立体中心
化学
全合成
立体化学
邻接
级联
双环分子
立体选择性
戒指(化学)
序列(生物学)
骨架(计算机编程)
级联反应
重排
立体异构
化学合成
多环化合物
螺旋桨烷
组合化学
萜类
计算化学
内酯
分子
药物发现
作者
Xing-Qian Shan,Xiang Zhang,Pengfei Lian,Bao-Kuan Guo,Yong‐Qiang Tu,Shuping Hou
摘要
-inflammatory activity, characterized by its intricate fused-bridged 5/5/5/6 tetracyclic skeleton and six contiguous stereocenters, including two adjacent bridgehead all-carbon quaternary centers, which pose significant challenges to chemical synthesis. Herein we describe the first total synthesis of papililone A in a nine-step longest linear sequence (LLS) from commercial materials without the use of a protecting group, achieved through a cyclization cascade strategy. The strained fused-bridged 5/5/6 tricyclic framework and the two contiguous stereocenters were efficiently constructed in a single step via an unprecedented Pd-catalyzed alkenylation/6-endo-trig cyclization, while the fused 5/5 bicyclic ring system and the vicinal all-carbon quaternary stereocenters were rapidly forged through a combination of a polar-radical cyclization cascade, a convergent fragment coupling, and a vinylogous α-ketol rearrangement in a highly stereoselective manner. This concise approach establishes the β-methyl configuration at C17 as the authentic stereochemistry of naturally occurring papililone A, resolving previous computational ambiguities and facilitating future biological studies.
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