Litcius/Paper detail

Modular access to chiral bridged piperidine-γ-butyrolactones via catalytic asymmetric allylation/aza-Prins cyclization/lactonization sequences

Cong Fu, Ling He, Hui Xu, Zongpeng Zhang, Xin Chang, Yanfeng Dang, Xiu‐Qin Dong, Chun‐Jiang Wang

2024Nature Communications16 citationsDOIOpen Access PDF

Abstract

Chiral functionalized piperidine and lactone heterocycles are widely spread in natural products and drug candidates with promising pharmacological properties. However, there remains no general asymmetric methodologies that enable rapid assemble both critical biologically important units into one three-dimensional chiral molecule. Herein, we describe a straightforward relay strategy for the construction of enantioenriched bridged piperidine-γ-butyrolactone skeletons incorporating three skipped stereocenters via asymmetric allylic alkylation and aza-Prins cyclization/lactonization sequences. The excellent enantioselectivity control in asymmetric allylation with the simplest allylic precursor is enabled by the synergistic Cu/Ir-catalyzed protocol; the success of aza-Prins cyclization/lactonization can be attributed to the pivotal role of the ester substituent, which acts as a preferential intramolecular nucleophile to terminate the aza-Prins intermediacy of piperid-4-yl cation species. The resulting chiral piperidine-γ-butyrolactone bridged-heterocyclic products show impressive preliminary biological activities against a panel of cancer cell lines.

Topics & Concepts

PiperidineStereocenterAllylic rearrangementIntramolecular forceChemistryNucleophileEnantioselective synthesisStereochemistrySubstituentCombinatorial chemistryPrins reactionTsuji–Trost reactionCatalysisOrganic chemistrySynthetic Organic Chemistry MethodsAsymmetric Synthesis and CatalysisTraditional and Medicinal Uses of Annonaceae
Modular access to chiral bridged piperidine-γ-butyrolactones via catalytic asymmetric allylation/aza-Prins cyclization/lactonization sequences | Litcius