TY - JOUR T1 - Rhodium(III)-catalyzed heterocycle synthesis using an internal oxidant: improved reactivity and mechanistic studies. AU - Guimond,Nicolas, AU - Gorelsky,Serge I, AU - Fagnou,Keith, Y1 - 2011/03/31/ PY - 2011/4/2/entrez PY - 2011/4/2/pubmed PY - 2011/8/2/medline SP - 6449 EP - 57 JF - Journal of the American Chemical Society JO - J Am Chem Soc VL - 133 IS - 16 N2 - Directing groups that can act as internal oxidants have recently been shown to be beneficial in metal-catalyzed heterocycle syntheses that undergo C-H functionalization. Pursuant to the rhodium(III)-catalyzed redox-neutral isoquinolone synthesis that we recently reported, we present in this article the development of a more reactive internal oxidant/directing group that can promote the formation of a wide variety of isoquinolones at room temperature while employing low catalyst loadings (0.5 mol %). In contrast to previously reported oxidative rhodium(III)-catalyzed heterocycle syntheses, the new conditions allow for the first time the use of terminal alkynes. Also, it is shown that the use of alkenes, including ethylene, instead of alkynes leads to the room temperature formation of 3,4-dihydroisoquinolones. Mechanistic investigations of this new system point to a change in the turnover limiting step of the catalytic cycle relative to the previously reported conditions. Concerted metalation-deprotonation (CMD) is now proposed to be the turnover limiting step. In addition, DFT calculations conducted on this system agree with a stepwise C-N bond reductive elimination/N-O bond oxidative addition mechanism to afford the desired heterocycle. Concepts highlighted by the calculations were found to be consistent with experimental results. SN - 1520-5126 UR - https://www.unboundmedicine.com/medline/citation/21452842/Rhodium_III__catalyzed_heterocycle_synthesis_using_an_internal_oxidant:_improved_reactivity_and_mechanistic_studies_ L2 - https://doi.org/10.1021/ja201143v DB - PRIME DP - Unbound Medicine ER -