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Potential recombinant vaccine against influenza A virus based on M2e displayed on nodaviral capsid nanoparticles

机译:潜在的基于M2e的甲型流感病毒重组疫苗展示在结直肠衣壳纳米颗粒上

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摘要

Influenza A virus poses a major threat to human health, causing outbreaks from time to time. Currently available vaccines employ inactivated viruses of different strains to provide protection against influenza virus infection. However, high mutation rates of influenza virus hemagglutinin (H) and neuraminidase (N) glycoproteins give rise to vaccine escape mutants. Thus, an effective vaccine providing protection against all strains of influenza virus would be a valuable asset. The ectodomain of matrix 2 protein (M2e) was found to be highly conserved despite mutations of the H and N glycoproteins. Hence, one to five copies of M2e were fused to the carboxyl-terminal end of the recombinant nodavirus capsid protein derived from Macrobrachium rosenbergii. The chimeric proteins harboring up to five copies of M2e formed nanosized virus-like particles approximately 30 nm in diameter, which could be purified easily by immobilized metal affinity chromatography. BALB/c mice immunized subcutaneously with these chimeric proteins developed antibodies specifically against M2e, and the titer was proportional to the copy numbers of M2e displayed on the nodavirus capsid nanoparticles. The fusion proteins also induced a type 1 T helper immune response. Collectively, M2e displayed on the nodavirus capsid nanoparticles could provide an alternative solution to a possible influenza pandemic in the future.
机译:甲型流感病毒对人类健康构成重大威胁,不时引起暴发。当前可用的疫苗采用不同菌株的灭活病毒来提供针对流感病毒感染的保护。但是,流感病毒血凝素(H)和神经氨酸酶(N)糖蛋白的高突变率产生了疫苗逃逸突变体。因此,提供针对所有流感病毒株的保护的有效疫苗将是有价值的资产。尽管H和N糖蛋白发生突变,但发现基质2蛋白(M2e)的胞外域高度保守。因此,将一到五个拷贝的M2e与源自罗氏沼虾的重组诺达病毒衣壳蛋白的羧基末端融合。带有最多五个拷贝的M2e的嵌合蛋白形成了直径约为30 nm的纳米病毒样颗粒,可以通过固定的金属亲和色谱法轻松纯化。用这些嵌合蛋白皮下免疫的BALB / c小鼠产生了针对M2e的特异性抗体,其滴度与在诺达病毒衣壳纳米颗粒上显示的M2e拷贝数成正比。融合蛋白还诱导了1 T型辅助免疫反应。总的来说,诺达病毒衣壳纳米颗粒上展示的M2e可能为将来可能的流感大流行提供替代解决方案。

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