Affiliation:
1. Department of Medicinal Chemistry, School of Pharmacy Qingdao University Qingdao, Shandong 266021 China
2. Department of Chemistry, Guangdong Provincial Key Laboratory of Catalysis, College of Science, Southern University of Science and Technology Guangming Advanced Research Institute Southern University of Science and Technology (SUSTech) Shenzhen 518055 China
Abstract
AbstractThe chemistry of quinone methides formed in situ has been flourishing in recent years. In sharp contrast, the development and utilization of biphenyl quinone methides are rare. In this study, we achieved a remote stereocontrolled 1,12‐conjugate addition of biphenyl quinone methides formed in situ for the first time. In the presence of a suitable chiral phosphoric acid, alkynyl biphenyl quinone methides were generated from α‐[4‐(4‐hydroxyphenyl)phenyl]propargyl alcohols, followed by enantioselective 1,12‐conjugate addition with indole‐2‐carboxylates. The strategy enabled the alcohols to serve as efficient allenylation reagents, providing practical access to a broad range of axially chiral allenes bearing a (1,1′‐biphenyl)‐4‐ol unit, which were previously less accessible. Combined with control experiments, density functional theory calculations shed light on the reaction mechanism, indicating that enantioselectivity originates from the nucleophilic addition of alkynyl biphenyl quinone methides. Notably, not only the presence of biphenyl quinone methides as versatile intermediates was confirmed but also organocatalytic enantioselective 1,12‐addition was established.
Funder
Natural Science Foundation of Shandong Province
Guangdong Provincial Key Laboratory Of Catalysis
National Natural Science Foundation of China