AI Article Synopsis

  • Researchers synthesized biotinylated oligo-α-(1 → 4)-d-galactosamines and their N-acetylated forms using a novel glycosylation method for the first time.
  • These compounds are related to fragments of galactosaminogalactan (GG) from Aspergillus, a significant human fungal pathogen.
  • The glycoconjugates were tested on streptavidin-coated plates to analyze antibody responses in patients with aspergillosis, offering a detailed understanding of immune responses to this complex fungal polysaccharide.

Article Abstract

Using 3--benzoyl-4,6--di--butylsilylidene-2-azido-2-deoxy-selenogalactoside, biotinylated oligo-α-(1 → 4)-d-galactosamines comprising from two to six GalN units were prepared for the first time together with their N-acetylated derivatives. The combination of blocking groups used herein provided stereocontrol for the α-stereospecific glycosylation, to show also high efficiency of phenyl 2-azido-2-deoxy-selenogalactosides as glycosyl donors. The obtained glycoconjugates are related to fragments of exopolysaccharide galactosaminogalactan (GG) found in , which is the most important airborne human fungal pathogen in industrialized countries. The synthesized glycoconjugates were arrayed on streptavidin-coated plates and used to investigate the GG epitopes recognized by mouse monoclonal antibodies against GG and by human antibodies in the sera of patients with aspergillosis. The obtained data showed that the oligo-α-(1 → 4)-d-galactosamines and their N-acetylated derivatives allowed the first precise analysis of the specificity of the antibody responses to this extremely complex fungal polysaccharide.

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Source
http://dx.doi.org/10.1021/jacs.9b11703DOI Listing

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