Your search keyword '"Takehara, Kazuhiko"' showing total 25 results

1. Potential immunologic targets for treating fibrosis in systemic sclerosis: a review focused on leukocytes and cytokines.

Author

Hasegawa M and Takehara K

Subjects

Antibodies, Monoclonal therapeutic use, B-Lymphocytes immunology, B-Lymphocytes pathology, Cytokines immunology, Cytokines metabolism, Fibrosis immunology, Humans, Interleukins antagonists & inhibitors, Scleroderma, Systemic immunology, Signal Transduction drug effects, T-Lymphocytes immunology, T-Lymphocytes pathology, B-Lymphocytes drug effects, Cytokines antagonists & inhibitors, Drug Delivery Systems methods, Fibrosis drug therapy, Scleroderma, Systemic drug therapy, T-Lymphocytes drug effects

Abstract

Objectives: Systemic sclerosis (SSc) is a connective tissue disease characterized by tissue fibrosis. Although the pathogenesis remains unclear, a variety of cells contribute to the fibrotic process via interactions with each other and production of various cytokines. Recent literature related to the immunologic pathogenesis and future strategies for treating the fibrosis of SSc are discussed and, especially, this literature-based review that includes the authors' perspective, focused on leukocytes and cytokines., Methods: A PubMed search for articles published between January 2005 and January 2012 was conducted using the following keywords: systemic sclerosis, leukocyte, cytokine, growth factor, and chemokine. The reference lists of identified articles were searched for further articles., Results: Targeting profibrogenic cytokines, including transforming growth factor-β, is still a very active area of research in SSc and most cellular studies have focused on the roles of fibroblasts in SSc. However, a growing number of recent studies indicate a role for B cells in the development of SSc and other autoimmune diseases such as systemic lupus erythematosus. Therefore, B-cell-targeted therapies, including currently available monoclonal antibodies against CD19, CD20, CD22, and B-cell-activating factor, belonging to the tumor necrosis factor family represent possible treatment options. Furthermore, the modulation of T-cell costimulatory molecules such as a recombinant fusion protein of cytotoxic T-lymphocyte antigen-4 may be as effective in SSc as it is in treating other autoimmune diseases. Approaches to antagonize interleukin (IL)-1, IL-6, or IL-17A signaling may also be attractive., Conclusions: This review describes recent advances in the treatment of fibrosis in SSc patients focused on immunologic strategies, such as leukocyte- or cytokine-targeted therapies., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

2. Neutralizing monoclonal antibody to human connective tissue growth factor ameliorates transforming growth factor-beta-induced mouse fibrosis.

Author

Ikawa Y, Ng PS, Endo K, Kondo M, Chujo S, Ishida W, Shirasaki F, Fujimoto M, and Takehara K

Subjects

Animals, Antibodies, Monoclonal genetics, Collagen Type I genetics, Collagen Type I metabolism, Connective Tissue Growth Factor, Female, Fibrosis pathology, Humans, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, RNA, Messenger metabolism, Scleroderma, Systemic immunology, Scleroderma, Systemic pathology, Skin pathology, Antibodies, Monoclonal metabolism, Fibrosis chemically induced, Immediate-Early Proteins metabolism, Intercellular Signaling Peptides and Proteins metabolism, Transforming Growth Factor beta pharmacology

Abstract

Skin fibrotic disorders such as systemic sclerosis (SSc) are characterized by an excessive accumulation of extracellular matrix (ECM) and are understood to develop under the influence of fibrogenic growth factors. To better understand the detailed mechanisms of persistent fibrosis in SSc, we have previously established an animal model of skin fibrosis induced by exogenous application of growth factors. In this model, transforming growth factor-beta (TGF-beta) transiently induced subcutaneous fibrosis and serial injections of connective tissue growth factor (CTGF) after TGF-beta caused persistent fibrosis. These results suggest that CTGF plays an important role in the development of persistent skin fibrosis and that CTGF may be a potential and specific therapeutic target in skin fibrosis. Therefore, the aim of the current study is to develop a neutralizing monoclonal antibody against human CTGF. We also investigated the neutralizing effect of the antibodies in our animal model. Firstly, by using the DNA immunization method, we developed a panel of anti-CTGF antibodies recognizing the native conformation of human CTGF. Next, to examine the anti-fibrosing effects of these antibodies, newborn B6 mice received subcutaneous injections of TGF-beta for 3 days with either anti-CTGF neutralizing antibodies or control purified immunoglobulin. Anti-CTGF antibodies significantly reduced skin fibrosis and collagen contents compared with the control group. These results suggest that our anti-CTGF antibodies are capable of blocking the development of skin fibrosis at least partially and these anti-CTGF neutralizing antibodies may be useful as the feasible strategy to treat skin fibrotic diseases as SSc.

