Intramolecular Ni-catalyzed reductive coupling enables enantiodivergent synthesis of linoxepin.
Zi-Hao LiuJian XiaoQian-Qian ZhaiXi TangLi-Jun XuZhi-Yuan ZhuangYa-Wen WangYu PengPublished in: Chemical communications (Cambridge, England) (2024)
A nickel-catalyzed reductive tandem cyclization of the elaborated β-bromo acetal with a dibenzoxepin scaffold was invented to strategically construct the remaining two rings in linoxepin. The generated diasterodivergent intermediates could be easily converted to both enantiomers of this unique cyclolignan molecule via facile oxidations, thus realizing enantiodivergent total synthesis of linoxepin for the first time.