Jing Chunxiu, Jiang Hui-Mei, Yan Qiuling, Huang Fanchen, Sun Jialu, Xu Li-Ping, Wei Hao
Key Laboratory of Synthetic and Natural Functional Molecule of the Ministry of Education, College of Chemistry & Materials Science, Northwest University, Xi'an, 710069, P.R. China.
School of Chemistry and Chemical Engineering, Shandong University, Jinan, 250100, P.R. China.
Angew Chem Int Ed Engl. 2025 Sep 22;64(39):e202512288. doi: 10.1002/anie.202512288. Epub 2025 Aug 8.
Heterocyclic replacements are crucial tools in medicinal chemistry, enhancing the physicochemical properties of lead compounds. Pyridine, a core structural motif in numerous drug candidates, often serves as a key heterocyclic scaffold. Nonetheless, a universally applicable synthetic strategy for the direct conversion of pyridines into a diverse array of other heterocycles has yet to be established. In this study, we present a skeletal remodeling strategy that enables the transformation of pyridines into corresponding anilines via Lewis acid-catalyzed nitrogen atom transposition. These anilines can subsequently serve as versatile intermediates for accessing a variety of heterocyclic structures, thereby facilitating the rapid synthesis of novel bioactive analogs. DFT calculations indicate that the Lewis acid catalyst not only aids in the formation of pyridinium salts, enhances nucleophilic addition and nitrogen release. This methodology demonstrates considerable utility across a range of complex pyridine derivatives and several commercially available drugs, highlighting its potential for pharmaceutical diversification.
杂环取代基是药物化学中的关键工具,可增强先导化合物的物理化学性质。吡啶是众多候选药物中的核心结构基序,常作为关键的杂环骨架。然而,尚未建立一种普遍适用的将吡啶直接转化为多种其他杂环的合成策略。在本研究中,我们提出了一种骨架重塑策略,该策略能够通过路易斯酸催化的氮原子转位将吡啶转化为相应的苯胺。这些苯胺随后可作为通用中间体用于构建各种杂环结构,从而促进新型生物活性类似物的快速合成。密度泛函理论计算表明,路易斯酸催化剂不仅有助于吡啶盐的形成,还能增强亲核加成和氮的释放。该方法在一系列复杂的吡啶衍生物和几种市售药物中显示出相当大的实用性,突出了其在药物多样化方面的潜力。