Published

2008

3. BAFF antagonist attenuates the development of skin fibrosis in tight-skin mice.

Author

Matsushita T, Fujimoto M, Hasegawa M, Matsushita Y, Komura K, Ogawa F, Watanabe R, Takehara K, and Sato S

Subjects

Animals, Autoantibodies metabolism, B-Cell Activating Factor blood, B-Cell Activating Factor physiology, B-Lymphocytes metabolism, Cytokines metabolism, Female, Fibrosis pathology, Genotype, Mice, Mice, Inbred C57BL, Mice, Transgenic, Models, Biological, B-Cell Activating Factor antagonists & inhibitors, B-Cell Activating Factor genetics, B-Cell Activation Factor Receptor metabolism, Fibrosis genetics, Gene Expression Regulation, Skin pathology

Abstract

The tight-skin (TSK/+) mouse, a genetic model for systemic sclerosis (SSc), develops cutaneous fibrosis and autoimmunity. Although immunological abnormalities have been demonstrated in TSK/+ mice, the roles of B-cell-activating factor belonging to the tumor necrosis factor family (BAFF), a potent B-cell survival factor, have not been investigated. Serum BAFF levels in TSK/+ mice were examined by ELISA. Newborn TSK/+ mice were treated with BAFF antagonist, and then skin fibrosis of 8-week-old mice was assessed. Serum BAFF levels were significantly elevated in TSK/+ mice. Remarkably, BAFF antagonist inhibited the development of skin fibrosis, hyper-gamma-globulinemia, and the autoantibody production in TSK/+ mice. The skin from TSK/+ mice showed upregulated expressions of fibrogenic cytokines, such as IL-6 and IL-10, while BAFF antagonist significantly suppressed them. Reciprocally, BAFF antagonist augmented antifibrogenic cytokines, such as IFN-gamma, in the skin of TSK/+ mice. Furthermore, TSK/+ B cells with BAFF stimulation had a significantly enhanced ability to produce IL-6. The results suggest that BAFF/BAFF receptor system is critical for the development of skin fibrosis in TSK/+ mice and could be a potent therapeutical target.

Published

2007

4. Connective tissue growth factor causes persistent proalpha2(I) collagen gene expression induced by transforming growth factor-beta in a mouse fibrosis model.

Author

Chujo S, Shirasaki F, Kawara S, Inagaki Y, Kinbara T, Inaoki M, Takigawa M, and Takehara K

Subjects

Animals, Chemotaxis, Leukocyte drug effects, Chemotaxis, Leukocyte physiology, Collagen Type I genetics, Connective Tissue Growth Factor, Disease Models, Animal, Fibroblasts drug effects, Fibroblasts metabolism, Fibrosis genetics, Fibrosis physiopathology, Gene Expression Regulation drug effects, Macrophages drug effects, Macrophages metabolism, Mast Cells drug effects, Mast Cells metabolism, Mice, Mice, Transgenic, Procollagen genetics, Promoter Regions, Genetic drug effects, Promoter Regions, Genetic genetics, RNA, Messenger drug effects, RNA, Messenger metabolism, Scleroderma, Systemic genetics, Scleroderma, Systemic physiopathology, Skin Diseases genetics, Skin Diseases metabolism, Skin Diseases physiopathology, Transcriptional Activation drug effects, Transcriptional Activation physiology, Transforming Growth Factor beta metabolism, Transforming Growth Factor beta3, Up-Regulation drug effects, Up-Regulation physiology, Collagen Type I biosynthesis, Extracellular Matrix metabolism, Fibrosis metabolism, Gene Expression Regulation physiology, Immediate-Early Proteins pharmacology, Intercellular Signaling Peptides and Proteins pharmacology, Procollagen biosynthesis, Scleroderma, Systemic metabolism, Transforming Growth Factor beta pharmacology

Abstract

Skin fibrotic disorders such as systemic sclerosis (SSc) are characterized by an excessive production of extracellular matrix (ECM) and understood to develop under the influence of certain growth factors. Connective tissue growth factor (CTGF) is a cysteine-rich mitogenic peptide that is implicated in various fibrotic disorders and induced in fibroblasts after activation with transforming growth factor-beta (TGF-beta). To better understand the mechanisms of persistent fibrosis seen in SSc, we previously established an animal model of skin fibrosis induced by exogenous application of growth factors. In this model, TGF-beta transiently induced subcutaneous fibrosis and serial injections of CTGF after TGF-beta caused persistent fibrosis. To further define the mechanisms of skin fibrosis induced by TGF-beta and CTGF in vivo, we investigated in this study, the effects of growth factors on the promoter activity of the proalpha2 (I) collagen (COL1A2) gene in skin fibrosis. For this purpose, we utilized transgenic reporter mice harboring the -17 kb promoter sequence of the mouse COL1A2 linked to either a firefly luciferase gene or a bacterial beta-galactosidase gene. Serial injections of CTGF after TGF-beta resulted in a sustained elevation of COL1A2 mRNA expression and promoter activity compared with consecutive injection of TGF-beta alone on day 8. We also demonstrated that the number of fibroblasts with activated COL1A2 transcription was increased by serial injections of CTGF after TGF-beta in comparison with the injection of TGF-beta alone. Furthermore, the serial injections recruited mast cells and macrophages. The number of mast cells reached a maximum on day 4 and remained relatively high up to day 8. In contrast to the kinetics of mast cells, the number of macrophages was increased on day 4 and continued to rise during the subsequent consecutive CTGF injections until day 8. These results suggested that CTGF maintains TGF-beta-induced skin fibrosis by sustaining COL1A2 promoter activation and increasing the number of activated fibroblasts. The infiltrated mast cells and macrophages may also contribute to the maintenance of fibrosis., (Copyright 2004 Wiley-Liss, Inc.)

