Automated glycan assembly of Streptococcus pneumoniae type 14 capsular polysaccharide fragments

João Louçano; Peter Both; Andrea Marchesi; Linda Del Bino; Roberto Adamo; Sabine Flitsch; Mario Salwiczek

doi:10.1039/d0ra01803a

Automated glycan assembly of Streptococcus pneumoniae type 14 capsular polysaccharide fragments

RSC Adv. 2020 Jun 22;10(40):23668-23674. doi: 10.1039/d0ra01803a. eCollection 2020 Jun 19.

Authors

João Louçano¹, Peter Both², Andrea Marchesi², Linda Del Bino³, Roberto Adamo³, Sabine Flitsch², Mario Salwiczek¹

Affiliations

¹ GlycoUniverse GmbH & Co KGaA Am Mühlenberg 11 14476 Potsdam Germany m.salwiczek@glycouniverse.de.
² School of Chemistry, University of Manchester, Manchester Institute of Biotechnology 131 Princess Street Manchester M1 7DN UK.
³ GSK Via Fiorentina 1 53100 Siena Italy.

Abstract

S. pneumoniae is a major human pathogen with increasing antibiotic resistance. Pneumococcal vaccines consist of capsular polysaccharide (CPS) or their related fragments conjugated to a carrier protein. The repeating unit of S. pneumoniae type 14 CPS shares a core structure with the CPS of Group B Streptococcus (GBS) type III: the only difference is that the latter exhibits a sialic acid unit, with a α-2,3 linkage to galactose. Here, the automated glycan assembly (AGA) of two frameshifts of the repeating unit of S. pneumoniae type 14 is described. The same strategy is used to assemble dimers of the different repeating unit frameshifts. The four structures are assembled with only three commercially available monosaccharide building blocks. We also report an example of how enzymatic sialylation of the compounds obtained with AGA completes a synthetic route for GBS type III glycans. The synthesized structures were tested in competitive ELISA and further confirmed the branched tetrasaccharide Gal-Glc-(Gal-)GlcNAc to be the minimal epitope of S. pneumoniae type 14.