Nitrones alkynylated, formation

The CDC between A-f-butyl nitrones and terminal alkynes to form alkynylated nitrones in good to excellent yields, catalysed by zinc trifiate, was achieved using 3,3, 5,5 -tetra-tertbutyldipheno-quinone and O2 as oxidants. The alkynylated nitrones were transformed to regioisomerically pure 3,5-disubstituted isoxazoles. Experimental and DFT computational studies of Pd(OAc)2/pyridine-catalysed intramolecular aerobic oxidative amination of alkenes supported a stepwise mechanism that involved (i) the formation of a Pd(ll)-amidate-alkene chelate with release of 1 equiv. of pyridine and AcOH from the catalyst centre, (ii) insertion of alkene into a Pd—N bond. 

In particular, the reactions of electrophilically activated benzonitrile A-oxides with 3-methylenephthalimidines with formation of 2-isoxazolines and oximes and the cycloaddition between alkynyl metal(O) Fischer carbenes and nitrones leading to 4-isoxazolines have been investigated by density functional theory methods <06JOC9319 06JOC6178>. 

The intramolecular nitrone-alkene cycloaddition reaction of monocyclic 2-azetidinone-tethered alkenyl(alkynyl) aldehydes 211, 214, and 216 with Ar-aIkylhydroxylamincs has been developed as an efficient route to prepare carbacepham derivatives 212, 215, and 217, respectively (Scheme 40). Bridged cycloadducts 212 were further transformed into l-amino-3-hydroxy carbacephams 213 by treatment with Zn in aqueous acetic acid at 75 °C. The aziridine carbaldehyde 217 may arise from thermal sigmatropic rearrangement. However, formation of compound 215 should be explained as the result of a formal reverse-Cope elimination reaction of the intermediate ct-hydroxy-hydroxylamine C1999TL5391, 2000TL1647, 2005EJ01680>. 

The formation of bicyclic nitrones of the 2-azetidinone A-oxide type, 32 and (33), has been achieved in a two-step route, through condensation of the corresponding 2-azetidinone tethered-alkenyl(alkynyl)aldehyde with hydroxylamine followed by phenylselenyl bromide treatment <02JOC7004>. 

Influenced by the ZnMe2-assisted addition of terminal aJkynes to nitrones developed by Chavant et al. [119,120], Micouin et al. performed the same type of reaction using AlMes and obtained several propargylic hydroxylamines [121], For a stereoselective variant, Desvergnes, Py, et al. prepared the carbohydrate-derived nitrone 74, but only achieved high diastereoselectivities in the additirm of phenylacetylene (Scheme 14b) [122]. Moreover, the preformed alkynyl alane had to be used because in situ formation from AlMes and the aUcyne predominantly led to methyl addition. From the reaction of stereoisomeric nitrones of the type 74, it was concluded that the diastereoselectivity solely depended on the configuration at C-3. 

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