Published

2005

5. Transforming Growth Factor-ß and Connective Tissue Growth Factor

Author

Fujimoto, Manabu, Takehara, Kazuhiko, Takehara, Kazuhiko, editor, Fujimoto, Manabu, editor, and Kuwana, Masataka, editor

Published

2016

6. Characteristics of Japanese patients with eosinophilic fasciitis: A brief multicenter study.

Author

Yamamoto, Toshiyuki, Ito, Takashi, Asano, Yoshihide, Sato, Shinichi, Motegi, Sei‐ichiro, Ishikawa, Osamu, Matsushita, Takashi, Takehara, Kazuhiko, Makino, Takamitsu, Okiyama, Naoko, Fujimoto, Manabu, Jinnin, Masatoshi, and Ihn, Hironobu

Abstract

Eosinophilic fasciitis is a relatively rare cutaneous fibrotic condition affecting the deep fascia of the extremities, with or without peripheral blood eosinophilia. To examine the characteristics of Japanese patients with eosinophilic fasciitis, we conducted a brief, multicenter, retrospective survey at seven university hospitals. In total, 31 patients were identified as having eosinophilic fasciitis, among whom 30 patients fulfilled the Japanese diagnostic criteria. The male : female ratio was 2.3:1, and the mean age was 47.7 years. Three of the patients were under 20 years old. The possible triggering factors included muscle training, sports, walking or sitting for a long time, physical work, insect bite and drug. Co‐occurrence of morphea was observed in nine cases (29%), and malignancies were associated in three (two hematological malignancies and one internal malignancy). Immunological abnormalities in the serum showed positive antinuclear antibody, positive rheumatoid factor, increased aldolase levels and increased immunoglobulin G levels. The patients were treated with either monotherapy or combination therapy by oral prednisolone (20–80 mg/day), methotrexate (6–10 mg/week), cyclosporin (100–150 mg/day), mizoribine, infliximab and phototherapy. Methylprednisolone pulse therapy was performed in six cases. By contrast, spontaneous improvement due to resting only was observed in two cases, and skin hardening was improved by withdrawal of the anticancer drug in one case. This study suggests several characteristics of Japanese patients with eosinophilic fasciitis, namely male predominance, rare pediatric occurrence, immunological abnormalities and coexistence with morphea. Systemic prednisolone is the first‐line therapy, but pulse therapy is occasionally required for severe cases. The triggering events of physical stress are not so frequent as have previously been reported, and various factors or even unknown factors may be associated with the induction of eosinophilic fasciitis. [ABSTRACT FROM AUTHOR]

Published

2020

7. Adipose‐derived stromal/stem cells successfully attenuate the fibrosis of scleroderma mouse models.

Author

Okamura, Ai, Matsushita, Takashi, Komuro, Akito, Kobayashi, Tadahiro, Maeda, Shintaro, Hamaguchi, Yasuhito, and Takehara, Kazuhiko

Subjects

STEM cells, SYSTEMIC scleroderma, PULMONARY fibrosis, PROGENITOR cells, FIBROSIS

Abstract

Aim: Systemic sclerosis (SSc) is an autoimmune disease characterized by skin and lung fibrosis. Although SSc has a high mortality risk, an effective treatment for the disease has not been established yet. Mesenchymal stromal/stem cells (MSCs) are multipotential nonhematopoietic progenitor cells that have the ability to regulate immune responses. Adipose‐derived stromal/stem cells (ASCs), one of the types of MSCs, have the advantage of accessibility and potent immunomodulatory effects when compared with other MSCs, such as bone marrow‐derived MSCs. This study aimed to investigate the antifibrotic effect of ASCs in scleroderma mouse models, including bleomycin‐induced scleroderma and sclerodermatous chronic graft‐versus‐host disease (Scl‐cGVHD) models. Method: ASCs were intravenously administered to a bleomycin‐induced scleroderma or Scl‐cGVHD model on day 0. We compared the skin and lung fibrosis of scleroderma model mice between the ASC‐treated group and control group. Results: Administration of ASCs attenuated the skin and lung fibrosis of bleomycin‐induced scleroderma and Scl‐cGVHD model mice compared to that in the control mice. Immunohistochemical staining showed that ASCs suppressed the infiltration of CD4+, CD8+ T cells and macrophages into the dermis of bleomycin model mice compared to that in control mice. In addition, ASCs attenuated the messenger RNA expression of collagen and fibrogenic cytokines, such as interleukin (IL)‐6 and IL‐13, in the skin of bleomycin model mice. ASCs also reduced the frequency of fibrogenic cytokine‐producing CD4+ T cells and effector B cells in the spleen of bleomycin model mice. Conclusion: ASCs could prove to be a potential therapeutic agent for use in patients with SSc. [ABSTRACT FROM AUTHOR]

Published

2020

8. An update on biomarker discovery and use in systemic sclerosis.

Author

Matsushita, Takashi and Takehara, Kazuhiko

Abstract

Introduction: Systemic sclerosis (SSc) is an autoimmune disease characterized by excessive extracellular matrix deposition in the skin and internal organs. Three major abnormalities, autoimmunity, vasculopathy, and fibrosis, are considered to play important roles in the pathophysiology of SSc. SSc is a heterogeneous disease with clinical features, disease progress, therapeutic response, and prognosis. Therefore, identification of biomarkers, which can predict the course of the disease, is required for the progress of clinical practice. Areas covered: This review focuses on various SSc biomarkers for diagnosis, disease severity, and activity, as well as newly emerging and promising SSc biomarkers. Search was through PubMed and we focus on the papers in the last 5 years. Expert commentary: Biomarkers for SSc can be categorized into several groups: activity biomarker, severity biomarker, predictive biomarker, and biomarkers for specific clinical features (skin fibrosis, lung fibrosis, pulmonary arterial hypertension, peripheral vasculopathy, gastrointestinal, and malignancy). Some chemokines, such as CCL2 and CXCL4, have been identified as biomarkers of skin and lung fibrosis in SSc. In addition, anti-RNA polymerase III antibody has been noted to be a predictive biomarker of gastric antral vascular ectasia and malignancy. [ABSTRACT FROM PUBLISHER]

