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Mycoplasma polysaccharide protects against complement

Authors :
Jeffrey R. Bolland
James M. Daubenspeck
Warren L. Simmons
Kevin Dybvig
Source :
Microbiology. 158:1867-1873
Publication Year :
2012
Publisher :
Microbiology Society, 2012.

Abstract

Although they lack a cell wall, mycoplasmas do possess a glycocalyx. The interactions between the glycocalyx, mycoplasmal surface proteins and host complement were explored using the murine pathogen Mycoplasma pulmonis as a model. It was previously shown that the length of the tandem repeat region of the surface lipoprotein Vsa is associated with susceptibility to complement-mediated killing. Cells producing a long Vsa containing about 40 repeats are resistant to complement, whereas strains that produce a short Vsa of five or fewer repeats are susceptible. We show here that the length of the Vsa protein modulates the affinity of the M. pulmonis EPS-I polysaccharide for the mycoplasma cell surface, with more EPS-I being associated with mycoplasmas producing a short Vsa protein. An examination of mutants that lack EPS-I revealed that planktonic mycoplasmas were highly susceptible to complement killing even when the Vsa protein was long, demonstrating that both EPS-I and Vsa length contribute to resistance. In contrast, the mycoplasmas were resistant to complement even in the absence of EPS-I when the cells were encased in a biofilm.

Details

ISSN :
14652080 and 13500872
Volume :
158
Database :
OpenAIRE
Journal :
Microbiology
Accession number :
edsair.doi.dedup.....ae2bc9697bcc92e2712683666f10a693
Full Text :
https://doi.org/10.1099/mic.0.058222-0