Despite the excellent chemical properties of N-heterocycles, pyrido[1,2-α]azepine remains elusive due to its potential antiaromaticity and lability. Herein, we demonstrate the synthesis and characterization of the first bicyclic pyrido[1,2-α]azepine that leverages the coordination to the ruthenium center to promote the stability of N-bridged bicycle.
![Graphical abstract: A missing member of conjugated N-heterocycles: realizing pyrido[1,2-α]azepine by reacting ruthenium alkenylcarbene complex with alkyne](/en/Image/Get?imageInfo.ImageType=GA&imageInfo.ImageIdentifier.ManuscriptID=C8CC00758F&imageInfo.ImageIdentifier.Year=2018)
X. Zhou, F. Huang, C. Tang, Q. Zhuo, Z. Chen, H. Zhang and H. Xia, Chem. Commun., 2018, 54, 4009 DOI: 10.1039/C8CC00758F
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