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477 results on '"Kita, Hiroto"'

1. Identification of HLA-A2–restricted CD8+ Cytotoxic T Cell Responses in Primary Biliary Cirrhosis

Author

Kita, Hiroto, Lian, Zhe-Xiong, Van de Water, Judy, He, Xiao-Song, Matsumura, Shuji, Kaplan, Marshall, Luketic, Velimir, Coppel, Ross L, Ansari, Aftab A, and Gershwin, M Eric

Subjects
Biomedical and Clinical Sciences, Immunology, Clinical Research, Immunization, Autoimmune Disease, Chronic Liver Disease and Cirrhosis, Digestive Diseases, Liver Disease, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Antigen Presentation, Antigen-Antibody Complex, Autoimmunity, Cytokines, Dendritic Cells, Dihydrolipoyllysine-Residue Acetyltransferase, Epitopes, HLA-A2 Antigen, Humans, Lymphocyte Activation, Oligopeptides, Pyruvate Dehydrogenase Complex, T-Lymphocytes, Cytotoxic, autoimmunity, cytotoxic T cells, cholangitis, epitopes, cross-priming, Medical and Health Sciences, Biomedical and clinical sciences, Health sciences
Abstract

Primary biliary cirrhosis (PBC) is characterized by an intense biliary inflammatory CD4(+) and CD8(+) T cell response. Very limited information on autoantigen-specific cytotoxic T lymphocyte (CTL) responses is available compared with autoreactive CD4(+) T cell responses. Using peripheral blood mononuclear cells (PBMCs) from PBC, we identified an HLA-A2-restricted CTL epitope of the E2 component of pyruvate dehydrogenase (PDC-E2), the immunodominant mitochondrial autoantigen. This peptide, amino acids 159-167 of PDC-E2, induces specific MHC class I-restricted CD8(+) CTL lines from 10/12 HLA-A2(+) PBC patients, but not controls, after in vitro stimulation with antigen-pulsed dendritic cells (DCs). PDC-E2-specific CTLs could also be generated by pulsing DCs with full-length recombinant PDC-E2 protein. Furthermore, using soluble PDC-E2 complexed with either PDC-E2-specific human monoclonal antibody or affinity-purified autoantibodies against PDC-E2, the generation of PDC-E2-specific CTLs, occurred at 100-fold and 10-fold less concentration, respectively, compared with soluble antigen alone. Collectively, these data demonstrate that autoantibody, helper, and CTL epitopes all contain a shared peptide sequence. The finding that autoantigen-immune complexes can not only cross-present but also that presentation of the autoantigen is of a higher relative efficiency, for the first time defines a unique role for autoantibodies in the pathogenesis of an autoimmune disease.

Published
2002

14. Cyclooxygenase-2 is required for activated pancreatic stellate cells to respond to proinflammatory cytokines

Author

Aoki, Hiroyoshi, Ohnishi, Hirohide, Hama, Kouji, Shinozaki, Satoshi, Kita, Hiroto, Osawa, Hiroyuki, Yamamoto, Hironori, Sato, Kiichi, Tamada, Kiichi, and Sugano, Kentaro

Subjects
COX-2 inhibitors -- Research, Cyclooxygenases -- Research, Biological sciences
Abstract

