化学
区域选择性
吲唑
配体(生物化学)
吡唑
电泳剂
三氟乙酸
钯
催化作用
新戊酸
组合化学
联氨(抗抑郁剂)
有机化学
药物化学
受体
生物化学
色谱法
作者
Hyun Tae Kim,Hyeri Ha,Geunhee Kang,Og Soon Kim,Ho Ryu,Abul Kalam Biswas,Sang Min Lim,Mu‐Hyun Baik,Jung Min Joo
标识
DOI:10.1002/ange.201709162
摘要
Abstract Regioselective C4‐, C5‐, and di‐alkenylations of pyrazoles were achieved. An electrophilic Pd catalyst generated by trifluoroacetic acid (TFA) and 4,5‐diazafluoren‐9‐one (DAF) leads to C4‐alkenylation, whereas KOAc and mono‐protected amino acid (MPAA) ligand Ac‐Val‐OH give C5‐alkenylation. A combination of palladium acetate, silver carbonate, and pivalic acid affords dialkenylation products. Annulation through sequential alkenylation, thermal 6π‐electrocyclization, and oxidation gives functionalized indazoles. This comprehensive strategy greatly expands the range of readily accessible pyrazole and indazole derivatives, enabling useful regiodivergent C−H functionalization of pyrazoles and other heteroaromatic systems.
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