17 カリクリン類の合成研究(口頭発表の部)
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概要
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Calyculins (1) isolated from the marine sponge Discodermia calyx have strong cytotoxic activity and calyculin A has been revealed to be an inhbitor of protein phosphatases 1 and 2A. The relative stereostructures of calyculins have been determined by X-ray diffraction studies and their absolute configurations have been depicted as the structures 1 by CD spectral studies of the C_<33>-C_<37> unit. We have provided conclusive evidence supporting the reported absolute configurations of calyculins by the synthesis of the C_<33>-C_<37> unit. The intriguing biological activities of calyculins coupled with their structural curiosities have led us to investigate the total synthesis of calyculins. Retrosynthetic analysis has revealed that 1 would be constructed from four fragments A, B, C, and D, shown in Scheme 1. Fragment A could be prepared by use of the Stille coupling of the vinyl iodide unit 4 with the nitrile unit 3 followed by converting to the vinyl iodide function according to the Barton's procedure. Fragment C have been prepared by the oxazoline formation of the N-acylserine (21, 27) and the subsequent oxidation of the oxazoline. Synthesis of fragment D has been accomplished from (S)-serine using osmium tetroxide mediated dihydroxylation of the Z-olefin. The common northern part 41 of calyculins A, B, E, and F has been synthesized by coupling of the 38 with the 39, followed by N, N-dimethylation.
- 天然有機化合物討論会の論文
- 1993-09-10
著者
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横川 文明
名市大・薬
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濱田 康正
名市大・薬
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塩入 孝之
名市大・薬
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塩入 孝之
名城大院・総合学術
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塩入 孝之
名古屋市大・薬
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濱田 康正
Faculty of Pharmaceutical Sciences, Nagoya City University
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横川 文明
ノバルティスファーマ・筑波研
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濱田 康正
Faculty Of Pharmaceutical Sciences Nagoya City University
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