首页> 美国卫生研究院文献>The Journal of Infectious Diseases >Broadly Protective Protein-Based Pneumococcal Vaccine Composed of Pneumolysin Toxoid–CbpA Peptide Recombinant Fusion Protein
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Broadly Protective Protein-Based Pneumococcal Vaccine Composed of Pneumolysin Toxoid–CbpA Peptide Recombinant Fusion Protein

机译:广泛保护蛋白的肺炎球菌疫苗由肺炎球菌溶血毒素类毒素-CbpA肽重组融合蛋白组成。

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摘要

>Background. Pneumococcus, meningococcus, and Haemophilus influenzae cause a similar spectrum of infections in the ear, lung, blood, and brain. They share cross-reactive antigens that bind to the laminin receptor of the blood-brain barrier as a molecular basis for neurotropism, and this step in pathogenesis was addressed in vaccine design.>Methods. Biologically active peptides derived from choline-binding protein A (CbpA) of pneumococcus were identified and then genetically fused to L460D pneumolysoid. The fusion construct was tested for vaccine efficacy in mouse models of nasopharyngeal carriage, otitis media, pneumonia, sepsis, and meningitis.>Results. The CbpA peptide–L460D pneumolysoid fusion protein was more broadly immunogenic than pneumolysoid alone, and antibodies were active in vitro against Streptococcus pneumoniae, Neisseria meningitidis, and H. influenzae. Passive and active immunization protected mice from pneumococcal carriage, otitis media, pneumonia, bacteremia, meningitis, and meningococcal sepsis.>Conclusions. The CbpA peptide–L460D pneumolysoid fusion protein was broadly protective against pneumococcal infection, with the potential for additional protection against other meningeal pathogens.
机译:>背景。肺炎球菌,脑膜炎球菌和流感嗜血杆菌在耳,肺,血液和脑部引起相似的感染谱。它们共享与血脑屏障层粘连蛋白受体结合的交叉反应性抗原,作为神经嗜性的分子基础,这一发病机理已在疫苗设计中得以解决。>方法。鉴定了肺炎球菌的胆碱结合蛋白A(CbpA),然后将其遗传融合到L460D肺炎溶质中。测试了该融合构建体在鼻咽运输,中耳炎,肺炎,败血症和脑膜炎的小鼠模型中的疫苗效力。并且抗体在体外具有抗肺炎链球菌,脑膜炎奈瑟氏球菌和流感嗜血杆菌的活性。被动和主动免疫保护小鼠免受肺炎球菌感染,中耳炎,肺炎,菌血症,脑膜炎和脑膜炎球菌败血症的侵害。对其他脑膜病原体的附加保护。

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