Enantioselective Synthesis of Cyclopropanone Equivalents and Application to the Synthesis of β-Lactams

27 December 2019, Version 1
This content is a preprint and has not undergone peer review at the time of posting.

Abstract

Cyclopropanone derivatives have long been considered unsustainable synthetic intermediates due to their extreme strain and kinetic instability. Herein, we report the enantioselective synthesis of 1-sulfonylcyclopropanols as stable yet powerful equivalents of the corresponding cyclopropanone derivatives, via α-hydroxylation of sulfonylcyclopropanes using a bis(silyl) peroxide as electrophilic oxygen source. Both the electronic and steric nature of the sulfonyl moiety, which serves as a base-labile protecting group and confers crystallinity to these cyclopropanone precursors, were found to have a crucial impact on the rate of equilibration to the corresponding cyclopropanone, highlighting the modular nature of these precursors and the potential for their widespread adoption as synthetic intermediates. The utility of these cyclopropanone surrogates is demonstrated in a mild and stereospecific formal [3+1] cycloaddition with simple hydroxylamines acting here as nitrene equivalents, leading to the efficient formation of chiral β-lactam derivatives.

Keywords

Cyclopropanone
β-Lactam antibiotics
silyl peroxides

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