Yoshifusa Aizawa
Kitasato University
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Featured researches published by Yoshifusa Aizawa.
Circulation Research | 1998
Haruo Hanawa; Takayuki Inomata; Yuji Okura; Satoru Hirono; Yusuke Ogawa; Tohru Izumi; Makoto Kodama; Yoshifusa Aizawa
Experimental autoimmune myocarditis (EAM) resembles the giant cell myocarditis seen in humans, and recurrent forms lead to dilated cardiomyopathy. EAM has been shown to be a T cell-mediated autoimmune myocarditis. We have previously shown that cDNA encoding Vbeta complementarity-determining region (CDR) 3 from heart- and pericardial space-infiltrating T cells in EAM induced by rod cardiac myosin contains more restricted sequences than that from normal spleen T cells. Recently, it has become apparent that several epitopes of EAM exist in rod cardiac myosin; therefore, T cells infiltrating into lesions may recognize certain epitopes in EAM induced by rod cardiac myosin. In this study, we examined heart- and pericardial space-infiltrating T-cell clonotypes in EAM induced by synthetic peptides of cardiac myosin. EAM was produced by immunization with synthetic peptides corresponding to N-terminally acetylated amino acids 1539 to 1555 of rat cardiac myosin alpha heavy chain. Five of 12 rats receiving synthetic peptides developed macroscopic signs of myocarditis. To examine T-cell receptor (TCR) Vbeta expression and CDR3 of the TCR beta chain of lesion-infiltrating T cells in EAM, total RNA was isolated from heart, pericardial effusion, spleen, lymph node, and peripheral blood. TCR Vbeta expression of the T cells infiltrating the lesions revealed a predominance of Vbeta4. On the basis of single-strand conformation polymorphism analysis for CDR3 of the TCR Vbeta4 chain, heart- and pericardial space-infiltrating T cells were considered to be oligoclonal, whereas spleen, lymph node, and peripheral blood in a rat with EAM and spleen in a native rat were considered to be polyclonal. In the same rat, clonotypes of heart-infiltrating T cells were almost the same as those of pericardial space-infiltrating T cells. Furthermore, on sequence analysis for CDR3 of the TCR Vbeta4 chain, the amino acid motifs were similar among T cells infiltrating into lesions of different EAM rats. In the present study, TCR beta chains of heart- and pericardial space-infiltrating T cells in EAM induced by synthesized peptide consisting of 17 amino acids were examined. Vbeta4+ T cells with similar Vbeta CDR3 motifs that infiltrate the heart and pericardial space may recognize the same epitope.
Shinzo | 1990
Akihiro Obata; Yoshifusa Aizawa; Shinichi Niwano; Masahito Satoh; Akira Shibata
/data/revues/00029149/v83i5/S000291499800976X/ | 2011
Hiroshi Furushima; Shinichi Niwano; Masaomi Chinushi; Masayuki Yamaura; Koji Taneda; Takashi Washizuka; Yoshifusa Aizawa
Archive | 2010
Shinpei Kimura; Wataru Mitsuma; Masahiro Ito; Hiromi Suzuki; Yukio Hosaka; Satoshi Hirayama; Osamu Hanyu; Satoru Hirono; Makoto Kodama; Yoshifusa Aizawa
Archive | 2009
Ken Toba; 健 鳥羽; Kiminori Kato; 公則 加藤; Haruo Hanawa; 晴雄 塙; Yoshifusa Aizawa; 義房 相澤; Masato Higuchi; 樋口 正人
Archive | 2009
Wataru Mitsuma; Masahiro Ito; Satoru Fujita; Akinori Sato; Takashi Washizuka; Makoto Kodama; Yoshifusa Aizawa
新潟医学会雑誌 | 2008
誠 小玉; 孔明 田中; 正洋 伊藤; 義房 相澤; Makoto Kodama; Komei Tanaka; Masahiro Ito; Yoshifusa Aizawa
Archive | 2008
Yuji Okura; Mahmoud M. Ramadan; Yukiko Ohno; Wataru Mitsuma; Komei Tanaka; Masahiro Ito; Keisuke Suzuki; Naohito Tanabe; Makoto Kodama; Yoshifusa Aizawa
Archive | 2008
Hiroshi Watanabe; Makoto Kodama; Naohito Tanabe; Yuichi Nakamura; Tsuneo Nagai; Masahito Sato; Masaaki Okabe; Yoshifusa Aizawa
Acta medica et biologica | 2007
Makoto Kodama; Mahmoud M. Ramadan; Wataru Mitsuma; Komei Tanaka; Makoto Hoyano; Shiro Minagawa; Takeshi Kashimura; Masahiro Ito; Koichi Fuse; Satoru Hirono; Yoshifusa Aizawa; Osamu Namura; Masakazu Sogawa; Jun-ichi Hayashi