外に,プロフェッショナル抗原提示細胞であるランゲルハンス細胞と上皮内T細胞が存在し,この3者間において,膜表面分子,あるいはサイトカインを介した相互作用によって免疫応答が営まれている.口腔粘膜上皮は,微生物やそれ以外の様々な外来刺激・ストレスを受ける最前線にあり,種々の寛容誘導・維持機構が備わっているはずであるが,その破綻により様々な病的状態が生じる.CD86(B7-2)発現制御もその重要な機構の一つである.慢性炎症状態の粘膜上皮においては,T細胞活性化において重要な補助シグナル分子CD86がプロフェッショナル抗原提示細胞のみならず,角化上皮細胞や上皮内T細胞上に異所性発現が認められ,炎症治癒遅延機序にCD86が関与することが示唆されている.それで我々はCD86分子に注目し,それをRNAiをもちいたノックダウンにより,慢性炎症をコントロールすることを試みた.前回,CD86分子の発現を効果的にノックダウンする配列を有する二本鎖RNAを同定したことを報告した.今回,マウス接触性過敏症モデルにおいて,その二本鎖RNAのin vivoでの効果を検討した.DNFBあるいはFITCをハプテン抗原とし,感作後,耳介への再刺激直前に上記の二本鎖RNAを投与し,続いて感作を行い,耳介腫脹反応を測定した.その結果,CD86抑制二本鎖RNA群は,コントロール二本鎖RNA群と比較して耳介腫脹反応において,有意に抑制が認められた.この結果は,in vivoにおける慢性炎症のコントロールに成功したことを示している.また,これまで未開拓であった,「RNAiのin vivoでの応用」において非常に意義があると考えられ,さらなる基礎データの蓄積により臨床応用も充分に期待できる.
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Functional analysis of costimulatory molecules in oral diseases and their intervention for clinical application
Grant number:13854021 2001 - 2005
Japan Society for the Promotion of Science Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (S)
AZUMA Miyuki, HASHIGUCHI Masaaki
Grant amount:\108550000 ( Direct Cost: \83500000 、 Indirect Cost:\25050000 )
We investigated expression and function of costimulatory molecules including PD-1:B7-H1/B7-DC, ICOS:B7h, BTLA, B7-H3, and B7-H3 in oral immune responses and diseases. B7-H1 that is one of ligands for PD-1 was induced on a various inflammatory tissue cells as well as immune cells, whereas expression of B7-DC was limited on activated dendritic cells (DCs) and macrophages. Our results demonstrate the involvement of PD-1:B7-H1 pathway in immune regulation based on the studies from the comparative analyses between expression and clinical features and prognosis in oral lichen planus (OLP) and oral cancer, and in addition, the in vivo treatments with blocking monoclonal antibodies in models of skin contact hypersensitivity and oral cancer. A ligand of ICOS, B7h was less expressed as compared with B7-H1, but was expressed at high levels on endothelial cells in OLP and oral cancer tissues, suggesting the involvement of B7h in lymphocyte infiltration into the tissues.
We have established a murine pulpitis model using fresh-frozen decalcified hard tissue sections and an immunofluorescence staining and examined dental pulp after dentin exposure. We found that two types of DCs, CD11c^+F4/80^- and CD11c^-F4/80^+, exist in dental pulp. CD11c^+F4/80^- cells located in the pulp-dentin border and expressed constitutively TLR2, TLR4, and CD205. CD11c^-F4/80^+ cells located in the central pulp and were lacking the above molecules. Both types of cells migrated rapidly to the P-D border of treated cusp side, but a part of F4/80^+ cells alone induced a costimulatory molecule CD86. Simultaneously, F4/80^+CD86^+ cells in the regional lymph nodes increased, suggesting the migration of these cells from the pulp. These results suggest that antigen-capture and migration of pulpal DCs may occur and the migrated DCs may induce a consequent adoptive immune response. Our findings provide important information for estimating the healing properties of dental pulp and for developing possible treatments of dental restoration. -
ホメオスターシスと自己寛容に関わるT細胞補助刺激分子の機能解析とその人為的制御
Grant number:13140201 2001 - 2005
日本学術振興会 科学研究費助成事業 特定領域研究
東 みゆき, 橋口 昌章, 小園 裕子
Grant amount:\135100000 ( Direct Cost: \135100000 )
エフェクターT細胞による臓器特異的な局所免疫応答においては、B7補助シグナル経路が正および負に免疫応答を調節していることを多くのマウス疾患モデルを用いた検討から明らかにしてきた.本年は、PD-1:B7-H1抑制経路に加え、BTLA,B7-H3,B7-H4経路の機能について検討を行なった.また、エフェクターT細胞と制御性T細胞のそれぞれに対する補助刺激分子の関わりという視点からも解析を進めた.炎症時に局所組織細胞に誘導されるB7-H1の機能を明らかにするために、角化細胞特異的にB7-H1を発現させたトランスジェニックマウスを作成した.ハプテン抗原を用いた接触性過敏反応において、早期応答と遅延型応答にB7-H1が異なって関与していることを示す結果を得た.また、B7-H3およびB7-H4の機能解析において、in vivoおよびin vitroにおける抗体を用いた分子機能解析結果は、これらのシグナル経路がB7-H1/B7-DCと同様に免疫応答を正または負に複雑に制御する可能性を示した.この複雑な機構の理由のひとつとして、制御性T細胞の関与が示唆された.Co-stimulatorであるCD28とGITR、Co-inhibitorであるPD-1とBTLAは、conventionalなCD25^-CD4^+エフェクターT細胞に対してのみならず、CD25^-CD4^+制御性T細胞に対しても増殖および機能調節Co-signal分子として働くこと、in vivoにおいては組織樹状細胞あるいは組織細胞と制御性T細胞間相互作用において調節されていることが示唆された.