化学
选择性
颠倒
吡啶
催化作用
配体(生物化学)
烷氧基
组合化学
立体化学
药物化学
有机化学
受体
生物化学
复合材料
材料科学
烷基
作者
Luo‐Yan Liu,Jennifer X. Qiao,Kap‐Sun Yeung,William R. Ewing,Jin‐Quan Yu
摘要
Controlling site selectivity of C-H activation without using a directing group remains a significant challenge. While Pd(II) catalysts modulated by a mutually repulsive pyridine-type ligand have been shown to favor the relatively electron-rich carbon centers of arenes, reversing the selectivity to favor palladation at the relatively electron-deficient positions has not been possible. Herein we report the first catalytic system that effectively performs meta C-H arylation of a variety of alkoxy aromatics including 2,3-dihydrobenzofuran and chromane with exclusive meta site selectivity, thus reversing the conventional site selectivity governed by native electronic effects. The identification of an effective ligand and modified norbornene (NBE-CO2Me), as well as taking advantage of the statistics, are essential for achieving the exclusive meta selectivity.
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