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N-Benzylhydroxylamine as a “C1N1 synthon” in Imidazoles Synthesis via Activation the α–C(sp3)−H under I2-DMSO System
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  • Yong-Xing Tang,
  • You Zhou,
  • Hao-Xuan Wu,
  • Li-Sheng Wang,
  • Chun-Yan Wu,
  • Shi-Yi Zhuang,
  • Anxin Wu
Yong-Xing Tang
Central China Normal University
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You Zhou
Central China Normal University
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Hao-Xuan Wu
Central China Normal University
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Li-Sheng Wang
Central China Normal University
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Chun-Yan Wu
Central China Normal University
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Shi-Yi Zhuang
China Jiliang University
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Anxin Wu
Central China Normal University

Corresponding Author:chwuax@mail.ccnu.edu.cn

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Abstract

A novel process using N-benzylhydroxylamine hydrochloride as a “C1N1 synthon” in [2 + 2 + 1] cyclization for the construction of 1,2,5-trisubstituted imidazoles has been described for the first time. The key to realizing this process lies on capturing arylamines by in situ generated novel acyl ketonitrone intermediates. Subsequent tautomerization activates the α–C(sp3)−H of N-benzylhydroxylamines, thus breaks through its inherent reaction mode and achieves N, α–C site-selective cyclization. Furthermore, this method enables scale-up synthesis and late-stage modification of complex molecules.