Kwon Yonghoon, Schulthoff Saskia, Dao Quang Minh, Wirtz Conny, Fürstner Alois
Max-Planck-Institut für Kohlenforschung, 45470, Mülheim/Ruhr, Germany.
Chemistry. 2018 Jan 2;24(1):109-114. doi: 10.1002/chem.201705550. Epub 2017 Dec 7.
The first total synthesis of the potent antibiotic disciformycin B (2) is described, which is exceptionally isomerization-prone and transforms into disciformycin A (1) even under notably mild conditions. To outweigh this bias, the approach to 2 hinged on the use of a silyl residue at C4 to lock the critical double bond in place and hence insure the integrity of the synthetic intermediates en route to 2. This tactic was instrumental for the preparation of the building blocks and formation of the macrocyclic ring via ring closing alkyne metathesis (RCAM). To make the end game successful, however, it proved necessary to cleave the C-silyl protecting group off; it was at this stage that the exceptional sensitivity of the target became fully apparent.
本文描述了强效抗生素盘状霉素B(2)的首次全合成,该化合物极易发生异构化,甚至在非常温和的条件下也会转化为盘状霉素A(1)。为了克服这种偏向性,合成2的方法依赖于在C4位使用硅烷基来锁定关键双键的位置,从而确保合成中间体在通往2的路线上的完整性。这种策略对于制备构建模块以及通过闭环炔烃复分解反应(RCAM)形成大环至关重要。然而,为了使最终合成成功,事实证明有必要脱去C-硅烷基保护基;正是在这个阶段,目标化合物的异常敏感性才完全显现出来。
Zotero 插件