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Featured researches published by Akira Masuda.


Chemistry & Biology | 1997

Stevastelins, a novel group of immunosuppressants, inhibit dual-specificity protein phosphatases

Takuya Hamaguchi; Akira Masuda; Tomio Morino

BACKGROUND Since the molecular target of the immunosuppressive reagents FK506 and cyclosporin A was revealed to be protein phosphatase PP2B (calcineurin), many researchers have been screening the protein phosphatase inhibitors from microbial metabolites to develop new immunosuppressive reagents. We isolated stevastelin B, which is composed of valine, threonine, serine and 3,5-dihydroxy-2,4-dimethyl stearic acid, and stevastelin A, which is a sulphonylated derivative of stevastelin B. To understand the action mechanism of stevastelins A and B, we synthesized a series of stevastelin derivatives and investigated their structure-activity relationships. RESULTS A series of stevastelin derivatives have been systematically synthesized. Stevastelin B inhibited gene expression that is dependent on interleukin-2 (IL-2) or IL-6 promoters in situ, but it had no inhibitory activity against any protein phosphatases in vitro. In contrast, stevastelin A, which is a sulphonylated derivative of stevastelin B, inhibited the phosphatase activity of a dual-specificity phosphatase, VH1-related human protein (VHR), in vitro, but it had no inhibitory activity against gene expression or cell-cycle progression in situ. CONCLUSIONS Stevastelin B is a novel immunosuppressant. It inhibited IL-2 or IL-6 dependent gene expression but did not inhibit the phosphatase activity of calcineurin. The structure-activity relationships show that the acidic functional group on the threonine residue and the stearic acid moiety in the stevastelin molecule are important for inhibitory effects on the dephosphorylation activity of VHR in vitro. Stevastelin B might be sulphonylated or phosphorylated after incorporation into the target cell, and then it interacts with protein tyrosine phosphatases and regulates cell-cycle progression.


The Journal of Antibiotics | 1994

Stevastelins, novel immunosuppressants produced by Penicillium

Tomio Morino; Akira Masuda; Masatoshi Yamada; Masakazu Nishimoto; Takaaki Nishikiori; Seiichi Saito; Nobuyoshi Shimada


The Journal of Antibiotics | 1996

Structural Determination of Stevastelins, Novel Depsipeptides from Penicillium sp.

Tomio Morino; Kei-Ichi Shimada; Akira Masuda; Noriyuki Yamashita; Masakazu Nishimoto; Takaaki Nishikiori; Seiichi Saito


Archive | 2005

Novel Water-Soluble Fullerene, Process for Producing the Same and Active Oxygen Generator Containing the Fullerene

Yasuhiko Tabata; Masatoshi Yamada; Akira Masuda


The Journal of Antibiotics | 1996

Stevastelin A3, D3 and E3, Novel Congeners from a High Producing Mutant of Penicillium sp.

Tomio Morino; Kei-Ichi Shimada; Akira Masuda; Masakazu Nishimoto; Seiichi Saito


The Journal of Antibiotics | 1996

Absolute structural determination of stevastelin B.

Kei-Ichi Shimada; Tomio Morino; Akira Masuda; Masaya Sato; Masayuki Kitagawa; Seiichi Saito


The Journal of Antibiotics | 1995

NK374200, a novel insecticidal agent from Taralomyces, found by physico-chemical screening.

Tomio Morino; Masakazu Nishimoto; Akira Masuda; Shinji Fujita; Takaaki Nishikior; Seiichi Saito


Archive | 1997

Triazine derivative and telomerase inhibitor

Masayuki Kitagawa; Akira Masuda; Makoto Morita; Eiko Sugihara; Masanobu Suzuki; 正行 北川; 亮 増田; 英光 杉原; 誠 森田; 政信 鈴木


Archive | 1997

Novel phenanethridinium derivatives

Akira Masuda; Masato Suwa; Masanobu Suzuki


Archive | 1992

Novel antibiotics NK374186A, NK374186B, NK374186B3 and NK374186C3, process for producing the same, and use of the same

Tomio Morino; Masakazu Nishimoto; Mit Uyuki Nishide; Akira Masuda; Masatoshi Yamada; Eiji Kawano; Takaaki Nishikiori; Seiichi Saito

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