化学
立体中心
对映选择合成
全合成
立体化学
废止
胺化
碎片(计算)
键裂
环加成
结构母题
迈克尔反应
立体选择性
序列(生物学)
氧化裂解
劈理(地质)
分子
双键
自由基环化
加合物
组合化学
立体异构
作者
Yelin Wu,Chuang Li,Junlin He,Yuanxu Liu,Ningwei Wang,Weiwei Fang,Lei Zhang,Xiaoyu Liu,Yong Qin
摘要
The first asymmetric total synthesis of the diterpenoid alkaloid (+)-vilmotenitine A has been accomplished. Strategically, we employed an enantioselective Michael addition to construct the C4 all-carbon quaternary stereocenter and an oxidative dearomatization/Diels-Alder cycloaddition for assembly of the A/B-ring system. Initial attempts to install the E-ring via hydrodealkenylative fragmentation/reductive amination in the presence of the D-ring, or conversely, to construct the D-ring via a Robinson-type annulation with the E-ring in place, were fruitless. The successful route ultimately relied on a hydrodealkenylative fragmentation/Mannich cyclization sequence to forge the E-ring as well as a biogenetically inspired Grob fragmentation to access the complete framework through cleavage of the C7-C17 bond and formation of the requisite C7-C8 double bond. The successful Grob fragmentation provides support for the proposed biosynthetic pathway. This work also leads to definitive revision of the structure originally assigned to hemsleyaconitine F.
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