Cyclization of 2-Aminopyridines as Binucleophile and Mucobromic Acid as C3 Synthon: A New Access to Imidazo[1,2-a]Pyridines

Author:

Chen Qi1,Li Huan-Qing1,Chen Zhao-Hua1,Chen Zu-Jia1,Yang Kai2,Zhang You-Cai1,Wang Zhao-Yang1

Affiliation:

1. School of Chemistry, South China Normal University, Key Laboratory of Theoretical Chemistry of Environment, Ministry of Education, Guangzhou Key Laboratory of Analytical Chemistry for Biomedicine, GDMPA Key Laboratory for Process Control and Quality Evaluation of Chiral Pharmaceuticals, Guangzhou, 510006, P.R. China

2. College of Pharmacy, Gannan Medical University, Ganzhou, 341000, P.R. China

Abstract

Abstract: For the first time, we have developed a strategy that provides an access to imidazo[ 1,2-a] pyridines via the cyclization of 2-aminopyridine with mucobromic acid as C3 synthon. In the combination with theoretical calculation, the reaction mechanism is proposed. Background: 2-Aminopyridines are the typical pyridine α-site derivatives, which have received growing interest in using as a kind of synthons in organic synthesis and drug synthesis because of their special binucleophilic framework. Methods: All these obtained compounds were characterized by NMR. Among them, 3a was characterized by single-crystal X-ray analysis. All the theoretical calculation works were performed by Gaussian software. Results: A series of the desired compounds can be synthesized at room temperature via a mild procedure under the promotion of simple inorganic base K2CO3. Conclusion: This mild strategy fits the concept of green chemistry, providing a novel idea for the construction of nitrogen-containing polyheterocyclic compounds.

Funder

NSFC, Natural Science Foundation of China

Guangdong Basic and Applied Basic Research Foundation

Publisher

Bentham Science Publishers Ltd.

Subject

General Medicine

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