化学
吡啶
立体化学
组合化学
分子
外围设备
吡啶类化合物
药物化学
催化作用
吡咯
作者
Shun Li,Pingyao Gan,Xiang Peng,XJ Huang,Minghui Xiao,Jinrong Jiang,Guanglian Zhu,Weichao Xue,Xueli Zheng,Ruixiang Li,Hua Chen,Juan Tang,Haiyan Fu
标识
DOI:10.1021/acs.orglett.6c02036
摘要
A mild and efficient skeletal editing strategy for the synthesis of fully substituted pyrroles from pyridinium salts is described. The transformation proceeds through a sequence of pyridinium salt ring opening, imidation, ring closing, and bromination steps, demonstrating broad substrate scope, good functional group tolerance, and scalability to the gram scale. Mechanistic studies support a pathway involving the regioselective addition of a succinimidyl radical to a Zincke aldehyde intermediate, followed by cyclization and bromination. The resulting pyrrole products are equipped with multiple orthogonal functional handles that enable diverse downstream derivatization.
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