14 茜草根より得られる抗腫瘍活性環状ヘキサペプチドRA-VIIの合成(口頭発表の部)
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概要
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The first total synthesis of RA-VII and deoxybouvardin(RA-V) is described. The synthetic strategies are shown in Chart II. Among them, Route A was only successful. It comprises construction of the 14-membered ring unit 3 and subsequent coupling with tetrapeptide 4. For the construction of the 14-membered ring, which is crucial to this strategy and should be versatile intermediate leading to related compounds, we employed two methods, Route A-1 and A-2. A-1 is intramolecular amidation of linear diphenyl ether 13 (Scheme I). A-2 is intramolecular oxidative coupling of two phenolic parts of dipeptide by thallium trinitrate (Table I, II). A-1 did not give 14-membered ring but dimeric 28-membered one. A-2 afforded 14-membered rings. Thus the oxidation of dichloro dibromo derivatives 20 gave the desired 14-membered ring 23. But tetrabromide 17 was found to cyclize in the opposite fashion comparing with RA. Conversion of 23 to RA-VII was achieved by the successive treatment illustrated in Scheme III and IV. Selective demethylation of RA-VII with AlCl_3 gave deoxybouvardin (RA-V). Other strategies, via 18- and 26-membered ring (Route B and C) are also reported (Chart I).
- 天然有機化合物討論会の論文
- 1987-07-25
著者
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三橋 進
東京薬科大学:(現)東菱薬品工業(株)大森研究所
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糸川 秀治
東京薬大
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井上 哲也
Faculty Of Pharmaceutical Sciences Osaka University
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糸川 秀治
東京薬科大学 薬学部
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井上 勗
Ohmiya Research Laboratory Fuji Yakuhin Co. Ltd.
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Inoue T
Ohmiya Research Laboratory Fuji Yakuhin Co. Ltd
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三橋 進
Tokyo College of Pharmacy
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梅沢 勲
東菱薬品
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湯浅 雅之
東菱薬品
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稲葉 隆之
東菱薬品
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井上 勗
東菱薬品
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三橋 進
東菱薬品
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小倉 克之
千葉大工
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梅沢 勲
Ohmiya Research Laboratory Fuji Yakuhin Co. Ltd.
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湯浅 雅之
Pola R & D Laboratory
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稲葉 隆之
Central Pharmaceutical Research Institute, Japan Tabaco Inc.,
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Inoue T
Osaka University Of Pharmaceutical Sciences
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井上 輝比古
Pharmaceutical Research Department Ube Laboratory Corporate Research & Development Ube Industrie
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稲葉 隆之
Central Pharmaceutical Research Institute Japan Tabaco Inc.
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小倉 克之
千葉大学工学部
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Inoue Takao
Faculty Of Pharmaceutical Sciences Hoshi University
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