The β-galactosidase (BgaC) of the Zoonotic Pathogen Streptococcus Suis is a Surface Protein Without the Involvement of Bacterial Virulence

Overview

Journal Sci Rep

Specialty Science

Date 2014 Feb 22

PMID 24556915

Citations 6

Authors

Dan Hu

Fengyu Zhang

Huimin Zhang

Lina Hao

Xiufang Gong

Meiling Geng

Min Cao

Feng Zheng

Jin Zhu

Xiuzhen Pan

Jiaqi Tang

Youjun Feng

Changjun Wang

Affiliations

Soon will be listed here.

Abstract

Streptococcal pathogens have evolved to express exoglycosidases, one of which is BgaC β-galactosidase, to deglycosidate host surface glycolconjucates with exposure of the polysaccharide receptor for bacterial adherence. The paradigm BgaC protein is the bgaC product of Streptococcus, a bacterial surface-exposed β-galactosidase. Here we report the functional definition of the BgaC homologue from an epidemic Chinese strain 05ZYH33 of the zoonotic pathogen Streptococcus suis. Bioinformatics analyses revealed that S. suis BgaC shared the conserved active sites (W240, W243 and Y454). The recombinant BgaC protein of S. suis was purified to homogeneity. Enzymatic assays confirmed its activity of β-galactosidase. Also, the hydrolysis activity was found to be region-specific and sugar-specific for the Gal β-1,3-GlcNAc moiety of oligosaccharides. Flow cytometry analyses combined with immune electron microscopy demonstrated that S. suis BgaC is an atypical surface-anchored protein in that it lacks the "LPXTG" motif for typical surface proteins. Integrative evidence from cell lines and mice-based experiments showed that an inactivation of bgaC does not significantly impair the ability of neither adherence nor anti-phagocytosis, and consequently failed to attenuate bacterial virulence, which is somewhat similar to the scenario seen with S. pneumoniae. Therefore we concluded that S. suis BgaC is an atypical surface-exposed protein without the involvement of bacterial virulence.

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