CVClient

村上 明

ムラカミ アキラ  (Akira Murakami)

基本情報

所属
兵庫県立大学 環境人間学部 教授
学位
博士(農学)

研究者番号
10271412
ORCID ID
 https://orcid.org/0000-0002-5694-2828
J-GLOBAL ID
200901091245390193
researchmap会員ID
5000027763

外部リンク

詳細については以下を参照してください。
https://sftnetts.jimdo.com/myself/


論文

 301
  • Ishisaka A, Fujiwara N, Mukai R, Nishikawa M, Ikushiro S, Murakami A
    Bioscience, Biotechnology, and Biochemistry. 2024年  査読有り招待有り
  • Akira Murakami
    Biosci. Biotechnol. Biochem. 2024年  査読有り筆頭著者責任著者
  • Akari Ishisaka, Ryosuke Sugimoto, Haruka Marumo, Tomoki Doi, Kaede Hamada, Misa Fujimoto, Nao Fujiwara, Masao Yamasaki, Akira Murakami
    Mol Nutr Food Res 2023年8月  査読有り責任著者
  • Nao Fujiwara, Rie Mukai, Miyu Nishikawa, Shinichi Ikushiro, Akira Murakami, Akari Ishisaka
    Bioscience, Biotechnology, and Biochemistry 87(4) 442-447 2023年1月20日  査読有り
    ABSTRACT This is the first study that quantified quercetin (QUE) and its 16 metabolites in the breast milk of QUE-fed maternal mice, the plasma and urine of that, and neonatal mice. Interestingly, the QUE aglycone concentration in the milk was much higher than in the plasma of maternal mice, suggesting that QUE may exert biological activity in neonates.
  • Yoichi Sunagawa, Shogo Kawaguchi, Yusuke Miyazaki, Yasufumi Katanasaka, Masafumi Funamoto, Kana Shimizu, Satoshi Shimizu, Hidetoshi Hamabe-Horiike, Maki Komiyama, Kiyoshi Mori, Akira Murakami, Koji Hasegawa, Tatsuya Morimoto
    Phytomedicine 107 154457-154457 2022年10月  査読有り
    BACKGROUND: Auraptene derived from the peel of Citrus hassaku possesses anti-tumor, anti-inflammatory, and neuroprotective activities. Thus, it could be a valuable pharmacological alternative to treat some diseases. However, the therapeutic value of auraptene for heart failure (HF) is unknown. STUDY DESIGN/METHODS: In cultured cardiomyocytes from neonatal rats, the effect of auraptene on phenylephrine-induced hypertrophic responses and peroxisome proliferator-activated receptor-alpha (PPARα)-dependent gene transcriptions. To investigate whether auraptene prevents the development of heart failure after myocardial infarction (MI) in vivo, Sprague-Dawley rats with moderate MI (fractional shortening < 40%) were randomly assigned for treatment with low- or high-dose auraptene (5 or 50 mg/kg/day, respectively) or vehicle for 6 weeks. The effects of auraptene were evaluated by echocardiography, histological analysis, and the measurement of mRNA levels of hypertrophy, fibrosis, and PPARα-associated genes. RESULTS: In cultured cardiomyocytes, auraptene repressed phenylephrine-induced hypertrophic responses, such as increases in cell size and activities of atrial natriuretic factor and endothelin-1 promoters. Auraptene induced PPARα-dependent gene activation by enhancing cardiomyocyte peroxisome proliferator-responsive element reporter activity. The inhibition of PPARα abrogated the protective effect of auraptene on phenylephrine-induced hypertrophic responses. In rats with MI, auraptene significantly improved MI-induced systolic dysfunction and increased posterior wall thickness compared to the vehicle. Auraptene treatment also suppressed MI-induced increases in myocardial cell diameter, perivascular fibrosis, and expression of hypertrophy and fibrosis response markers at the mRNA level compared with vehicle treatment. MI-induced decreases in the expression of PPARα-dependent genes were improved by auraptene treatment. CONCLUSIONS: Auraptene has beneficial effects on MI-induced cardiac hypertrophy and left ventricular systolic dysfunction in rats, at least partly due to PPARα activation. Further clinical studies are required to evaluate the efficacy of auraptene in patients with HF.

MISC

 83

書籍等出版物

 162

講演・口頭発表等

 78

担当経験のある科目(授業)

 37

共同研究・競争的資金等の研究課題

 21

産業財産権

 6

社会貢献活動

 1