39 細胞毒性ポリケチドcallystatin Aの構造活性相関とその作用機序(口頭発表の部)
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概要
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During the course of our investigation searching for new bioactive substances from marine organisms, we isolated an extremely potent cytotoxic polyketide designated callystatin A (1) from the marine sponge Callyspongia truncata and determined its absolute stereostructure. In order to create a new anti-tumor lead compound, the structure-activity relationships of 1 using several synthetic analogues have been studied. As a result of evaluating their cytotoxicities, the following crucial factors have been disclosed; 1) α, β-unsaturated δ-lactone moiety is a conclusive pharmacophore; 2) 5-R configuration, asymmetric center at C-10, and β-hydroxy ketone moiety contribute to affinity to receptor molecule. From the experiment utilizing the fission yeast expressing an NES-GFP-NLS fusion protein, callystatin A (1) was found to inhibit nuclear export signals (NES) dependent transport of proteins from the nucleus to the cytoplasm as well as leptomycin B (2). In addition, 1 was shown to inhibit direct binding between NES and CRM1 through the competitive experiment by use of the biotinylated leptomycin B.
- 天然有機化合物討論会の論文
- 1999-09-01
著者
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村上 啓寿
阪大院薬
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MURAKAMI Nobutoshi
Kyoto Pharmaceutical University
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樋口 浩一
阪大院薬
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筒井 康裕
阪大院薬
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村上 啓寿
阪大院薬:presto
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Matsumura N
Res. Foundation Itsuu Lab. Tokyo Jpn
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青木 俊二
兵庫医療大薬
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小林 資正
阪大院薬
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青木 俊二
阪大院薬
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中島 辰雄
阪大院薬
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杉本 昌則
阪大院・薬
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杉本 昌則
阪大院薬
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吉田 稔
東大院農
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工藤 信明
東大院農
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吉田 稔
理研
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