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Vaccination against Streptococcus pneumoniae Using Truncated Derivatives of Polyhistidine Triad Protein D

机译:使用多组氨酸三联体蛋白D的截短衍生物对肺炎链球菌进行疫苗接种

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摘要

Polyhistidine triad protein D (PhtD) has been described as a promising vaccine candidate for use against Streptococcus pneumoniae, but there has been a lack of examination of its structure and of which region(s) of the protein are targeted by protective immune responses. In this study, we purified recombinant truncated derivatives of PhtD and examined their secondary structural composition, as well as their capacity to bind antibodies from polyclonal murine serum generated against the full length protein. This allowed the identification of a particularly immunogenic fragment of PhtD, which was also purified and characterised. The truncated derivatives were tested as vaccine antigens in mouse models of pneumococcal sepsis and colonisation, using alum and E. coli heat labile toxin B subunit respectively as adjuvants. These experiments revealed that whilst the immunogenic region identified may be a promising candidate to protect against sepsis, the full length PhtD was ineffective at conferring significant protective immunity. These results are significant for the potential for PhtD to be used in novel vaccines, which are currently being tested in clinical trials.
机译:聚组氨酸三联体蛋白D(PhtD)被描述为用于抗肺炎链球菌的有前途的疫苗候选者,但缺乏对其结构的检查以及保护性免疫反应靶向该蛋白的哪个区域。在这项研究中,我们纯化了PhtD的重组截短衍生物,并检查了它们的二级结构组成,以及它们结合多克隆鼠血清中针对全长蛋白产生的抗体的能力。这使得可以鉴定出具有特别免疫原性的PhtD片段,该片段也经过了纯化和鉴定。分别使用明矾和大肠杆菌热不稳定毒素B亚基作为佐剂,在肺炎球菌败血症和定殖的小鼠模型中测试了截短的衍生物作为疫苗抗原。这些实验表明,虽然确定的免疫原性区域可能是预防败血症的有前途的候选者,但全长PhtD在赋予重要的保护性免疫方面无效。这些结果对于PhtD在新型疫苗中的应用潜力具有重大意义,目前正在临床试验中对其进行测试。

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