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Host‐ and pathogen‐derived adjuvant coatings on protein nanoparticle vaccines

机译:蛋白纳米颗粒疫苗上的宿主和病原体佐剂涂层

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摘要

Nanoparticulate and molecular adjuvants have shown great efficacy in enhancing immune responses, and the immunogenic vaccines of the future will most likely contain both. To investigate the immunostimulatory effects of molecular adjuvants on nanoparticle vaccines, we have designed ovalbumin (OVA) protein nanoparticles coated with two different adjuvants—flagellin (FliC) and immunoglobulin M (IgM). These proteins, derived from Salmonella and mice, respectively, are representatives of pathogen‐ and host‐derived molecules that can enhance immune responses. FliC‐coated OVA nanoparticles, soluble FliC (sFliC) admixed with OVA nanoparticles, IgM‐coated nanoparticles, and OVA‐coated nanoparticles were assessed for immunogenicity in an in vivo mouse immunization study. IgM coatings on nanoparticles significantly enhanced both antibody and T cell responses, and promoted IgG2a class switching but not affinity maturation. FliC‐coated nanoparticles and FliC‐admixed with nanoparticles both triggered IgG2a class switching, but only FliC‐coated nanoparticles enhanced antibody affinity maturation. Our findings that affinity maturation and class switching can be directed independently of one another suggest that adjuvant coatings on nanoparticles can be tailored to generate specific vaccine effector responses against different classes of pathogens.
机译:纳米颗粒和分子佐剂已显示出增强免疫反应的巨大功效,未来的免疫原性疫苗很可能会同时包含两者。为了研究分子佐剂对纳米颗粒疫苗的免疫刺激作用,我们设计了包被有两种不同佐剂-鞭毛蛋白(FliC)和免疫球蛋白M(IgM)的卵清蛋白(OVA)蛋白纳米颗粒。这些蛋白质分别来自沙门氏菌和小鼠,是可增强免疫反应的病原体和宿主分子的代表。在体内小鼠免疫研究中,评估了FliC包覆的OVA纳米颗粒,与FVA纳米颗粒混合的可溶性FliC(sFliC),IgM包覆的纳米颗粒和OVA包覆的纳米颗粒的免疫原性。纳米颗粒上的IgM涂层可显着增强抗体和T细胞反应,并促进IgG2a类转换,但不能促进亲和力成熟。 FliC包被的纳米颗粒和与FliC混合的纳米颗粒均触发IgG2a类转换,但只有FliC包被的纳米颗粒可增强抗体亲和力成熟度。我们的发现,亲和力成熟和类别转换可以彼此独立地进行,这表明纳米颗粒上的佐剂包衣可以定制以产生针对不同类别病原体的特异性疫苗效应物反应。

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