What question did this study set out to answer?

This research aims to advance ribosomal translation by integrating glycosyl-amino acids for novel glycopeptide discovery.

March 7, 2026

Ribosomal Translation and Display Selection of Cyclic Glycopeptides through Genetic Reprogramming

Key Points

This research aims to advance ribosomal translation by integrating glycosyl-amino acids for novel glycopeptide discovery.
Utilized flexizyme-mediated reprogramming to incorporate glycosyl-amino acids into ribosomal translation.
Applied in vitro mRNA display for the discovery of cyclic glycopeptide ligands.
Focused on inhibitors of P-selectin and agonists of the asialoglycoprotein receptor.
Identified α-l-fucosylated cyclic peptide inhibitors effective against antiplatelet-monocyte aggregation.
Discovered β-d-N-acetylgalactosamine-containing cyclic glycopeptides with strong lysosome trafficking activity.

Abstract

A robust method for the ribosomal incorporation of glycosyl-amino acids through the flexizyme-mediated reprogramming of initiating AUG codons with glycosyl-dipeptides is described. This reprogramming strategy was applied to in vitro mRNA display for the de novo discovery of α-l-fucosylated cyclic peptide inhibitors of P-selectin with antiplatelet-monocyte aggregation activity, and β-d-N-acetylgalactosamine-containing cyclic glycopeptide agonists of the asialoglycoprotein receptor (ASGPR) with potent lysosome trafficking activity. This work provides a powerful platform for the de novo discovery of glycopeptide ligands and expands genetic reprogramming capabilities to large modifications previously intractable for ribosomal translation.

Bookmark

Ribosomal Translation and Display Selection of Cyclic Glycopeptides through Genetic Reprogramming

Key Points

Abstract

Cite This Study