Published

2017

9. Potential roles of interleukin-17A in the development of skin fibrosis in mice.

Author

Okamoto, Yoshinobu, Hasegawa, Minoru, Matsushita, Takashi, Hamaguchi, Yasuhito, Huu, Doanh Le, Iwakura, Yoichiro, Fujimoto, Manabu, and Takehara, Kazuhiko

Subjects

ANIMAL experimentation, BIOLOGICAL models, FLOW cytometry, IMMUNOHISTOCHEMISTRY, INTERLEUKINS, MICE, POLYMERASE chain reaction, RESEARCH funding, SKIN, STATISTICS, SYSTEMIC scleroderma, U-statistics, DATA analysis, FIBROSIS, EQUIPMENT & supplies, REVERSE transcriptase polymerase chain reaction

Abstract

Objective Although transforming growth factor β (TGFβ) and connective tissue growth factor (CTGF) have been considered to play central roles in the pathogenesis of systemic sclerosis (SSc), other cytokines may also be crucial for the development of SSc. The aim of this study was to examine the roles of T helper cytokines in the development of skin fibrosis. Methods To compare the roles of Th1, Th2, and Th17 cytokines, we examined bleomycin-induced SSc in mice deficient for interferon-γ (IFNγ), interleukin-4 (IL-4), and IL-17A. The mechanism by which IL-17A contributes to bleomycin-induced fibrosis was investigated in vivo and in vitro. The outcome of mice lacking IL-17A was also investigated in TSK-1 mice. Results The loss of IL-17A significantly attenuated bleomycin-induced skin fibrosis, whereas a deficiency of IFNγ or IL-4 did not. Leukocyte infiltration and the expression of TGFβ and CTGF messenger RNA in bleomycin-injected skin were significantly reduced in IL-17A-deficient mice compared with wild-type (WT) mice. Daily bleomycin injections induced the expression of IL-17A in the skin and potent IL-17A producers in splenic CD4+ T cells from WT mice. Furthermore, a skin fibroblast cell line expressed increased TGFβ, CTGF, and collagen after the addition of recombinant IL-17A. IL-17A deficiency also attenuated skin thickness in TSK-1 mice. Conclusion This study demonstrates that IL-17A contributes to skin fibrosis in 2 mouse models of SSc. These findings suggest that inhibition of IL-17A represents a therapeutic target for antagonizing fibrotic skin disorders such as SSc. [ABSTRACT FROM AUTHOR]

Published

2012

10. Egr-1 Induces a Profibrotic Injury/Repair Gene Program Associated with Systemic Sclerosis.

Author

Bhattacharyya, Swati, Sargent, Jennifer L., Du, Pan, Lin, Simon, Tourtellotte, Warren G., Takehara, Kazuhiko, Whitfield, Michael L., and Varga, John

Subjects

SYSTEMIC scleroderma, ENDOTHELIAL growth factors, TRANSFORMING growth factors, FIBROSIS, SCLERODERMA (Disease), TRANSCRIPTION factors, EXTRACELLULAR matrix, GENE expression, SKIN biopsy

Abstract

Transforming growth factor-ß (TGF-ß) signaling is implicated in the pathogenesis of fibrosis in scleroderma or systemic sclerosis (SSc), but the precise mechanisms are poorly understood. The immediate-early gene Egr-1 is an inducible transcription factor with key roles in mediating fibrotic TGF-ß responses. To elucidate Egr-1 function in SSc-associated fibrosis, we examined change in gene expression induced by Egr-1 in human fibroblasts at the genome-wide level. Using microarray expression analysis, we derived a fibroblast "Egr-1-responsive gene signature" comprising over 600 genes involved in cell proliferation, TGF-ß signaling, wound healing, extracellular matrix synthesis and vascular development. The experimentally derived "Egr-1-responsive gene signature" was then evaluated in an expression microarray dataset comprising skin biopsies from 27 patients with localized and systemic forms of scleroderma and six healthy controls. We found that the "Egr-1 responsive gene signature" was substantially enriched in the "diffuse-proliferation" subset comprising exclusively of patients with diffuse cutaneous SSc (dcSSc) of skin biopsies. A number of Egr-1-regulated genes was also associated with the "inflammatory" intrinsic subset. Only a minority of Egr-1-regulated genes was concordantly regulated by TGF-ß. These results indicate that Egr-1 induces a distinct profibrotic/wound healing gene expression program in fibroblasts that is associated with skin biopsies from SSc patients with diffuse cutaneous disease. These observations suggest that targeting Egr-1 expression or activity might be a novel therapeutic strategy to control fibrosis in specific SSc subsets. [ABSTRACT FROM AUTHOR]

Published

2011

11. Inducible Costimulator Ligand Regulates Bleomycin-Induced Lung and Skin Fibrosis in a Mouse Model Independently of the Inducible Costimulator/Inducible Costimulator Ligand Pathway.

Author

Tanaka, Chihiro, Fujimoto, Manabu, Hamaguchi, Yasuhito, Sato, Shinichi, Takehara, Kazuhiko, and Hasegawa, Minoru

Subjects

FIBROSIS, COLLAGEN diseases, BLEOMYCIN, TISSUES, SKIN diseases

Abstract

The article focuses on a study which assessed the roles of inducible costimulator (ICOS) and its ligand (ICOSL) in tissue fibrosis by administering bleomycin intratracheally or intradermaly into mice deficient in ICOS and ICOSL. It found that ICOS deficiency attenuated the lung and skin fibrosis, while ICOSL deficiency aggravated it. It concludes that ICOSL expression on antigen-presenting cells plays a previously unknown regulatory role during the development of bleomycin-induced tissue fibrosis that is independent of the ICOS/ICOSLl pathway.

