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Polymorphisms in regulator of protease B (RopB) alter disease phenotype and strain virulence of serotype M3 group A Streptococcus
Authors:Olsen Randall J  Laucirica Daniel R  Watkins M Ebru  Feske Marsha L  Garcia-Bustillos Jesus R  Vu Chau  Cantu Concepcion  Shelburne Samuel A  Fittipaldi Nahuel  Kumaraswami Muthiah  Shea Patrick R  Flores Anthony R  Beres Stephen B  Lovgren Maguerite  Tyrrell Gregory J  Efstratiou Androulla  Low Donald E  Van Beneden Chris A  Musser James M
Institution:Department of Pathology and Laboratory Medicine, The Methodist Hospital Research Institute, Houston, TX, USA. rjolsen@tmhs.org
Abstract:Whole-genome sequencing of serotype M3 group A streptococci (GAS) from oropharyngeal and invasive infections in Ontario recently showed that the gene encoding regulator of protease B (RopB) is highly polymorphic in this population. To test the hypothesis that ropB is under diversifying selective pressure among all serotype M3 GAS strains, we sequenced this gene in 1178 strains collected from different infection types, geographic regions, and time periods. The results confirmed our hypothesis and discovered a significant association between mutant ropB alleles, decreased activity of its major regulatory target SpeB, and pharyngitis. Additionally, isoallelic strains with ropB polymorphisms were significantly less virulent in a mouse model of necrotizing fasciitis. These studies provide a model strategy for applying whole-genome sequencing followed by deep single-gene sequencing to generate new insight to the rapid evolution and virulence regulation of human pathogens.
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