Catalytic Asymmetric Total Syntheses of (-)-Galanthamine and (-)-Lycoramine.
Qing ZhangFu-Min ZhangChang-Sheng ZhangSi-Zhan LiuJin-Miao TianShao-Hua WangXiao-Ming ZhangYong-Qiang TuPublished in: The Journal of organic chemistry (2019)
The catalytic asymmetric total syntheses of the biologically important and therapeutically valuable Amaryllidaceae alkaloids (-)-galanthamine and (-)-lycoramine have been divergently achieved from commercially available 3-butyn-1-ol. A newly developed spirocyclic pyrrolidine (SPD)-catalyzed enantioselective Robinson annulation rapidly constructs the key cis-hydrodibenzofuran core, which bears an all-carbon quaternary stereocenter of the target molecules with an excellent stereoselective control. Additionally, the current asymmetric synthetic strategy provides an alternative approach toward the syntheses of (-)-galanthamine and its analogues.