Published

2010

12. Subtraction method for determination of N-terminal connective tissue growth factor.

Author

Miyazaki, Osamu, Kurashita, Syunsuke, Fukamachi, Isamu, Endo, Koki, Poh-Sing Ng, and Takehara, Kazuhiko

Subjects

CONNECTIVE tissue growth factor, FIBROSIS, BLOOD platelet activation, ENZYME-linked immunosorbent assay, GROWTH factors, MONOCLONAL antibodies

Abstract

Background: Connective tissue growth factor (CTGF) may be a potential marker of fibrosis. However, platelet-derived CTGF may be released into the plasma by platelet activation during or after blood collection, thereby interfering with accurate determination of the true plasma CTGF level. Plasma CTGF exists as the N-terminal CTGF fragment (N-fragment), composed of modules 1 and 2, whereas platelet CTGF exists as full-length CTGF (full-length), composed of modules 1-4. We perceived the need to develop a method for distinguishing between the N-fragment and full-length CTGF levels, so that the true plasma and serum CTGF (N-fragment) levels could be accurately determined. Methods: Full-length levels were determined by a sandwich enzyme-linked immunosorbent assay (ELISA) using two monoclonal antibodies recognizing modules 1 and 4, respectively (M1/4 ELISA). Total CTGF (full-length CTGF plus N-terminal CTGF) levels were determined by a sandwich ELISA using two monoclonal antibodies recognizing modules 1 and 2, respectively (M1/2 ELISA). N-terminal CTGF levels were determined by subtracting the full-length levels from the total CTGF levels. Results: Both the M1/2 and M1/4 ELISAs showed good analytical performance. When the CTGF levels of plasma and serum collected simultaneously from the same subject were compared, the N-fragment levels determined by the subtraction method were the same, in spite of the fact that full-length CTGF was present in the sample. Conclusion: N-fragment levels in plasma and serum can be accurately determined by this subtraction method, even if full-length CTGF in platelets is released during or after blood collection. [ABSTRACT FROM AUTHOR]

Published

2010

13. Identification of Myocardial Damage in Systemic Sclerosis: A Nuclear Cardiology Approach.

Author

Nakajima, Kenichi, Matsuo, Shinro, Hasegawa, Minoru, Kinuya, Seigo, and Takehara, Kazuhiko

Subjects

CARDIOMYOPATHIES, SYSTEMIC scleroderma, FIBROSIS, MICROCIRCULATION, ELECTROCARDIOGRAPHY, IODINE, PERFUSION, CARDIAC radionuclide imaging, REGULATION of blood circulation, DIAGNOSIS

Abstract

Myocardial involvement is an important prognostic factor in patients with systemic sclerosis, and early diagnosis and staging of the disease have been sought after. Since myocardial damage is characterized by connective tissue disease, including fibrosis and diffuse vascular lesions or microcirculation, nuclear myocardial perfusion imaging has been a promising option for evaluating myocardial damages in early stages. In addition to the conventional stress-rest perfusion imaging, the current use of quantitative electrocardiographic gated imaging has contributed to more precise evaluation of cardiac perfusion, ventricular wall motion, and diastolic function, all of which have enhanced diagnostic ability of evaluating myocardial dysfunction. Abnormal sympathetic imaging with Iodine-123 metaiodobenzylguanidine might be another option for identifying myocardial damage. This paper deals with approaches from nuclear cardiology to detect perfusion and functional abnormality as an early sign of myocardial involvement as well as possible prognostic values in patients with abnormal imaging results. The role of nuclear cardiology in the era of multiple imaging modalities is discussed. [ABSTRACT FROM AUTHOR]

Published

2010

14. The Transcriptional Cofactor Nab2 Is Induced by TGF-β and Suppresses Fibroblast Activation: Physiological Roles and Impaired Expression in Scleroderma.

Author

Bhattacharyya, Swati, Jun Wei, Melichian, Denisa S., Milbrandt, Jeffrey, Takehara, Kazuhiko, and Varga, John

Subjects

COLLAGEN, MYOFIBROBLASTS, GROWTH factors, FIBROSIS, FIBROBLASTS, ECTOPIC tissue, SKIN, BIOPSY, KERATINOCYTES

Abstract

By stimulating collagen synthesis and myofibroblasts differentiation, transforming growth factor-β (TGF- β) plays a pivotal role in tissue repair and fibrosis. The early growth response-1 (Egr-1) transcription factor mediates profibrotic TGF-β responses, and its expression is elevated in biopsies from patients with scleroderma. NGF1-A-binding protein 2 (Nab2) is a conserved transcriptional cofactor that directly binds to Egr-1 and positively or negatively modulates Egr-1 target gene transcription. Despite the recognized importance of Nab2 in governing the intensity of Egr-1-dependent responses, the regulation and function of Nab2 in the context of fibrotic TGF-β signaling is unknown. Here we show that TGF-β caused a time-dependent stimulation of Nab2 protein and mRNA in normal fibroblasts. Ectopic expression of Nab2 in these cells blocked Egr-1-dependent transcriptional responses, and abrogated TGF-β-induced stimulation of collagen synthesis and myofibroblasts differentiation. These inhibitory effects of Nab2 involved recruitment of the NuRD chromatin remodeling complex to the COL1A2 promoter and were accompanied by reduced histone H4 acetylation. Mice with targeted deletion of Nab2 displayed increased collagen accumulation in the dermis, and genetic or siRNA-mediated loss of Nab2 in fibroblasts was associated with constitutively elevated collagen synthesis and accentuation of Egr-1-dependent TGF-β responses in vitro. Expression of Nab2 was markedly up-regulated in skin biopsies from patients with scleroderma, and was localized primarily to epidermal keratinocytes. In contrast, little Nab2 could be detected in dermal fibroblasts. These results identify Nab2 as a novel endogenous negative regulator of Egr-1-dependent TGF-β signaling responsible for setting the intensity of fibrotic responses. Defective Nab2 expression or function in dermal fibroblasts might play a role in persistent fibrotic responses in scleroderma. [ABSTRACT FROM AUTHOR]

