封装(网络)
结晶学
X射线
材料科学
化学
纳米技术
光学
计算机科学
物理
计算机网络
作者
Gavin Tay,Toshiaki Wayama,Hiroki Takezawa,Satoshi Yoshida,Sota Sato,Makoto Fujita,Hiroki Oguri
标识
DOI:10.1002/anie.202305122
摘要
Abstract Numerous indole alkaloids such as the iboga‐ and aspidosperma ‐type are believed to be biosynthesized via a common hypothetical intermediate, dehydrosecodine. The highly reactive nature of dehydrosecodine‐type compounds has hampered their isolation and structural elucidation. In this study, we achieved the first X‐ray structural determination of a dehydrosecodine‐type compound by integrating synthetic optimization of the reactivity and stabilizing the fragile molecule by encapsulation into a supramolecular host. Formation of a 1 : 1 complex of the dehydrosecodine‐type labile guest bearing both vinyl indole and dihydropyridine units with the host was observed. This integrated approach not only provides insights into the biosynthetic conversions but also allows stabilization and storage of the reactive and otherwise short‐lived intermediate within the confined hydrophobic cavity.
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