Cyclooxygenase-2 (COX-2) mediates various inflammatory responses and is expressed in pancreatic tissue from patients with chronic pancreatitis. To examine the role of COX-2 in chronic pancreatitis, we investigated its participation in regulating functions of pancreatic stellate cells (PSCs), using isolated rat PSCs. COX-2 was expressed in culture-activated PSCs but not in freshly isolated quiescent PSCs. TGF-[beta]1, IL-1[beta], and IL-6 enhanced COX-2 expression in activated PSCs, concomitantly increasing the expression of [alpha]-smooth muscle actin ([alpha]-SMA), a parameter of PSC activation. The COX-2 inhibitor NS-398 blocked culture activation of freshly isolated quiescent PSCs. NS-398 also inhibited the enhancement of [alpha]-SMA expression by TGF-[beta]1, IL-1[beta], and IL-6 in activated PSCs. These data indicate that COX-2 is required for the initiation and promotion of PSC activation. We further investigated the mechanism by which cytokines enhance COX-2 expression in PSCs. Adenovirus-mediated expression of dominant negative Smad2/3 inhibited the increase in expression of COX-2, [alpha]-SMA, and collagen-1 mediated by TGF-[beta]1 in activated PSCs. Moreover, dominant negative Smad2/3 expression attenuated the expression of COX-2 and [alpha]-SMA enhanced by IL-1[beta] and IL-6. Anti-TGF-[beta] neutralizing antibody also attenuated the increase in COX-2 and [alpha]-SMA expression caused by IL-l[beta] and IL-6. IL-6 as well as IL-l[beta] enhanced TGF-[beta]1 secretion from PSCs. These data indicate that Smad2/3-dependent pathway plays a central role in COX-2 induction by TGF-[beta]1, IL-1[beta], and IL-6. Furthermore, IL-1[beta] and IL-6 promote PSC activation by enhancing COX-2 expression indirectly through Smad2/3-dependent pathway by increasing TGF-[beta]1 secretion from PSCs. transforming growth factor-[beta]; interleukin; Smad; autocrine; pancreatic fibrosis

Published
2007

17. Autocrine loop between TGF-[[beta].sub.1] and IL-1[beta] through Smad3- and ERK-dependent pathways in rat pancreatic stellate cells

Author

Aoki, Hiroyoshi, Ohnishi, Hirohide, Hama, Kouji, Ishijima, Takako, Satoh, Yukihiro, Hanatsuka, Kazunobu, Ohashi, Akira, Wada, Shinichi, Miyata, Tomohiko, Kita, Hiroto, Yamamoto, Hironori, Osawa, Hiroyuki, Sato, Kiichi, Tamada, Kiichi, Yasuda, Hiroshi, Mashima, Hirosato, and Sugano, Kentaro

Subjects
Fibrosis -- Research, Cytokines -- Research, Cytokines -- Analysis, Pancreatitis -- Research, Pancreatitis -- Analysis, Pancreatitis -- Care and treatment, Biological sciences
Abstract

Pancreatic stellate cells (PSCs) are activated during pancreatitis and promote pancreatic fibrosis by producing and secreting ECMs such as collagen and fibronectin. IL-1[beta] has been assumed to participate in pancreatic fibrosis by activating PSCs. Activated PSCs secrete various cytokines that regulate PSC function. In this study, we have examined IL-1[beta] secretion from culture-activated PSCs as well as its regulatory mechanism. RT-PCR and ELISA have demonstrated that PSCs express IL-1[beta] mRNA and secrete IL-1[beta] peptide. Inhibition of TGF-1[beta] activity secreted from PSCs by TGF-[[beta].sub.1]-neutralizing antibody attenuated IL-1[beta] secretion from PSCs. Exogenous TGF-1[beta] increased IL-1[beta] expression and secretion by PSCs in a dose-dependent manner. Adenovirus-mediated expression of dominant-negative (dn)Smad2/3 expression reduced both basal and TGF-[[beta].sub.1]stimulated IL-1[beta] expression and secretion by PSCs. Coexpression of Smad3 with dnSmad2/3 restored IL-1[beta] expression and secretion by PSCs, which were attenuated by dnSmad2/3 expression. In contrast, coexpression of Smad2 with dnSmad2/3 did not alter them. Furthermore, inhibition of IL-1[beta] activity secreted from PSCs by IL-1[beta]-neutralizing antibody attenuated TGF-[[beta].sub.1] secretion from PSCs. Exogenous IL-1[beta] enhanced TGF-[[beta].sub.1] expression and secretion by PSCs. IL-1[beta] activated ERK, and PD-98059, a MEK1 inhibitor, blocked IL-1[beta] enhancement of TGF-[[beta].sub.1] expression and secretion by PSCs. We propose that an autocrine loop exists between TGF-[[beta].sub.1] and IL-1[beta] in activated PSCs through Smad3- and ERK-dependent pathways. fibrosis; cytokine; chronic pancreatitis

Published
2006

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