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首页> 外文期刊>International Journal of Nanomedicine >Liposomal nanoparticle-based conserved peptide influenza vaccine and monosodium urate crystal adjuvant elicit protective immune response in pigs
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Liposomal nanoparticle-based conserved peptide influenza vaccine and monosodium urate crystal adjuvant elicit protective immune response in pigs

机译:基于脂质体的保守肽流感疫苗和尿酸一钠晶体佐剂可引起猪的保护性免疫反应

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Background: Influenza (flu) is a constant threat to humans and animals, and vaccination is one of the most effective ways to mitigate the disease. Due to incomplete protection induced by current flu vaccines, development of novel flu vaccine candidates is warranted to achieve greater efficacy against constantly evolving flu viruses. Methods: In the present study, we used liposome nanoparticle (200 nm diameter)-based subunit flu vaccine containing ten encapsulated highly conserved B and T cell epitope peptides to induce protective immune response against a zoonotic swine influenza A virus (SwIAV) H1N1 challenge infection in a pig model. Furthermore, we used monosodium urate (MSU) crystals as an adjuvant and co-administered the vaccine formulation as an intranasal mist to flu-free nursery pigs, twice at 3-week intervals. Results: Liposome peptides flu vaccine delivered with MSU adjuvant improved the hemagglutination inhibition antibody titer and mucosal IgA response against the SwIAV challenge and also against two other highly genetically variant IAVs. Liposomal vaccines also enhanced the frequency of peptides and virus-specific T-helper/memory cells and IFN-γ response. The improved specific cellular and mucosal humoral immune responses in adjuvanted liposomal peptides flu vaccine partially protected pigs from flu-induced fever and pneumonic lesions, and reduced the nasal virus shedding and viral load in the lungs. Conclusion: Overall, our study shows great promise for using liposome and MSU adjuvant-based subunit flu vaccine through the intranasal route, and provides scope for future, pre-clinical investigations in a pig model for developing potent human intranasal subunit flu vaccines.
机译:背景:流感是对人类和动物的持续威胁,而疫苗接种是减轻这种疾病最有效的方法之一。由于当前的流感疫苗诱导的保护作用不完全,因此有必要开发新型流感疫苗候选物,以实现针对不断发展的流感病毒的更高功效。方法:在本研究中,我们使用了基于脂质体纳米颗粒(直径<200 nm)的亚基流感疫苗,其中包含十种封装的高度保守的B和T细胞表位肽,以诱导针对人畜共患性猪A型流感病毒(SwIAV)H1N1攻击的保护性免疫应答猪模型感染。此外,我们使用尿酸一钠(MSU)晶体作为佐剂,并以每3周间隔两次将疫苗制剂作为鼻内雾剂共同施用给无流感的保育猪。结果:佐以MSU佐剂的脂质体流感疫苗改善了血凝抑制抗体的效价和粘膜IgA对SwIAV攻击的抵抗力,以及对另外两种高度遗传变异的IAV的抵抗力。脂质体疫苗还增加了肽和病毒特异性T辅助细胞/记忆细胞以及IFN-γ反应的频率。佐剂脂质体肽流感疫苗中特异性细胞和粘膜体液免疫反应的改善部分保护了猪免受流感引起的发烧和肺炎损害,并减少了鼻部病毒的释放和肺部病毒载量。结论:总体而言,我们的研究表明通过鼻内途径使用脂质体和基于MSU佐剂的亚单位流感疫苗具有广阔的前景,并为未来的临床前研究在猪模型中开发有效的人鼻内亚单位流感疫苗提供了空间。

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