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Design of a protective single-dose intranasal nanoparticle-based vaccine platform for respiratory infectious diseases

机译:基于保护性单剂量鼻内纳米颗粒的呼吸道传染病疫苗平台的设计

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摘要

Despite the successes provided by vaccination, many challenges still exist with respect to controlling new and re-emerging infectious diseases. Innovative vaccine platforms composed of adaptable adjuvants able to appropriately modulate immune responses, induce long-lived immunity in a single dose, and deliver immunogens in a safe and stable manner via multiple routes of administration are needed. This work describes the development of a novel biodegradable polyanhydride nanoparticle-based vaccine platform administered as a single intranasal dose that induced long-lived protective immunity against respiratory disease caused by Yesinia pestis, the causative agent of pneumonic plague. Relative to the responses induced by the recombinant protein F1-V alone and MPLA-adjuvanted F1-V, the nanoparticle-based vaccination regimen induced an immune response that was characterized by high titer and high avidity IgG1 anti-F1-V antibody that persisted for at least 23 weeks post-vaccination. After challenge, no Y. pestis were recovered from the lungs, livers, or spleens of mice vaccinated with the nanoparticle-based formulation and histopathological appearance of lung, liver, and splenic tissues from these mice post-vaccination was remarkably similar to uninfected control mice.
机译:尽管接种疫苗取得了成功,但在控制新的和重新出现的传染病方面仍然存在许多挑战。需要由适应性佐剂组成的创新疫苗平台,这些佐剂能够适当地调节免疫反应,以单剂量诱导长期免疫,并通过多种给药途径以安全,稳定的方式递送免疫原。这项工作描述了一种新型的可生物降解的基于聚酸酐纳米颗粒的疫苗平台的开发,该平台以单次鼻内剂量给药,可诱导长期抵抗由鼠疫鼠疫所引起的呼吸道疾病的保护性免疫力。相对于仅由重组蛋白F1-V和佐以MPLA的F1-V诱导的应答,基于纳米颗粒的疫苗接种方案诱导了以高滴度和高亲和力的IgG1抗F1-V抗体为特征的免疫应答。接种后至少23周。攻击后,未从接种了纳米颗粒制剂的小鼠的肺,肝或脾中回收鼠疫耶尔森氏菌,接种后这些小鼠的肺,肝和脾组织的组织病理学外观与未感染的对照小鼠非常相似。

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