Published

2009

15. Role of connective tissue growth factor and its interaction with basic fibroblast growth factor and macrophage chemoattractant protein-1 in skin fibrosis.

Author

CHUJO, SONOKO, SHIRASAKI, FUMIAKI, KONDO-MIYAZAKI, MIKI, IKAWA, YUKA, and TAKEHARA, KAZUHIKO

Subjects

CONNECTIVE tissues, TISSUES, GROWTH factors, FIBROBLAST growth factors, FIBROSIS

Abstract

Activation of the immune system and abnormal growth of skin fibroblasts cause systemic sclerosis. Growth factors have various biological activities, including mediation of immune reactions. The growth factor family includes basic fibroblast growth factor (bFGF), transforming growth factor-beta (TGF-β), and connective tissue growth factor (CTGF). CTGF, an important downstream mediator of TGF-β in fibrosis, has been suggested to play a specific role in fibrotic disorders. We have directed our attention to the role of CTGF in sustaining skin fibrosis. To better understand its effects in vivo, we established an animal model of skin fibrosis induced by exogenous application of growth factors. In this model, bFGF transiently induced subcutaneous fibrosis. Simultaneous injection of bFGF and CTGF increased skin fibrosis compared with a single injection of bFGF. Serial injections of bFGF for 3 days followed by CTGF for 4 days, or of CTGF followed by bFGF, did not cause skin fibrosis but simultaneous injections increased macrophage chemoattractant protein-1 (MCP-1) mRNA expression levels. To further define the mechanisms of skin fibrosis in vivo, bFGF and CTGF were injected simultaneously into MCP-1 knockout mice, resulting in decreased collagen levels in granulation tissues on day 8. The number of inflammatory cells, such as mast cells, macrophages and lymphocytes, was significantly decreased in MCP-1 knockout mice compared with wild-type mice. These results suggest that bFGF induces collagen production by stimulating skin fibroblasts and CTGF cooperates with bFGF. Our results indicate that the induction of MCP-1 is necessary for infiltration of inflammatory cells. J. Cell. Physiol. 220: 189–195, 2009. © 2009 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2009

16. Neutralizing monoclonal antibody to human connective tissue growth factor ameliorates transforming growth factor-β-induced mouse fibrosis.

Author

Ikawa, Yuka, Poh-Sing Ng, Endo, Koki, Kondo, Miki, Chujo, Sonoko, Ishida, Wataru, Shirasaki, Fumiaki, Fujimoto, Manabu, and Takehara, Kazuhiko

Subjects

SYSTEMIC scleroderma, EXTRACELLULAR matrix, CONNECTIVE tissues, GROWTH factors, FIBROSIS, IMMUNOGLOBULINS

Abstract

Skin fibrotic disorders such as systemic sclerosis (SSc) are characterized by an excessive accumulation of extracellular matrix (ECM) and are understood to develop under the influence of fibrogenic growth factors. To better understand the detailed mechanisms of persistent fibrosis in SSc, we have previously established an animal model of skin fibrosis induced by exogenous application of growth factors. In this model, transforming growth factor-β (TGF-β) transiently induced subcutaneous fibrosis and serial injections of connective tissue growth factor (CTGF) after TGF-β caused persistent fibrosis. These results suggest that CTGF plays an important role in the development of persistent skin fibrosis and that CTGF may be a potential and specific therapeutic target in skin fibrosis. Therefore, the aim of the current study is to develop a neutralizing monoclonal antibody against human CTGF. We also investigated the neutralizing effect of the antibodies in our animal model. Firstly, by using the DNA immunization method, we developed a panel of anti-CTGF antibodies recognizing the native conformation of human CTGF. Next, to examine the anti-fibrosing effects of these antibodies, newborn B6 mice received subcutaneous injections of TGF-β for 3 days with either anti-CTGF neutralizing antibodies or control purified immunoglobulin. Anti-CTGF antibodies significantly reduced skin fibrosis and collagen contents compared with the control group. These results suggest that our anti-CTGF antibodies are capable of blocking the development of skin fibrosis at least partially and these anti-CTGF neutralizing antibodies may be useful as the feasible strategy to treat skin fibrotic diseases as SSc. J. Cell. Physiol. 216: 680–687, 2008, © 2008 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2008

17. The clinical characteristics of juvenile-onset systemic sclerosis in Japanese patients.

Author

Hatta, Yuri, Hasegawa, Minoru, Matsushita, Takashi, Hamaguchi, Yasuhito, Fujimoto, Manabu, and Takehara, Kazuhiko

Subjects

SYSTEMIC scleroderma, JAPANESE people, JUVENILE diseases, FIBROSIS, CONNECTIVE tissue diseases, PATIENTS, THERAPEUTICS, DISEASES

