Li Shun, Tang Juan, Shi Yonglin, Yan Meixin, Fu Yihua, Su Zhishan, Xu Jiaqi, Xue Weichao, Zheng Xueli, Ge Yicen, Li Ruixiang, Chen Hua, Fu Haiyan
Key Laboratory of Green Chemistry & Technology, Ministry of Education, College of Chemistry, Sichuan University, Chengdu, Sichuan, 610064, PR China.
College of Materials, Chemistry and Chemical Engineering, Chengdu University of Technology, Chengdu, Sichuan, 610059, PR China.
Nat Commun. 2024 Aug 28;15(1):7420. doi: 10.1038/s41467-024-51452-0.
Regioselective C-H functionalization of pyridines remains a persistent challenge due to their inherent electronically deficient properties. In this report, we present a strategy for the selective pyridine C3-H thiolation, selenylation, and fluorination under mild conditions via classic N-2,4-dinitrophenyl Zincke imine intermediates. Radical inhibition and trapping experiments, as well as DFT theoretical calculations, indicated that the thiolation and selenylation proceeds through a radical addition-elimination pathway, whereas fluorination via a two-electron electrophilic substitution pathway. The pre-installed electron-deficient activating N-DNP group plays a crucial and positive role, with the additional benefit of recyclability. The practicability of this protocol was demonstrated in the gram-scale synthesis and the late-stage modification of pharmaceutically relevant pyridines.
由于吡啶固有的电子缺欠性质,其区域选择性C-H官能化仍然是一个长期存在的挑战。在本报告中,我们提出了一种策略,通过经典的N-2,4-二硝基苯基津克烯胺中间体,在温和条件下实现吡啶C3-H的硫醇化、硒化和氟化反应。自由基抑制和捕获实验以及密度泛函理论(DFT)计算表明,硫醇化和硒化反应通过自由基加成-消除途径进行,而氟化反应则通过双电子亲电取代途径进行。预先安装的缺电子活化N-DNP基团起着关键的积极作用,并且具有可回收利用的额外优势。该方法的实用性在克级规模合成以及药学相关吡啶的后期修饰中得到了证明。
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