Abstract
The synthesis of isoquinolines by site-selective CH activation of O-acyl oximes with a Cp*CoIII catalyst is described. In the presence of this catalyst, the CH activation of various unsymmetrically substituted O-acyl oximes selectively occurred at the sterically less hindered site, and reactions with terminal as well as internal alkynes afforded the corresponding products in up to 98 % yield. Whereas the reactions catalyzed by the Cp*CoIII system proceeded with high site selectivity (15:1 to 20:1), use of the corresponding Cp*RhIII catalysts led to low selectivities and/or yields when unsymmetrical O-acyl oximes and terminal alkynes were used. Deuterium labeling studies indicate a clear difference in the site selectivity of the CH activation step under Cp*CoIII and Cp*RhIII catalysis.
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