Published

2014

18. Novel Autoantibody to Cu/Zn Superoxide Dismutase in Patients with Localized Scleroderma.

Author

Nagai, Masaki, Hasegawa, Minoru, Takehara, Kazuhiko, and Sato, Shinichi

Subjects

*AUTOIMMUNITY, *FIBROMYALGIA, *REACTIVE oxygen species, *SUPEROXIDES, *SCLERODERMA (Disease), *AUTOANTIBODIES

Abstract

Abnormal production of reactive oxygen species (ROS) induces tissue damage and superoxide dismutase (SOD) that converts superoxide radicals to hydrogen peroxide functions as defense against ROS. Cu/Zn SOD administration has been shown to be effective for various fibrotic conditions by inhibiting the fibrogenic effects of ROS. We hypothesized that autoimmune background in localized scleroderma induced anti-Cu/Zn SOD autoantibodies that inhibited SOD activity and thereby contributed to fibrosis by increasing ROS. ELISA using human purified Cu/Zn SOD revealed that IgG or IgM anti-Cu/Zn SOD Ab was detected in the serum of 89% of localized scleroderma patients, especially 100% of patients with generalized morphea, the severest form of localized scleroderma, but was positive only in the serum of less than 15% of patients with other autoimmune disorders, including systemic sclerosis, systemic lupus erythematosus, dermatomyositis, and autoimmune bullous disorders. The immunoblotting analysis confirmed the presence of IgG anti-Cu/Zn SOD Ab in sera from localized scleroderma patients. Remarkably, anti-Cu/Zn SOD autoantibody could inhibit Cu/Zn SOD enzymatic activity. Collectively, these results indicate that anti-Cu/Zn SOD Ab is a novel, major autoantibody in localized scleroderma, and also suggest that the autoantibody may play a role in the development of fibrosis by directly inhibiting SOD activity. [ABSTRACT FROM AUTHOR]

Published

2004

19. A role for FcγRIIB in the development of murine bleomycin-induced fibrosis.

Author

Sawada, Kaori, Hamaguchi, Yasuhito, Mizumaki, Kie, Oishi, Kyosuke, Maeda, Shintaro, Ikawa, Yuka, Komuro, Akito, Takehara, Kazuhiko, and Matsushita, Takashi

Subjects

*FC receptors, *PULMONARY fibrosis, *THERAPEUTICS, *SYSTEMIC scleroderma, *ANTIGEN receptors

Abstract

• The loss of FcγRIIB exacerbated skin and lung fibrosis in bleomycin-induced fibrosis model. • FcγRIIB regulated leukocytes infiltration and cytokine and chemokine production. • Modulating FcγRIIB signaling has potential as a therapeutic approach for systemic sclerosis. Systemic sclerosis (SSc) is a systemic autoimmune disease characterized by excessive fibrosis. FcγRIIB is a low-affinity receptor for the Fc fragment of IgG. FcγRIIB is expressed on the surface of various leukocyte subsets and signals negative feedback pathways to down-regulate B-cell antigen receptor signaling. The aim of the present study was to investigate the role of FcγRIIB in the development of a murine bleomycin-induced scleroderma model. The experimental fibrosis model was generated by the intradermal injection of bleomycin into wild-type (WT) and FcγRIIB-deficient (FcγRIIB-/-) mice. We histologically assessed skin and lung fibrosis as well as inflammatory cell infiltration. Cytokine and chemokine expression levels were measured with RT-PCR. The severity of fibrosis in the skin and lung was significantly worse in FcγRIIB-/- mice than in WT mice. In the skin of bleomycin-treated mice, the numbers of CD8+ T cells, F4/80+ macrophages, MPO+ neutrophils, NK1.1+NK cells, and B220+ B cells were significantly higher in FcγRIIB-/- mice than in WT mice. The expression of TNF-α and IL-1β was significantly higher in FcγRIIB-/- mice than in WT mice as was the expression of ICAM-1, CXCL2, and CCL3 in the affected skin. An adoptive transfer of splenic leukocytes from FcγRIIB-/- mice into WT mice showed exacerbated skin and lung fibrosis compared to WT mice without an adoptive transfer. These results indicate that FcγRIIB plays an inhibitory role in skin and lung fibrosis. Moreover, modulating FcγRIIB signaling has potential as a therapeutic approach for SSc. [ABSTRACT FROM AUTHOR]

Published

2021

20. CD22 and CD72 contribute to the development of scleroderma in a murine model.

Author

Zhao, Chunyan, Matsushita, Takashi, Ha Nguyen, Vinh Thi, Tennichi, Momoko, Fujimoto, Manabu, Takehara, Kazuhiko, and Hamaguchi, Yasuhito

Subjects

*PULMONARY fibrosis, *SYSTEMIC scleroderma, *POLYMERASE chain reaction, *B cells, *T cells

