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Direct Entry to 4,10-Didesmethyl (9S)-Dihydroerythronolide A via Catalytic Allene Osmylation

机译:通过催化异戊烯基甲磺酰化直接进入4,10-二甲基(9S)-二氢赤藓内酯A

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摘要

Desmethyl erythronolides have emerged as macrolide targets that may prove effective against resistant bacteria. A five-step sequence to 4,10-didesmethyl (9S)-dihydroerythronolide A (1) from known cyclic bis[allene] 13 is reported. Key structural and mechanistic aspects of the synthesis are discussed along with catalytic allene osmylation. An improved route to 13 is also described.
机译:脱甲基赤藓醇内酯已成为大环内酯的靶标,可能证明对耐药菌有效。据报道,从已知的环状双[Allene] 13到4,10-二甲基(9S)-二氢赤藓醇内酯A(1)的五步序列。讨论了合成的关键结构和机理,以及催化的烯丙糖基化。还描述了一种改进的到达13的途径。

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