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Recognition of specific sialoglycan structures by oral streptococci impacts the severity of endocardial infection

机译:口服链球菌对特定唾液酸聚糖结构的识别影响心内膜感染的严重性

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Streptococcus gordonii and Streptococcus sanguinis are primary colonizers of the tooth surface. Although generally non-pathogenic in the oral environment, they are a frequent cause of infective endocarditis. Both streptococcal species express a serine-rich repeat surface adhesin that mediates attachment to sialylated glycans on mucin-like glycoproteins, but the specific sialoglycan structures recognized can vary from strain to strain. Previous studies have shown that sialoglycan binding is clearly important for aortic valve infections caused by some S. gordonii, but this process did not contribute to the virulence of a strain of S. sanguinis. However, these streptococci can bind to different subsets of sialoglycan structures. Here we generated isogenic strains of S. gordonii that differ only in the type and range of sialoglycan structures to which they adhere and examined whether this rendered them more or less virulent in a rat model of endocarditis. The findings indicate that the recognition of specific sialoglycans can either enhance or diminish pathogenicity. Binding to sialyllactosamine reduces the initial colonization of mechanically-damaged aortic valves, whereas binding to the closely-related trisaccharide sialyl T-antigen promotes higher bacterial densities in valve tissue 72 hours later. A surprising finding was that the initial attachment of streptococci to aortic valves was inversely proportional to the affinity of each strain for platelets, suggesting that binding to platelets circulating in the blood may divert bacteria away from the endocardial surface. Importantly, we found that human and rat platelet GPIbα (the major receptor for S. gordonii and S. sanguinis on platelets) display similar O-glycan structures, comprised mainly of a di-sialylated core 2 hexasaccharide, although the rat GPIbα has a more heterogenous composition of modified sialic acids. The combined results suggest that streptococcal interaction with a minor O-glycan on GPIbα may be more important than the over-all affinity for GPIbα for pathogenic effects.
机译:戈登氏链球菌和血红链球菌是牙齿表面的主要定居者。尽管通常在口腔环境中无致病性,但它们是感染性心内膜炎的常见原因。两种链球菌都表达富含丝氨酸的重复表面粘附素,该粘附素介导粘蛋白样糖蛋白上唾液酸化聚糖的附着,但是所识别的特定唾液酸聚糖结构因菌株而异。先前的研究表明,唾液酸聚糖的结合对于某些戈登氏链球菌引起的主动脉瓣感染显然很重要,但该过程并未导致血红链球菌菌株的毒性。但是,这些链球菌可以结合唾液酸聚糖结构的不同子集。在这里,我们产生了戈登氏链球菌的同基因菌株,它们仅在它们所粘附的唾液酸聚糖结构的类型和范围上有所不同,并检查了这是否使它们在心内膜炎的大鼠模型中或多或少地具有毒性。研究结果表明,对特定唾液聚糖的识别可以增强或减少致病性。结合唾液酸乳糖胺减少了机械损伤的主动脉瓣膜的最初定植,而与紧密相关的三糖唾液酸T-抗原的结合则在72小时后促进了瓣膜组织中更高的细菌密度。令人惊讶的发现是,链球菌与主动脉瓣的初始附着与每种菌株对血小板的亲和力成反比,这表明与血液中循环的血小板的结合可能会使细菌从心内膜表面转移出去。重要的是,我们发现人和大鼠的血小板GPIbα(血小板中的S. gordonii和S.sanguinis的主要受体)显示出相似的O-聚糖结构,主要由二唾液酸化的核心2六糖组成,尽管大鼠GPIbα具有更多的改性唾液酸的异质组成。综合结果表明,链球菌与少量O-聚糖对GPIbα的相互作用可能比对GPIbα的总体致病性亲和力更为重要。

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