Abstract

• The loss of CD22 and CD72 reduced skin and lung fibrosis in bleomycin- and hypochlorous acid-induced fibrosis model. • CD22 and CD72 regulated leukocytes infiltration and cytokine and chemokine production. • The inhibition of CD22 and CD72 function might be a therapeutic target for systemic sclerosis. Systemic sclerosis (SSc) is a systemic autoimmune disease that is characterized by excessive fibrosis. CD22 and CD72 are B cell-specific cell surface molecules that negatively regulate B cell function. The aim of the present study was to investigate the roles of CD22 and CD72 in a murine scleroderma model. The experimental fibrosis model was generated by subcutaneous injection of bleomycin or hypochlorous acid (HOCL) into wild-type (WT), CD22-deficient (CD22−/−), CD72-deficient (CD72−/−) and CD22 and CD72 double-deficient (CD22−/−/CD72−/−) mice. We histologically assessed skin fibrosis and inflammatory cell infiltration. Cytokine and chemokine expression levels were measured by real-time polymerase chain reaction. The severity of fibrosis in the skin and lung was significantly less in CD22−/−, CD72−/−, and CD22−/−/CD72−/− mice than in WT mice in the bleomycin-induced model. In the skin of bleomycin-treated mice, the numbers of CD3+ T cells, CD8+ T cells, and F4/80+ macrophages were significantly lower in CD22−/−, CD72−/−, and CD22−/−/CD72−/− mice than in WT mice. The expression levels of mRNAs for IL-6, TNF-α, TGF-β, CTGF, IL-1β, IL-13, CXCL2, and ICAM-1 were significantly lower in CD22−/−, CD72−/−, and CD22−/−/CD72−/− mice than in WT mice. In the HOCL-induced model, both skin and lung fibrosis were ameliorated in CD22−/−, CD72−/− and CD22−/−/CD72−/− mice compared to WT mice. These results indicate that CD22 and CD72 likely play crucial roles in skin and lung fibrosis. Moreover, the inhibition of CD22 and CD72 function has potential as a therapeutic approach to SSc. [ABSTRACT FROM AUTHOR]

Published

2020

21. Role of the Interleukin-1 Family in the Fibrogenic Phenotype in Systemic Sclerosis

Author

Kawaguchi, Yasushi, Takehara, Kazuhiko, editor, Fujimoto, Manabu, editor, and Kuwana, Masataka, editor

Published

2016

22. Autoimmunity in Systemic Sclerosis: Overview

Author

Yoshizaki, Ayumi, Sato, Shinichi, Takehara, Kazuhiko, editor, Fujimoto, Manabu, editor, and Kuwana, Masataka, editor

Published

2016

23. Biomarker

Author

Hasegawa, Minoru, Takehara, Kazuhiko, editor, Fujimoto, Manabu, editor, and Kuwana, Masataka, editor

Published

2016

24. CD19-dependent B lymphocyte signaling thresholds influence skin fibrosis and autoimmunity in the tight-skin mouse.

Author

Saito, Eriko, Fujimoto, Manabu, Hasegawa, Minoru, Komura, Kazuhiro, Hamaguchi, Yasuhito, Kaburagi, Yuko, Nagaoka, Tetsuya, Takehara, Kazuhiko, Tedder, Thomas F., and Sato, Shinichi

Subjects

*PHENOTYPES, *MICE physiology, *IMMUNOGLOBULINS, *AUTOANTIBODIES, *CALCIUM metabolism, *PROLINE metabolism, *TYROSINE metabolism, *ANIMAL experimentation, *ANTIGENS, *B cells, *BIOCHEMISTRY, *BIOLOGICAL models, *CELLULAR signal transduction, *DOSE-effect relationship in pharmacology, *ENZYME-linked immunosorbent assay, *FLOW cytometry, *GLYCOSIDASES, *INTERLEUKINS, *PHENOMENOLOGY, *MICE, *PHOSPHORYLATION, *RESEARCH funding, *SKIN, *SYSTEMIC scleroderma, *TIME, *WESTERN immunoblotting, *FIBROSIS, *MEMBRANE glycoproteins, *PRECIPITIN tests, *PHYSIOLOGY

Abstract

The tight-skin (TSK/+) mouse, a genetic model for human systemic sclerosis (SSc), develops cutaneous fibrosis and autoantibodies against SSc-specific target autoantigens. Although molecular mechanisms explaining the development of fibrosis and autoimmunity in SSc patients or TSK/+ mice remain unknown, we recently demonstrated that SSc patients overexpress CD19, an important regulatory molecule expressed by B lymphocytes. B cells from CD19-deficient mice are hyporesponsive to transmembrane signals, while B cells overexpressing CD19 are hyperresponsive and generate autoantibodies. In this study, TSK/+ B cells also exhibited a hyperresponsive phenotype with decreased surface IgM expression, enhanced serum Ig production, and spontaneous autoantibody production. Moreover, CD19 tyrosine phosphorylation was constitutively augmented in TSK/+ B cells. CD19-mediated [Ca(2+)](i) responses, Vav phosphorylation, and Lyn kinase activity were similarly enhanced. Studies of TSK/+ mice deficient in CD19 expression demonstrated that CD19 deficiency significantly decreased skin fibrosis in TSK/+ mice. Additionally, CD19 loss in TSK/+ mice upregulated surface IgM expression and completely abrogated hyper-gamma-globulinemia and autoantibody production. CD19 deficiency also inhibited IL-6 production by TSK/+ B cells. Thus, chronic B cell activation resulting from augmented CD19 signaling in TSK/+ mice leads to skin sclerosis possibly through IL-6 overproduction as well as autoimmunity. [ABSTRACT FROM AUTHOR]

Published

2002

25. The inhibitor of p38 MAP kinase suppresses skin fibrosis in the sclerodermatous chronic GVHD.

Author

Date, Mutsumi, Matsushita, Takashi, Hamaguchi, Yasuhito, and Takehara, Kazuhiko

Subjects

*GRAFT versus host disease, *MITOGEN-activated protein kinases, *FIBROSIS, *SCLERODERMA (Disease), *KINASE inhibitors

Published

2016