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Immune responses and protection induced by mucosal and systemic immunisation with recombinant measles nucleoprotein in a mouse model of measles virus-induced encephalitis.

机译:在麻疹病毒引起的脑炎的小鼠模型中,用重组麻疹核蛋白进行粘膜和全身免疫诱导的免疫应答和保护作用。

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In this study the immunogenicity of recombinant nucleoprotein (Np) administered intranasally or intraperitoneally, and its ability to support a systemic protective anti-virus antibody response was examined, in a mouse model of measles virus (MV)-induced encephalitis. Although both intranasal and intraperitoneal routes of immunisation resulted in priming Np- and MV-specific T-cell responses, the intraperitoneal route was shown to prime for a predominantly IgG2a serum anti-MV antibody response of high avidity, which confered complete protection following intracranial challenge with a neuroadapted strain of MV. On the other hand, intranasal priming resulted in a mixed IgG1, IgG2a serum anti-MV antibody response of low avidity, and only 43% of immunised mice survived following intracranial challenge with the neuroadapted strain of MV. These findings suggest that the route of immunisation in combination with an appropriate adjuvant could influence the induction of a quality antibody response with protective capacity.
机译:在这项研究中,在麻疹病毒(MV)诱发的脑炎小鼠模型中,对经鼻腔或腹膜内给予的重组核蛋白(Np)的免疫原性及其支持全身保护性抗病毒抗体应答的能力进行了研究。尽管鼻内和腹膜内免疫途径均引发了Np和MV特异性T细胞反应,但腹膜内途径显示出主要针对高亲和力的IgG2a血清抗MV抗体反应,在颅内攻击后赋予了完全保护具有神经适应性的MV菌株。另一方面,鼻内引发导致低亲和力的混合IgG1,IgG2a血清抗MV抗体反应,颅内攻击MV后,只有43%的免疫小鼠存活下来。这些发现表明,与适当佐剂结合的免疫途径可能影响具有保护能力的优质抗体应答的诱导。

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