Literature DB >> 23888036

A general strategy for the chemoenzymatic synthesis of asymmetrically branched N-glycans.

Zhen Wang1, Zoeisha S Chinoy, Shailesh G Ambre, Wenjie Peng, Ryan McBride, Robert P de Vries, John Glushka, James C Paulson, Geert-Jan Boons.   

Abstract

A systematic, efficient means of producing diverse libraries of asymmetrically branched N-glycans is needed to investigate the specificities and biology of glycan-binding proteins. To that end, we describe a core pentasaccharide that at potential branching positions is modified by orthogonal protecting groups to allow selective attachment of specific saccharide moieties by chemical glycosylation. The appendages were selected so that the antenna of the resulting deprotected compounds could be selectively extended by glycosyltransferases to give libraries of asymmetrical multi-antennary glycans. The power of the methodology was demonstrated by the preparation of a series of complex oligosaccharides that were printed as microarrays and screened for binding to lectins and influenza-virus hemagglutinins, which showed that recognition is modulated by presentation of minimal epitopes in the context of complex N-glycans.

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Year:  2013        PMID: 23888036      PMCID: PMC3826785          DOI: 10.1126/science.1236231

Source DB:  PubMed          Journal:  Science        ISSN: 0036-8075            Impact factor:   47.728


  42 in total

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3.  The influenza A virus hemagglutinin glycosylation state affects receptor-binding specificity.

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  98 in total

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2.  Highly Selective β-Mannosylations and β-Rhamnosylations Catalyzed by Bis-thiourea.

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6.  Hemagglutinin receptor specificity and structural analyses of respiratory droplet-transmissible H5N1 viruses.

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Review 10.  Chemoenzymatic Methods for the Synthesis of Glycoproteins.

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