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Dive into the research topics where Takemitsu Asaoka is active.

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Featured researches published by Takemitsu Asaoka.


Antimicrobial Agents and Chemotherapy | 2002

Strong antifungal activity of SS750, a new triazole derivative, is based on its selective binding affinity to cytochrome P450 of fungi.

Masaru Matsumoto; Kazuya Ishida; Akihiro Konagai; Kazunori Maebashi; Takemitsu Asaoka

ABSTRACT SS750 [(R)-(−)-2-(2,4-difluorophenyl)-1-(ethylsulfonyl)-1,1-difluoro-3-(1H-1,2,4-triazol-1-yl)-2-propanol] is a new triazole, and its potential as an antifungal agent was evaluated by in vitro and in vivo studies. In a comparison of the MICs at which 50% of isolates are inhibited (MIC50s) for all strains of Candida species and Cryptococcus neoformans tested, SS750 was four times or more active than fluconazole and had activity comparable to that of itraconazole. The most important advantage of SS750 was that, when the MIC90s were compared, SS750 had 64 and 32 times greater antifungal activities than fluconazole against Candida krusei and Candida glabrata, respectively, which are intrinsically less susceptible to fluconazole. In cyclophosphamide-immunosuppressed mouse models of systemic and pulmonary candidiasis caused by C. albicans, oral SS750 prolonged the number of days of survival of infected animals in a dose-dependent manner and was 4 and ≥64 times more potent than fluconazole and itraconazole, respectively. In a safety profile, SS750, like fluconazole, had less of an affinity for binding to mammalian cytochrome P450 compared with that of ketoconazole, despite its strong affinity for binding to fungal cytochrome P450. The mechanism for the increased in vitro antifungal activity of SS750 against C. krusei is partially due to the potent inhibitory activity (3.7 times versus that of fluconazole) of C. krusei cytochrome P450 sterol 14α-demethylase; SS750 showed a strong affinity for binding to cytochrome P450 of C. krusei, indicating that SS750 acts by inhibiting the cytochrome P450 sterol 14α-demethylase of fungal cells.


Archive | 1991

Quinolone carboxylic acid derivatives

Fujiko Konno; Akihiro Shibata; Hideaki Matsuda; Takemitsu Asaoka; Ryuichi Kawahara; Naokata Taido; Tasdayuki Kuraishi; Sunao Takeda


Chemical & Pharmaceutical Bulletin | 2001

New Antifungal 1,2,4-Triazoles with Difluoro(substituted sulfonyl)methyl Moiety

Hiromichi Eto; Yasushi Kaneko; Sunao Takeda; Minoru Tokizawa; Susumu Sato; Kouiti Yoshida; Setsuo Namiki; Masaki Ogawa; Kazuki Maebashi; Kazuya Ishida; Masaru Matsumoto; Takemitsu Asaoka


The Journal of Antibiotics | 1982

A new saframycin, saframycin R.

Takemitsu Asaoka; Katsukiyo Yazawa; Yuzuru Mikami; Tadashi Arai; Katsuhiro Takahashi


Archive | 2002

Quinolone carboxylic acid compositions and related methods of treatment

Samir Roy; Santosh Kumar Chandrasekaran; Katsumi Imamori; Takemitsu Asaoka; Akihiro Shibata; Masami Takahashi; Lyle M. Bowman


Archive | 1984

Quinoline carboxylic acid derivatives

Fujiko Konno; Akihiro Shibata; Hideaki Matsuda; Takemitsu Asaoka; Ryuichi Kawahara; Naokata Taido; Tadayuki Kuraishi; Sunao Takeda


The Journal of Antibiotics | 1982

Bioconversions of saframycin A specific to some genera of actinomycetes.

Katsukiyo Yazawa; Takemitsu Asaoka; Katsuhiro Takahashi; Yuzuru Mikami; Tadashi Arai


Archive | 1997

Triazole derivative or salt thereof

Minoru Tokizawa; Sunao Takeda; Yasushi Kaneko; Hiromichi Eto; Kazuya Ishida; Kazunori Maebashi; Masaru Matsumoto; Takemitsu Asaoka; Susumu Sato; Hideaki Matsuda


The Journal of Antibiotics | 1987

Pyrroxamycin, a new antibiotic taxonomy, fermentation, isolation, structure determination and biological properties

Kenichi Yano; Junji Oono; Kinichi Mogi; Takemitsu Asaoka; Toshiaki Nakashima


Archive | 1984

Novel Fredericamycin A derivatives

Koichi Yokoi; Hiroshi Hasegawa; Tadashi Narita; Takemitsu Asaoka; Kenichi Kukita; Seiji Ishizeki; Toshiaki Nakashima

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Susumu Sato

University of Shizuoka

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Fujiko Konno

Takeda Pharmaceutical Company

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