Convergent chemo-enzymatic synthesis of mannosylated glycopeptides; targeting of putative vaccine candidates to antigen presenting cells.

نویسندگان

  • Julie D McIntosh
  • Margaret A Brimble
  • Anna E S Brooks
  • P Rod Dunbar
  • Renata Kowalczyk
  • Yusuke Tomabechi
  • Antony J Fairbanks
چکیده

The combination of solid phase peptide synthesis and endo-β-N-acetylglucosaminidase (ENGase) catalysed glycosylation is a powerful convergent synthetic method allowing access to glycopeptides bearing full-length N-glycan structures. Mannose-terminated N-glycan oligosaccharides, produced by either total or semi-synthesis, were converted into oxazoline donor substrates. A peptide from the human cytomegalovirus (CMV) tegument protein pp65 that incorporates a well-characterised T cell epitope, containing N-acetylglucosamine at specific Asn residues, was accessed by solid phase peptide synthesis, and used as an acceptor substrate. High-yielding enzymatic glycosylation afforded glycopeptides bearing defined homogeneous high-mannose N-glycan structures. These high-mannose containing glycopeptides were tested for enhanced targeting to human antigen presenting cells (APCs), putatively mediated via the mannose receptor, and for processing by the APCs for presentation to human CD8+ T cells specific for a 9-mer epitope within the peptide. Binding assays showed increased binding of glycopeptides to APCs compared to the non-glycosylated control. Glycopeptides bearing high-mannose N-glycan structures at a single site outside the T cell epitope were processed and presented by the APCs to allow activation of a T cell clone. However, the addition of a second glycan within the T cell epitope resulted in ablation of T cell activation. We conclude that chemo-enzymatic synthesis of mannosylated glycopeptides enhances uptake by human APCs while preserving the immunogenicity of peptide epitopes within the glycopeptides, provided those epitopes are not themselves glycosylated.

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منابع مشابه

Convergent chemo-enzymatic synthesis of mannosylated glycopeptides; targeting of putative vaccine candidates to antigen presenting cells† †Electronic supplementary information (ESI) available: Experimental details for the synthesis of all peptides and glycopeptides and spectra. See DOI: 10.1039/c5sc00952a Click here for additional data file.

School of Chemical Sciences, The Universit New Zealand. E-mail: m.brimble@auckland School of Biological Sciences, University of 1142, New Zealand. E-mail: r.dunbar@auck Department of Chemistry, University of Can 8140, New Zealand. E-mail: antony.fairban Maurice Wilkins Centre for Molecular Biod Bag 92019, Auckland 1010, New Zealand † Electronic supplementary information ( the synthesis of all p...

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عنوان ژورنال:
  • Chemical science

دوره 6 8  شماره 

صفحات  -

تاریخ انتشار 2015