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Dive into the research topics where Taketoshi Fujimori is active.

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Featured researches published by Taketoshi Fujimori.


Journal of Dermatological Science | 2014

Depigmentation caused by application of the active brightening material, rhododendrol, is related to tyrosinase activity at a certain threshold.

Shinya Kasamatsu; Akira Hachiya; Shun Nakamura; Yuka Yasuda; Taketoshi Fujimori; Kei Takano; Shigeru Moriwaki; Tadashi Hase; Tamio Suzuki; Kayoko Matsunaga

BACKGROUND Tyrosinase, the rate-limiting enzyme required for melanin production, has been targeted to develop active brightening/lightening materials for skin products. Unexpected depigmentation of the skin characterized with the diverse symptoms was reported in some subjects who used a tyrosinase-competitive inhibiting quasi-drug, rhododendrol. OBJECTIVE To investigate the mechanism underlying the depigmentation caused by rhododendrol-containing cosmetics, this study was performed. METHODS The mechanism above was examined using more than dozen of melanocytes derived from donors of different ethnic backgrounds. The RNAi technology was utilized to confirm the effect of tyrosinase to induce the cytotoxicity of rhododendrol and liquid chromatography-tandem mass spectrometry was introduced to detect rhododendrol and its metabolites in the presence of tyrosinase. RESULTS Melanocyte damage was related to tyrosinase activity at a certain threshold. Treatment with a tyrosinase-specific siRNA was shown to dramatically rescue the rhododendrol-induced melanocyte impairment. Hydroxyl-rhododendrol was detected only in melanocytes with higher tyrosinase activity. When an equivalent amount of hydroxyl-rhododendrol was administered, cell viability was almost equally suppressed even in melanocytes with lower tyrosinase activity. CONCLUSION The generation of a tyrosinase-catalyzed hydroxyl-metabolite is one of the causes for the diminishment of the melanocyte viability by rhododendrol.


Food and Chemical Toxicology | 2011

Measurement of glycidol hemoglobin adducts in humans who ingest edible oil containing small amounts of glycidol fatty acid esters.

Hiroshi Honda; Masayuki Onishi; Kenkichi Fujii; Naohiro Ikeda; Tohru Yamaguchi; Taketoshi Fujimori; Naohiro Nishiyama; Toshio Kasamatsu

Hemoglobin (Hb) adducts are frequently used to address and/or monitor exposure to reactive chemicals. Glycidol (G), a known animal carcinogen, has been reported to form Hb adducts. Here, we measure G adduct levels in humans who daily ingest DAG oil, an edible oil consisting mainly of diacylglycerol. Since DAG oil contains a small amount of glycidol fatty acid esters (GEs), possible exposure to G released from GEs has been raised as a possible concern. For measurement of Hb adducts, we employed the N-alkyl Edman method reported by Landin et al. (1996) using gas chromatography-tandem mass spectrometry with minor modifications to detect G-Hb adducts as N-(2,3-dihydroxy-propyl)valine (diHOPrVal). Blood samples were collected from 7 DAG oil users and 6 non-users, and then G-Hb adduct levels were measured. G-Hb adducts were detected in all samples. The average level of diHOPrVal was 3.5±1.9pmol/g globin in the DAG oil users and 7.1±3.1pmol/g globin in the non-users. We conclude that there is no increased exposure to G in individuals who daily ingest DAG oil.


Journal of Natural Medicines | 2014

The inhibitory effect of a Platycodon root extract on ultraviolet B-induced pigmentation due to a decrease in Kit expression

Shinya Kasamatsu; Akira Hachiya; Yoshie Shimotoyodome; Akiyo Kameyama; Yuki Miyauchi; Kazuhiko Higuchi; Taketoshi Fujimori; Atsushi Ohuchi; Yusuke Shibuya; Takashi Kitahara

The signaling of stem cell factor (SCF) through its receptor Kit is known to play an important role in regulating cutaneous melanogenesis. In the course of UVB-induced pigmentation, the expression of membrane-bound SCF by epidermal keratinocytes is upregulated at an early phase and subsequently activates neighboring melanocytes via their Kit receptors. In order to identify effective skin-lightening materials, we screened botanical extracts to determine their abilities to diminish Kit expression in melanocytes. A Platycodon root extract was consequently found to have a remarkable inhibitory activity on Kit expression. When the extract was applied to three-dimensional human skin substitutes in vitro and to human skin in vivo after UVB irradiation, their pigmentation was significantly reduced, confirming the substantial contribution of the suppression of SCF/Kit signaling to preventing or inhibiting melanin synthesis. These data demonstrate that a Platycodon root extract is a promising material for a skin-lightening product to improve pigmentation-related diseases.


Archive | 1994

Amine derivative and dermatologic preparation containing the same

Yukihiro Ohashi; Yukihiro Yada; Yoshinori Takema; Taketoshi Fujimori; Akira Kawamata; Hiroyuki Ohsu; Kazuhiko Higuchi; Genji Imokawa; Hiroshi Kusuoku; Ayumi Ogawa; Tsutomu Fujimura


Archive | 1995

Method of smoothing or removing wrinkles and method of stimulating collagen synthesis

Tsutomu Fujimura; Ayumi Ogawa; Hiroyuki Ohsu; Yoshinori Takema; Kimihiko Hori; Shinya Amano; Taketoshi Fujimori; Yukihiro Ohashi; Yasuto Suzuki


Archive | 1993

Amide derivative and external skin care preparation containing the same

Taketoshi Fujimori; Yukihiro Ohashi; Akira Kawamata


Archive | 1998

Acne prevention and amelioration agent

Taketoshi Fujimori; Kazuhiko Higuchi; Junko Ishikawa; Takashi Kitahara; Yukihiro Ohashi; 隆志 北原; 幸浩 大橋; 和彦 樋口; 准子 石川; 健敏 藤森


Archive | 1992

Composition for external skin care

Yukihiro Ohashi; Taketoshi Fujimori; Minoru Nagai; Akira Kawamata; Yukihiro Yada; Kazuhiko Higuchi; Genji Imokawa; Yoshinori Takema; Yukiko Sakaino; Ayumi Ogawa; Tsutomu Fujimura


Archive | 2008

Method for producing cross-coupling compound

Taketoshi Fujimori; Mio Ishita; Yoshinori Nishizawa


Archive | 2007

Method for producing branched fatty acid

Taketoshi Fujimori; Mio Ishita; Yoshinori Nishizawa; 美緒 井下; 健敏 藤森; 義則 西澤

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