Rhodium(II)-Catalyzed Hydroamination of Propargylguanidines

M. J. Gainer; N. R. Bennett; Y. Takahashi; R. E. Looper

doi:10.1055/s-0030-1259746

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Synfacts 2011(4): 0374-0374
DOI: 10.1055/s-0030-1259746

Synthesis of Heterocycles

Rhodium(II)-Catalyzed Hydroamination of Propargylguanidines

Contributor(s): Victor Snieckus, Emilie David
M. J. Gainer, N. R. Bennett, Y. Takahashi, R. E. Looper*
University of Utah, Salt Lake City, USA

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Publication History

Publication Date:
18 March 2011 (online)

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Significance

Following a previous lanthanum(III)-catalyzed report on an addition-hydroamination sequence of propargylcyanamides to 2-aminoimidazoles (R. L. Giles, J. D. Sullivan, A. M. Steiner, R. E. Looper Angew. Chem. Int. Ed. 2009, 48, 3116), Looper and co-workers have developed selective 5-exo-dig versus 6-endo-dig hydroamination-cyclization reactions of propargylguanidine derivatives 1 to give products 2 and 3, respectively. Thus, dirhodium(II) carboxylates, such as [Rh₂(oct)₄], as catalysts effect the highly 6-endo-dig-selective hydroamination of propargylguanidines 1 to give products 2, whereas silver(I) in combination with acetic acid proved to be the optimal catalyst for the selective formation of 5-exo-dig products 3. For R^³ = alkyl, catalytic rhodium(II) gave very high selectivity towards the 6-endo-dig products 2, in contrast with the poor selectivity observed for the 5-exo-dig products 3 using catalytic silver(I). For R^³ = aryl, the selectivity is completely reversed depending on the EDG or EWG nature of R^³. Bulky R^³ substituents were not tolerated for the rhodium(II)-catalyzed cyclization, but alkyl alcohols and chlorides were compatible. The nature of R^² on the guanidine nitrogen has modest impact on the selectivity.