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Featured researches published by Shigeki Miyawaki.


Journal of Immunology | 2000

Increased Frequency of Surface IgA-Positive Plasma Cells in the Intestinal Lamina Propria and Decreased IgA Excretion in Hyper IgA (HIGA) Mice, a Murine Model of IgA Nephropathy with Hyperserum IgA

Tadashi Kamata; Fumiaki Nogaki; Sidonia Fagarasan; Toshio Sakiyama; Ikei Kobayashi; Shigeki Miyawaki; Koichi Ikuta; Eri Muso; Haruyoshi Yoshida; Shigetake Sasayama; Tasuku Honjo

Because abnormalities of mucosal immunity have been suggested in human IgA nephropathy, we examined the involvement of mucosal immunity in IgA deposition to the kidney in hyper IgA (HIGA) mice, which was established as a mouse model for human IgA nephropathy with hyperserum IgA. The number of surface IgA+B220− lymphocytes in the intestinal lamina propria (LP) of HIGA mice increased 2.7-fold at 30 wk of age as compared with those at 10 wk of age, whereas normal mice did not show such increase. The surface IgA+B220− LP lymphocytes spontaneously secreted IgA in culture. Morphological studies showed that the surface IgA+B220− lymphocytes of murine intestinal LP are identical with plasma cells (PCs). About 20% of IgA+B220− PC in LP expressed both Mac-1 and CD19, suggesting that they may derive from peritoneal B-1 cells. Cell cycle study on intestinal IgA-PCs using bromodeoxyuridine revealed no difference between HIGA mice and normal mice, suggesting that the high frequency of IgA-producing PCs in HIGA mice is not due to enhanced proliferation or prolonged survival of IgA-producing PCs in LP. In addition, IgA secretion into the gut lumen of HIGA mice decreased drastically (to one forth) with aging. These data suggest that the increased number of intestinal IgA-producing PCs and the down-regulation of IgA excretion into the intestinal lumen might synergistically contribute to the hyperserum IgA in HIGA mice and resultant IgA deposition to the kidney.


Nephron | 2002

Heminephrectomy Causes the Progression of Glomerulosclerosis and Apoptosis in High IgA Strain ddY Mice

Hitoshi Kusano; Eri Muso; Takahiko Ono; Fumiaki Nogaki; Keiko Nomura; Toshiya Takeda; Shigeki Miyawaki; Akira Matsumori; Haruyoshi Yoshida; Shigetake Sasayama

Background: The reduction in nephrons in IgA nephropathy is critical to the prognosis of this disease. However, the immunopathological mechanism of the modifications seen in glomerular lesions is not clear. We thus investigated the influence of nephron reduction by heminephrectomy on renal lesions in a high immunoglobulin A inbred strain of ddY mouse (HIGA mouse), which shows progressive mesangial sclerosis with elevated renal expression of transforming growth factor (TGF)-β. Methods: Five-week-old HIGA mice were heminephrectomized (Nx), and were evaluated in comparison with a sham-operated group (S) at 40 weeks old. Histological findings, immunoglobulin depositions (IgG, IgA, and IgM), and expressions of cytokine and extracellular matrix proteins (TGF-β, fibronectin, collagen type I and IV) were analysed. PCNA and TUNEL stainings were performed with electron microscopic detection of apoptosis. Tissue renin-angiotensin systems (RAS) were also investigated by real-time quantitative RT-PCR. Results: In the Nx group, the glomerular tuft area and ratio of mesangial matrix area per tuft were significantly increased, and the glomerular cell count per tuft area was significantly decreased. Glomerular immunoglobulin deposits of IgG, IgA, and IgM in Nx were all significantly expanded in the paramesangium. The glomerular expressions of TGF-β and the extracellular matrix proteins were significantly increased in Nx mice. In contrast to the significant decrease of PCNA-positive cells, TUNEL-positive cells were significantly increased in Nx. Angiotensin-converting enzyme (ACE) was significantly increased in the renal cortex of Nx. Conclusion: Simple heminephrectomy, other than 5/6 renal ablation, of HIGA mice may be a potential model for research into the progressive glomerulosclerosis of human IgA nephropathy. The pathological role of apoptosis is apparently involved in these disease processes, possibly through upregulated RAS.


European Journal of Immunology | 2004

Quantitative trait loci (QTL) analysis reveals a close linkage between the hinge region and trimeric IgA dominancy in a high IgA strain (HIGA) of ddY mice

Emi Oida; Fumiaki Nogaki; Ikei Kobayashi; Tadashi Kamata; Takahiko Ono; Shigeki Miyawaki; Tadao Serikawa; Haruyoshi Yoshida; Toru Kita; Eri Muso

Polymerization of IgA has been suggested as one of the causes of mesangial deposition in IgA nephropathy. HIGA mice are an inbred model of IgA nephropathy, established by selective mating of ddY mice. This strain is characterized by a unique profile of the IgA molecule that is dominantly polymeric and has high serum levels with intense IgA deposition on the mesangium. We carried out quantitative trait loci (QTL) analysis, using F2 generations by crossing HIGA with BALB/c mice. Significant linkage of polymeric IgA in serum samples was identified around D12Mit263, which is close to the gene of the immunoglobulin heavy chain on chromosome 12. The amino acid sequence of the α heavy chain revealed marked differences between BALB/c and HIGA mice. Furthermore, most differences were focussed on the hinge region. The DBA/2J strain, which has the same amino acid sequence in the hinge region as the HIGA strain, also showed polymeric IgA dominance but low IgA levels in sera. Size fraction analysis revealed that these polymeric IgA showed trimer dominance in both DBA/2J and HIGA mice. In conclusion, the hinge region plays a key role in trimeric IgA formation in HIGA mice.


