Yu Tianzi, Sun Ying, Tu Canhui, Chen Ting, Fu Shaomin, Liu Bo
Key Laboratory of Green Chemistry & Technology of Ministry of Education, College of Chemistry, Sichuan University 29 Wangjiang Rd. Chengdu Sichuan 610064 China
Chem Sci. 2020 Jun 19;11(27):7177-7181. doi: 10.1039/d0sc02829k.
As a natural diterpenoid, crotophorbolone possesses a challenging ,-5/7/6 framework decorated with six contiguous stereogenic centers and is structurally and biogenetically related to tigliane-type diterpenoids with intriguing bioactivities such as phorbol and prostratin. Based on the convergent strategy, we completed an eighteen-step total synthesis of crotophorbolone starting from (-)-carvone and (+)-dimethyl-2,3--isopropylidene-l-tartrate. The key elements of the synthesis involve expedient installation of the six-membered ring and the five-membered ring with multiple functional groups at an early stage, cyclization of the seven-membered ring through alkenylation of the ketone between the five-membered ring and the six-membered ring, functional group-sensitive ring-closing metathesis and final selective introduction of hydroxyls at C and C.
作为一种天然二萜类化合物,巴豆大戟醇酮具有一个具有挑战性的 5/7/6 骨架,其上装饰有六个相邻的手性中心,并且在结构和生源上与具有有趣生物活性的大戟烷型二萜类化合物(如佛波醇和原锥虫素)相关。基于汇聚策略,我们从 (-)-香芹酮和 (+)-二甲基-2,3-O-异亚丙基-l-酒石酸酯出发,完成了巴豆大戟醇酮的十八步全合成。该合成的关键步骤包括在早期方便地构建带有多个官能团的六元环和五元环,通过五元环和六元环之间酮的烯基化反应进行七元环的环化,官能团敏感的闭环复分解反应以及最后在 C 和 C 处选择性引入羟基。
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