What question did this study set out to answer?

This research aims to develop a method for creating cross-linked cyclic peptides using dithiane-alkyne metathesis.

February 13, 2026

Dithiane-Alkyne Metathesis Enables Trp(C2)-Alkene-Cross-Linked Cyclic Peptides

Key Points

This research aims to develop a method for creating cross-linked cyclic peptides using dithiane-alkyne metathesis.
Utilized indium(III) as a catalyst for the metathesis process.
Applied an intramolecular approach to transform linear peptide precursors.
Emphasized operational simplicity and high atom economy in the synthesis.
Achieved exclusive E-selectivity in the formation of cyclic peptides.
Demonstrated broad substrate scope for diverse macrocycle production.
Showed the efficiency of the method in transforming linear precursors.

Abstract

Cyclic peptides represent a privileged class of scaffolds in drug discovery owing to their unique balance between structural rigidity and functional diversity. Herein, we disclose an indium(III)-catalyzed intramolecular dithiane-alkyne metathesis (DAM) that facilitates the efficient construction of Trp(C2)-alkene-cross-linked cyclic peptides with exclusive E-selectivity. This protocol directly transforms linear peptide precursors into diverse macrocycles with broad substrate scope, high atom economy, and operational simplicity. These features establish DAM as a mechanistically distinct and practical peptide stapling strategy.

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Dithiane-Alkyne Metathesis Enables Trp(C2)-Alkene-Cross-Linked Cyclic Peptides

Key Points

Abstract

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