Nephron | 1999

Ultrastructural Localization of Dominantly Increased Fibronectin in the Markedly Thickened Glomerular Basement Membrane in a Selectively Mated Murine High IgA Strain (HIGA Mice)

Takahide Kawamura; Eri Muso; Tadashi Kamata; Katsuo Suyama; Atsushi Oyama; Takahiko Ono; Haruyoshi Yoshida; Shigeki Miyawaki; Shigetake Sasayama

To clarify which matrix component(s) contributes to glomerular sclerosis with mesangial IgA deposits in a murine high serum IgA strain (HIGA) derived from ddY mice, morphological and immunopathological analyses of glomeruli were performed in comparison with original ddY and BALB/c mice as controls. Significantly increased thickness of the glomerular basement membrane (GBM), especially the lamina densa, was observed in HIGA mice. Immunofluorescent staining showed marked increases in levels of fibronectin and laminin in both the mesangium and capillary wall in aged HIGA mice. Analysis of the distribution of immunogold-labeled antibody in GBM revealed a significant increase (p < 0.0001) and specific orientation of fibronectin in the endothelial side, which suggested that mesangial fibronectin produced at high levels due to IgA deposition extended to the endothelial side of GBM and contributed to the thickening of GBM with further development to glomerulosclerosis in the HIGA mice.


Nephron | 2001

Up-Regulated TGF-β mRNA Expression in Splenic T Cells of High IgA-Prone Mice: A Murine Model of IgA Nephropathy with Glomerulosclerosis

Atsushi Oyama; Eri Muso; Takahiko Ono; Hiroyuki Matsushima; Masatomo Yashiro; Katsuo Suyama; Tadashi Kamata; Fumiaki Nogaki; Ikei Kobayashi; Shigeki Miyawaki; Haruyoshi Yoshida; Shigetake Sasayama

Background/Aims: Recently, we established a high serum IgA-prone inbred (HIGA) mouse strain as a murine model of spontaneous IgA nephropathy by selective mating of high serum IgA ddY mice, and found that they showed enhanced production of glomerular extracellular matrix components with increased expression of TGF-β mRNA and protein in the kidneys. In this study, we examined the roles of lymphocytes in the development of high serum IgA in this strain. Methods: We performed flow cytometric analyses of T and B cells in splenic mononuclear cells (SMNCs) from these mice using BALB/c mice as normal controls. We also compared serum TGF-β1 concentrations and TGF-β mRNA expression levels in the B-cell-depleted (T-cell-rich) fraction of SMNCs in these mice. Results: HIGA mice showed significantly fewer CD3-positive cells compared with BALB/c mice when young, but not when aged. The CD4/CD8 ratio of HIGA mice was lower than that of BALB/c mice, but this difference was not significant. Although the number of B220-positive cells did not vary significantly, the ratio of surface IgA-positive B cells was significantly increased in both young and adult HIGA mice. The B-cell-depleted SMNCs from HIGA mice exhibited higher levels of expression of TGF-β and TGF-β1 mRNA than controls from a young age, which were maintained throughout life, but there were no differences in PDGF, MCP-1 or bFGF expression between these two strains. In contrast to local mRNA expression, serum TGF-β1 concentration was decreased in HIGA mice compared with BALB/c controls. Conclusion: These findings suggest that the mating procedure performed to establish HIGA mice selected for a unique phenotype of local up-regulation of TGF-β production in the kidneys, as well as T cells that may contribute to both the early and consistently high serum IgA expression and enhanced production of renal extracellular matrix components in HIGA mice. Additionally, TGF-β1 may act locally, not systemically, in a paracrine or autocrine manner.


European Journal of Immunology | 1996

Autoimmune disease of exocrine organs in immunodeficient alymphoplasia mice: a spontaneous model for Sjören's syndrome

Rieko Tsubata; Takeshi Tsubata; Hiroshi Hiai; Reiko Shinkura; Ryutaro Matsumura; Takayuki Sumida; Shigeki Miyawaki; Hiroshi Ishida; Shunichi Kumagai; Kazuwa Nakao; Tasuku Honjo


Kidney International | 1999

Bone marrow transplantation attenuates murine IgA nephropathy: Role of a stem cell disorder1

Toshiyuki Imasawa; Ryuji Nagasawa; Yasunori Utsunomiya; Tetsuya Kawamura; Yu Zhong; Noriko Makita; Eri Muso; Shigeki Miyawaki; Naoki Maruyama; Tatsuo Hosoya; Osamu Sakai; Tsuneya Ohno


Kidney International | 1996

Enhanced production of glomerular extracellular matrix in a new mouse strain of high serum IgA ddY mice

Eri Muso; Haruyoshi Yoshida; Eiji Takeuchi; Masatomo Yashiro; Hiroyuki Matsushima; Atsushi Oyama; Katsuo Suyama; Takahide Kawamura; Tadashi Kamata; Shigeki Miyawaki; Shozo Izui; Shigetake Sasayama


Nephron | 1997

Selective Breeding for High Serum IgA Levels from Noninbred ddY Mice: Isolation of a Strain with an Early Onset of Glomerular IgA Deposition

Shigeki Miyawaki; Eri Muso; Eiji Takeuchi; Hiroyuki Matsushima; Yoshihisa Shibata; Shigetake Sasayama; Haruyoshi Yoshida


Nephrology Dialysis Transplantation | 2002

Interleukin‐12 alters the physicochemical characteristics of serum and glomerular IgA and modifies glycosylation in a ddY mouse strain having high IgA levels

Ikei Kobayashi; Fumiaki Nogaki; Hitoshi Kusano; Takahiko Ono; Shigeki Miyawaki; Haruyoshi Yoshida; Eri Muso

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