Synthesis and Structure-activity Relationships of Amastatin Analogues, Inhibitors of Aminopeptidase A
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概要
- 論文の詳細を見る
Stereoisomers and analogues of amastatin, [(2S, 3R)-3-amino-2-hydroxy-5-methylhexanoyl]-L-Val-L-Val-L-Asp, were synthesized and their inhibitory activities towards aminopeptidase A (AP-A) and other arylamidases tested. Among the four stereoisomers of a new amino acid residue in amastatin, the 2S stereoisomers exhibited strong activity. In a series of compounds in which the C-terminal amino acid of amastatin was substituted by other amino acids, the one containing Asp or Glu showed the strongest activity towards AP-A. In a series of compounds in which the second or third residue from the amino terminal of amastatin was substituted by other amino acids, the one containing hydrophobic amino acids showed strong activity. In the study of the relationship of the length of the peptide chain and inhibitory activity, the activity towards AP-A was seen to increase until the length of the peptide reached that of a tetrapeptide.
- 社団法人 日本農芸化学会の論文
著者
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AOYAGI Takaaki
Institute of Microbial Chemistry
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UMEZAWA HAMAO
Institute of Microbial Chemistry
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Yoshioka Takeo
Central Research Laboratories Mercian Corporation
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Inui Taiji
Central Research Laboratories Sanraku-ocean Co. Ltd.
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Shimauchi Yasutaka
Central Research Laboratories Sanraku Ocean Co. Ltd.
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Nakamura Kenji
Central Research Laboratory Japan Aviation Electronics Industry Ltd.
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Inui Taiji
Central Research Laboratories, Sanraku-Ocean Co., Ltd.
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TOBE Hiroyasu
Institute of Microbial Chemistry
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MORISHIMA Hajime
Institute of Microbial Chemistry
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ISHIKI Kunio
Central Research Laboratories, Sanraku-Ocean Co., Ltd.
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Umezawa Hamao
Institute of Bioorganic Chemistry
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YOSHIOKA Takeo
Central Research Laboratories, Sanraku-Ocean Co., Ltd.
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NAKAMURA Kenji
Central Research Laboratories, Sanraku-Ocean Co., Ltd.
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SHIMAUCHI Yasutaka
Central Research Laboratories, Sanraku-Ocean Co., Ltd.
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