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Conserved Surface Accessible Nucleoside ABC Transporter Component SP0845 Is Essential for Pneumococcal Virulence and Confers Protection In Vivo

机译:保守的表面可及核苷ABC转运蛋白组分SP0845对于肺炎球菌毒力和体内保护至关重要

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摘要

Streptococcus pneumoniae is a leading cause of bacterial pneumonia, sepsis and meningitis. Surface accessible proteins of S. pneumoniae are being explored for the development of a protein-based vaccine in order to overcome the limitations of existing polysaccharide-based pneumococcal vaccines. To identify a potential vaccine candidate, we resolved surface-associated proteins of S. pneumoniae TIGR4 strain using two-dimensional gel electrophoresis followed by immunoblotting with antisera generated against whole heat-killed TIGR4. Ten immunoreactive spots were identified by mass spectrometric analysis that included a putative lipoprotein SP0845. Analysis of the inferred amino acid sequence of sp0845 homologues from 36 pneumococcal strains indicated that SP0845 was highly conserved (>98% identity) and showed less than 11% identity with any human protein. Our bioinformatic and functional analyses demonstrated that SP0845 is the substrate-binding protein of an ATP-binding cassette (ABC) transporter that is involved in nucleoside uptake with cytidine, uridine, guanosine and inosine as the preferred substrates. Deletion of the gene encoding SP0845 renders pneumococci avirulent suggesting that it is essential for virulence. Immunoblot analysis suggested that SP0845 is expressed in in vitro grown pneumococci and during mice infection. Immunofluorescence microscopy and flow cytometry data indicated that SP0845 is surface exposed in encapsulated strains and accessible to antibodies. Subcutaneous immunization with recombinant SP0845 induced high titer antibodies in mice. Hyperimmune sera raised against SP0845 promoted killing of encapsulated pneumococcal strains in a blood bactericidal assay. Immunization with SP0845 protected mice from intraperitoneal challenge with heterologous pneumococcal serotypes. Based on its surface accessibility, role in virulence and ability to elicit protective immunity, we propose that SP0845 may be a potential candidate for a protein-based pneumococcal vaccine.
机译:肺炎链球菌是细菌性肺炎,败血症和脑膜炎的主要原因。为了克服现有的基于多糖的肺炎球菌疫苗的局限性,正在研究肺炎链球菌的表面可及蛋白以开发基于蛋白质的疫苗。为了确定潜在的疫苗候选者,我们使用二维凝胶电泳解析了肺炎链球菌TIGR4菌株的表面相关蛋白,然后用抗血清免疫印迹法对整个热灭活的TIGR4进行了免疫。通过质谱分析鉴定出十个免疫反应斑点,其中包括推定的脂蛋白SP0845。对来自36株肺炎球菌菌株的sp0845同源物推断的氨基酸序列的分析表明,SP0845是高度保守的(> 98%同一性),与任何人类蛋白质的同一性均低于11%。我们的生物信息学和功能分析表明,SP0845是ATP结合盒(ABC)转运蛋白的底物结合蛋白,其参与胞苷,尿苷,鸟苷和肌苷作为优选底物的核苷摄取。编码SP0845的基因的缺失使肺炎链球菌无毒,这表明它对毒力至关重要。免疫印迹分析表明,SP0845在体外生长的肺炎球菌和小鼠感染期间表达。免疫荧光显微镜和流式细胞术数据表明,SP0845表面暴露于封装的菌株中,抗体可及。用重组SP0845进行皮下免疫可在小鼠中诱导高滴度抗体。在血液杀菌试验中,针对SP0845产生的超免疫血清促进了封装的肺炎球菌菌株的杀死。 SP0845免疫可保护小鼠免受腹膜内异种肺炎球菌血清型攻击。基于其表面可及性,在毒力中的作用以及引起保护性免疫的能力,我们建议SP0845可能是基于蛋白质的肺炎球菌疫苗的潜在候选者。

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