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Tadakiyo Nakagawa

Ajinomoto

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International Journal of Molecular Medicine | 2017

AJS1669, a novel small-molecule muscle glycogen synthase activator, improves glucose metabolism and reduces body fat mass in mice

Kazuhiro Nakano; Sen Takeshita; Noriko Kawasaki; Wataru Miyanaga; Yoriko Okamatsu; Mizuki Dohi; Tadakiyo Nakagawa

Impaired glycogen synthesis and turnover are common in insulin resistance and type 2 diabetes. As glycogen synthase (GS) is a key enzyme involved in the synthetic process, it presents a promising therapeutic target for the treatment of type 2 diabetes. In the present study, we identified a novel, potent and orally available GS activator AJS1669 {sodium 2-[[5-[[4-(4,5-difluoro-2-methylsulfanyl-phenyl) phenoxy] methyl]furan-2-carbonyl]-(2-furylmethyl)amino] acetate}. In vitro, we performed a glycogen synthase 1 (GYS1) activation assay for screening GS activators and identified that the activity of AJS1669 was further potentiated in the presence of glucose-6-phosphate (G6P). In vivo, we used ob/ob mice to evaluate the novel anti-diabetic effects of AJS1669 by measuring basal blood glucose levels, glucose tolerance and body fat mass index. Repeated administration of AJS1669 over 4 weeks reduced blood glucose and hemoglobin A1c (HbA1c) levels in ob/ob mice. AJS1669 also improved glucose tolerance in a dose-dependent manner, and decreased body fat mass. The mRNA levels of genes involved in mitochondrial fatty acid oxidation and mitochondrial biogenesis were elevated in skeletal muscle tissue following AJS1669 treatment. Hepatic tissue of treated mice also exhibited elevated expression of genes associated with fatty acid oxidation. In contrast to ob/ob mice, in C57Bl/6 mice AJS1669 administration did not alter body weight or reduce glucose levels. These results demonstrate that pharmacological agents that activate GYS1, the main GS subtype found in skeletal muscle, have potential for use as novel treatments for diabetes that improve glucose metabolism in skeletal muscle.

Archive | 2001

Novel phenylalanine derivatives

Kazuyuki Sagi; Tatsuya Okuzumi; Tatsuhiro Yamada; Shunsuke Kageyama; Yoichiro Shima; Tadakiyo Nakagawa; Munetaka Tokumasu; Masayuki Sugiki; Hajime Ito; Itsuya Tanabe; Tamotsu Suzuki; Akira Nakayama; Kazuyuki Ubukata; Kenji Shinkai; Yasuhiro Tanaka; Misato Noguchi; Ayatoshi Andou; Yoriko Yamamoto; Noriyasu Kataoka; Koichi Fujita

Journal of Medicinal Chemistry | 2003

Rational design, synthesis, and structure-activity relationships of novel factor Xa inhibitors: (2-Substituted-4-amidinophenyl)pyruvic and -propionic acids

Kazuyuki Sagi; Tadakiyo Nakagawa; Masahiro Yamanashi; Shingo Makino; Mitsuo Takahashi; Masaru Takayanagi; Kaoru Takenaka; Nobuyasu Suzuki; Seiji Oono; Noriyasu Kataoka; Kohki Ishikawa; Sayaka Shima; Yumiko Fukuda; Takashi Kayahara; Shunji Takehana; Yoichiro Shima; Kazumi Tashiro; Hiroshi Yamamoto; Ryota Yoshimoto; Seinosuke Iwata; Takashi Tsuji; Kuniya Sakurai; Masataka Shoji

Archive | 2016

Pharmaceutical composition for treating diabetes

Tadakiyo Nakagawa; Kayo Matsumoto; Sen Takeshita; Tomomi Yoshida; Munetaka Tokumasu; Hiroki Inoue; Kaori Kobayashi

Archive | 2008

POLY(AMINO ACID) COMPOUND HAVING INHIBITORY ACTIVITY ON ABSORPTION OF PHOSPHORUS AND PHOSPHORUS ABSORPTION INHIBITOR

Tadakiyo Nakagawa; Hironobu Tsugeno; Naomi Matsutani; Masayuki Sugiki; Haruko Hirashima; Tatsuya Okuzumi; Tatsuya Kasahara; Wataru Miyanaga; Takashi Yamamoto; Masatsugu Noguchi; Kayo Matsumoto; Hideyuki Tanaka; Tomoyuki Konda

Archive | 2010

NOVEL ACYL GUANIDINE DERIVATIVES

Wataru Miyanaga; Yoichiro Shima; Misato Noguchi; Akiko Oonuki; Yayoi Kawato; Hiroshi Iwata; Eri Harada; Ryuta Takashita; Hirokazu Ueno; Tadakiyo Nakagawa

Archive | 2017

composto, composição farmacêutica, e, métodos para inibir serina protease, para inibir tripsina e enteropeptidase, para tratar hiperglicemia, para profilaxia ou tratamento da diabetes, para melhorar a sensibilidade à insulina e para profilaxia ou tratamento da obesidade, hiperlipidemia, uma complicação diabética ou síndrome metabólica

Kayo Matsumoto; Koji Ohsumi; Munetaka Tokumasu; Tadakiyo Nakagawa; Taisuke Ichimaru; Takahiro Koshiba; Tamotsu Suzuki; Tatsuhiro Yamada

Archive | 2013

Dérivé d'ester d'acide hétéroarylcarboxylique

Takahiro Koshiba; Munetaka Tokumasu; Taisuke Ichimaru; Koji Ohsumi; Tadakiyo Nakagawa; Tatsuhiro Yamada; Kayo Matsumoto; Tamotsu Suzuki

Archive | 2008

Composé poly(acide aminé) à activité inhibitrice de l'absorption de phosphore et inhibiteur d'absorption de phosphore

Tadakiyo Nakagawa; Hironobu Tsugeno; Naomi Matsutani; Masayuki Sugiki; Haruko Hirashima; Tatsuya Okuzumi; Tatsuya Kasahara; Wataru Miyanaga; Takashi Yamamoto; Masatsugu Noguchi; Kayo Matsumoto; Hideyuki Tanaka; Tomoyuki Konda

Archive | 2004

Nouveau derive phenylalanines

Kazuyuki Sagi; Tatsuya Okuzumi; Tatsuhiro Yamada; Shunsuke Kageyama; Yoichiro Shima; Tadakiyo Nakagawa; Munetaka Tokumasu; Masayuki Sugiki; Hajime Ito; Itsuya Tanabe; Tamotsu Suzuki; Akira Nakayama; Kazuyuki Ubukata; Kenji Shinkai; Yasuhiro Tanaka; Misato Noguchi; Ayatoshi Andou; Yoriko Yamamoto; Noriyasu Kataoka; Koichi Fujita

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Kayo Matsumoto

Ajinomoto

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Kazuyuki Sagi

Ajinomoto

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Munetaka Tokumasu

Ajinomoto

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Tamotsu Suzuki

Ajinomoto

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Masayuki Sugiki

Ajinomoto

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Takashi Kayahara

Ajinomoto

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Tatsuhiro Yamada

Ajinomoto

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Tatsuya Okuzumi

Ajinomoto

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Wataru Miyanaga

Ajinomoto

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Yoichiro Shima

Ajinomoto

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