What question did this study set out to answer?

This research aims to synthesize γ-sulfoxonium carbonyl compounds via a novel tandem reaction.

February 28, 2026

Synthesis of γ-Carbonyl Aliphatic Sulfoxonium Salts via Site-Selective Ring Opening of In Situ Formed 2-Sulfoxonium Cyclobutanone

Key Points

This research aims to synthesize γ-sulfoxonium carbonyl compounds via a novel tandem reaction.
Utilized Rh-catalyzed tandem reactions.
Reacted pivaloyl-substituted sulfoxonium-iodonium ylides with varied nucleophiles.
Achieved site-selective ring-opening of in situ-generated 2-sulfoxonium cyclobutanone.
Successfully synthesized previously inaccessible γ-sulfoxonium carbonyl compounds.
Displayed mild reaction conditions and broad substrate scope.
Demonstrated scalability and conversion of resulting γ-sulfoxonium amides to γ-lactams.

Abstract

We report herein a Rh-catalyzed tandem reaction between a pivaloyl-substituted sulfoxonium-iodonium ylide and diverse nucleophiles, enabling the efficient synthesis of γ-sulfoxonium carbonyl compounds, which were previously inaccessible. This transformation proceeds through a novel site-selective ring-opening of in situ-generated 2-sulfoxonium cyclobutanone by N-, O-, S-, and Se-centered nucleophiles. The reaction exhibits mild conditions, a broad substrate scope, and excellent scalability. Additionally, the resulting γ-sulfoxonium amides can undergo base-promoted intramolecular cyclization to afford γ-lactams, which are valuable scaffolds in medicinal chemistry.

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Cite This Study

Han et al. (Thu,) studied this question.

synapsesocial.com/papers/69a288170a974eb0d3c04050 https://doi.org/https://doi.org/10.1021/acs.orglett.5c03836

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