Yasuko Morimoto
Kobe Gakuin University
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Publication
Featured researches published by Yasuko Morimoto.
Journal of Pharmacy and Pharmacology | 2017
Shinichi Harada; Kei Miyagi; Tokio Obata; Yasuko Morimoto; Kazuo Nakamoto; Ke Ih Kim; Soo Ki Kim; Soo Ryang Kim; Shogo Tokuyama
A non‐alcoholic fatty liver disease (NAFLD) has high prevalence and now important issue of public health. In general, there exists strong interaction between NAFLD and diabetes, but the detailed mechanism is unclear. In this study, we determined the effects of hyperglycemia on progression in the early phase of NAFLD in mice.
European Journal of Pharmacology | 2018
Kazuo Nakamoto; Koki Shimada; Shinichi Harada; Yasuko Morimoto; Akira Hirasawa; Shogo Tokuyama
ABSTRACT Nonalcoholic steatohepatitis (NASH) is one of the most common liver diseases involving chronic accumulation of fat and inflammation, often leading to advanced fibrosis, cirrhosis and carcinoma. However, the pathological mechanism for this is unknown. GPR120/FFAR4 has been recognized as a functional fatty acid receptor and an attractive therapeutic target for metabolic diseases. In this study, we investigated the involvement of GPR120/FFAR4 in the pathogenesis of NASH. Mice fed with a 0.1% methionine and choline deficient high‐fat (CDAHF) diet showed a significant increase in plasma aspartate transaminase and alanine transaminase levels, fatty deposition, inflammatory cell infiltration, and mild fibrosis. Docosahexaenoic acid (DHA, GPR120/FFAR4 agonist) suppressed the inflammatory cytokines in the liver tissues and prevented fibrosis in the wild type (WT) mice fed CDAHF diet, but not GPR120/FFAR4 deficient (GPR120KO) mice. GPR120KO mice fed CDAHF diet showed increment of the number of crown like structures and the immunoreactivity for F4/80 positive cells, and increased TNF‐&agr; mRNA in the liver compared to WT mice fed CDAHF diet. GPR120 KO mice fed CDAHF diet showed more severe liver inflammation than that of WT mice fed CDAHF diet, but not fibrosis. Our findings suggest that DHA supplementation could be prevented the development of NASH via GPR120/FFAR4 signaling. Furthermore, decrease of GPR120/FFAR4 signaling could be facilitated an inflammatory response in the process of NASH progression.
Biological & Pharmaceutical Bulletin | 1995
Yasuko Morimoto; Kaori Tanaka; Yoko Iwakiri; Sumika Tokuhiro; Shoji Fukushima; Yoshikazu Takeuchi
Chemical & Pharmaceutical Bulletin | 1992
Yoshikazu Takeuchi; Hidehito Yasukawa; Yumiko Yamaoka; Yuichi Kato; Yasuko Morimoto; Yoshinobu Fukumori; Tomoaki Fukuda
Biological & Pharmaceutical Bulletin | 1995
Yoshikazu Takeuchi; Hidehito Yasukawa; Yumiko Yamaoka; Kenji Taguchi; Shoji Fukushima; Yasuhiro Shimonaka; Hiroko Nishinaga; Yasuko Morimoto
Chemical & Pharmaceutical Bulletin | 1992
Yoshikazu Takeuchi; Hidehito Yasukawa; Yumiko Yamaoka; Yasuko Morimoto; Satoshi Nakao; Yoshinobu Fukumori; Tomoaki Fukuda
Journal of Pharmaceutical Sciences | 1989
Yoshikazu Takeuchi; Yumiko Yamaoka; Yasuko Morimoto; Ikue Kaneko; Yoshinobu Fukumori; Tomoaki Fukuda
Biological & Pharmaceutical Bulletin | 1995
Yasuko Morimoto; Yuichiro Yutani; Yoshiko Kado; Tamaki Iida; Megumi Shiota; Yoshikazu Takeuchi
Chemical & Pharmaceutical Bulletin | 1994
Yasuko Morimoto; Yoshikazu Takeuchi
Chemical & Pharmaceutical Bulletin | 1994
Yasuko Morimoto; Mikio Hosokawa; Hiroteru Sayo; Yoshikazu Takeuchi
