Synthesis of Benzodiazepines Through Ring Opening/Ring Closure of Benzimidazole Salts

Sheng Tao; Qingqing Bu; Qianqian Shi; Donghui Wei; Bin Dai; Ning Liu

doi:10.1002/chem.201905828

Synthesis of Benzodiazepines Through Ring Opening/Ring Closure of Benzimidazole Salts

Chemistry. 2020 Mar 12;26(15):3252-3258. doi: 10.1002/chem.201905828. Epub 2020 Feb 25.

Authors

Sheng Tao¹, Qingqing Bu¹, Qianqian Shi², Donghui Wei², Bin Dai¹, Ning Liu¹

Affiliations

¹ School of Chemistry and Chemical Engineering, Key Laboratory for Green Processing of Chemical Engineering of Xinjiang Bingtuan, Shihezi University, 832003, Shihezi, P. R. China.
² College of Chemistry, Center of Computational Chemistry, Zhengzhou University, 450001, Zhengzhou, P. R. China.

PMID: 31950547
DOI: 10.1002/chem.201905828

Abstract

Pyrido-benzodiazepine derivatives are undoubtedly one of the most important structural motifs in the marketed drugs and the drug candidates. Commonly synthetic methods for construction of the benzodiazepine ring derivatives are based on the condensation reactions of two highly functionalized synthons. The development of synthesis for these compounds, however, is hampered by the regioselectivity and atom economy. In this work, a one-step synthesis of pyrido-benzodiazepine backbones and its analogues is achieved through continuous ring-opening hydrolysis of benzimidazole salts and intramolecular C-H bond activation. The reaction mechanism is explored by control experiments and density functional theory (DFT) calculations.

Keywords: C−H bond activation; benzodiazepines; cascade reaction; seven-membered ring; silver.

Grants and funding

21868033/National Natural Science Foundation of China