posted on 2011-12-16, 00:00authored byYanke Liang, Nathan Hnatiuk, John M. Rowley, Bryan
T. Whiting, Geoffrey W. Coates, Paul R. Rablen, Martha Morton, Amy R. Howell
The first psico-oxetanocin analogue
of the powerful
antiviral natural product, oxetanocin A, has been readily synthesized
from cis-2-butene-1,4-diol. Key 2-methyleneoxetane
precursors were derived from β-lactones prepared by the carbonylation
of epoxides. F+-mediated nucleobase incorporation provided
the corresponding nucleosides in good yield but with low diastereoselectivity.
Surprisingly, attempted exploitation of anchimeric assistance to increase
the selectivity was not fruitful. A range of 2-methyleneoxetane and
related 2-methylenetetrahydrofuran substrates was prepared to explore
the basis for this. With one exception, these substrates also showed
little stereoselectivity in nucleobase incorporation. Computational
studies were undertaken to examine if neighboring group participation
involving fused [4.2.0] or [4.3.0] intermediates is favorable.