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首页> 外文期刊>Viral immunology >Segments of puumala hantavirus nucleocapsid protein inserted into chimeric polyomavirus-derived virus-like particles induce a strong immune response in mice.
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Segments of puumala hantavirus nucleocapsid protein inserted into chimeric polyomavirus-derived virus-like particles induce a strong immune response in mice.

机译:插入嵌合多瘤病毒衍生的病毒样颗粒的肺部puumala汉坦病毒核衣壳蛋白片段在小鼠中诱导强烈的免疫反应。

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摘要

Insertion of a short-sized epitope at four different sites of yeast-expressed hamster polyomavirus major capsid protein VP1 has been found to result in the formation of chimeric virus-like particles. Here, we demonstrate that the insertion of 45 or 120 amino acid-long segments from the N-terminus of Puumala hantavirus nucleocapsid protein into sites 1 (amino acids 80-89) and 4 (amino acids 288-295) of VP1 allowed the highly efficient formation of virus-like particles. In contrast, expression level and assembly capacity of fusions to sites 2 (amino acids 222-225) and 3 (amino acids 243-247) were drastically reduced. Immunization of BALB/c mice with chimeric virus-like particles induced a high-titered antibody response against the hantavirus nucleocapsid protein, even in the absence of any adjuvant. The strongest response was observed in mice immunized with virus-like particles harboring 120 amino acids of hantavirus nucleocapsid protein. According to the immunoglobulin subclass distribution of nucleocapsid protein-specific antibodies a mixed Th1/Th2 response was detected. The VP1 carrier itself also induced a mixed Th1/Th2 response, which was found to be reduced in mice immunized with virus-like particles harboring 120 amino acid-long inserts. In conclusion, hamster polyomavirus VP1 represents a promising carrier moiety for future vaccine development.
机译:已经发现在酵母表达的仓鼠多瘤病毒主要衣壳蛋白VP1的四个不同位点插入短表位会导致嵌合病毒样颗粒的形成。在这里,我们证明了从Puumala汉坦病毒核衣壳蛋白N端的N末端插入45或120个氨基酸长的片段到VP1的位点1(氨基酸80-89)和4(氨基酸288-295)允许高度有效形成病毒样颗粒。相反,与位点2(氨基酸222-225)和位点3(氨基酸243-247)的融合物的表达水平和装配能力大大降低。即使没有任何佐剂,用嵌合病毒样颗粒免疫BALB / c小鼠也会诱导针对汉坦病毒核衣壳蛋白的高滴度抗体应答。在用含有120个氨基酸的汉坦病毒核衣壳蛋白的病毒样颗粒免疫的小鼠中观察到最强的反应。根据核衣壳蛋白特异性抗体的免疫球蛋白亚类分布,检测到混合的Th1 / Th2反应。 VP1载体本身也诱导了混合的Th1 / Th2反应,在用含有120个氨基酸长的插入片段的病毒样颗粒免疫的小鼠中,这种反应被降低。总之,仓鼠多瘤病毒VP1代表了未来疫苗开发的有希望的载体部分。

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