Metabolic Engineering Optimizes Bioorthogonal Glycan Labeling in Living Cells

Author:

Cioce Anna,Bineva-Todd Ganka,Agbay Anthony J.ORCID,Choi JunwonORCID,Wood Thomas M.,Debets Marjoke,Browne William,Douglas Holly,Roustan Chloe,Yilmaz Tastan Omur,Kjaer Svend,Bush Jacob T.ORCID,Bertozzi Carolyn,Schumann Benjamin1ORCID

Affiliation:

1. Imperial College London, The Francis Crick Institute

Abstract

Metabolic oligosaccharide engineering (MOE) has fundamentally contributed to our understanding of protein glycosylation. Efficient MOE reagents are activated into nucleotide-sugars by cellular biosynthetic machineries, introduced into glycoproteins and traceable by bioorthogonal chemistry. Despite their widespread use, the metabolic fate of many MOE reagents is only beginning to be mapped. While metabolic interconnectivity can affect probe specificity, poor uptake by biosynthetic salvage pathways may impact probe sensitivity and trigger side reactions. Here, we use metabolic engineering to turn the weak alkyne-tagged MOE reagents Ac4GalNAlk and Ac4GlcNAlk into efficient chemical tools to probe protein glycosylation. We find that bypassing a metabolic bottleneck with an engineered version of the pyrophosphorylase AGX1 boosts nucleotide-sugar biosynthesis and increases bioorthogonal cell surface labeling by up to two orders of magnitude. Comparison with known azide-tagged MOE reagents reveals major differences in glycoprotein labeling, substantially expanding the toolbox of chemical glycobiology.

Publisher

American Chemical Society (ACS)

Cited by 2 articles. 订阅此论文施引文献 订阅此论文施引文献,注册后可以免费订阅5篇论文的施引文献,订阅后可以查看论文全部施引文献

1. Biosynthetic Glycan Labeling;Journal of the American Chemical Society;2021-10-04

2. Benefits of Chemical Sugar Modifications Introduced by Click Chemistry for Glycoproteomic Analyses;Journal of the American Society for Mass Spectrometry;2021-04-19

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