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A Schistosoma mansoni fatty acid-binding protein, Sm14, is the potential basis of a dual-purpose anti-helminth vaccine.

机译:曼氏血吸虫脂肪酸结合蛋白Sm14是两用抗蠕虫疫苗的潜在基础。

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摘要

Molecular cloning of components of protective antigenic preparations has suggested that related parasite fatty acid-binding proteins could form the basis of the protective immune crossreactivity between the parasitic trematode worms Fasciola hepatica and Schistosoma mansoni. Molecular models of the two parasite proteins showed that both molecules adopt the same basic three-dimensional structure, consisting of a barrel-shaped molecule formed by 10 antiparallel beta-pleated strands joined by short loops, and revealed the likely presence of crossreactive, discontinuous epitopes principally derived from amino acids in the C-terminal portions of the molecules. A recombinant form of the S. mansoni antigen, rSm14, protected outbred Swiss mice by up to 67% against challenge with S. mansoni cercariae in the absence of adjuvant and without provoking any observable autoimmune response. The same antigen also provided complete protection against challenge with F. hepatica metacercariae in the same animal model. The results suggest that it may be possible to produce a single vaccine that would be effective against at least two parasites, F. hepatica and S. mansoni, of veterinary and human importance, respectively.
机译:保护性抗原制剂组分的分子克隆表明,相关的寄生虫脂肪酸结合蛋白可以构成寄生性吸虫线虫Fasciola hepatica和曼氏血吸虫之间的保护性免疫交叉反应的基础。两种寄生虫蛋白的分子模型显示,两种分子都采用相同的基本三维结构,由桶形分子组成,该桶形分子由10条反平行的β折叠链通过短环连接而成,并揭示了交叉反应性,不连续表位的可能存在主要来自分子C末端部分的氨基酸。曼氏葡萄球菌抗原的重组形式rSm14在不存在佐剂且不引起任何可观察到的自身免疫反应的情况下,可将高达67%的外来瑞士小鼠抵御曼氏葡萄球菌的攻击。在相同的动物模型中,相同的抗原还提供了完全的保护,以抵抗肝尾F的侵染。结果表明,可能有可能生产出一种对至少两种对兽医和人具有重要意义的寄生虫有效的抗肝炎链球菌和曼氏链球菌的疫苗。

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