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纳米颗粒疫苗中持续抗原释放在塑造 T 细胞记忆表型中的作用。

Role of sustained antigen release from nanoparticle vaccines in shaping the T cell memory phenotype.

机构信息

Department of Biomedical Engineering, Yale University, New Haven, CT-06511, USA.

出版信息

Biomaterials. 2012 Jun;33(19):4957-64. doi: 10.1016/j.biomaterials.2012.03.041. Epub 2012 Apr 6.

Abstract

Particulate vaccines are emerging promising technologies for the creation of tunable prophylactics against a wide variety of conditions. Vesicular and solid biodegradable polymer platforms, exemplified by liposomes and polyesters, respectively, are two of the most ubiquitous platforms in vaccine delivery studies. Here we directly compared the efficacy of each in a long-term immunization study and in protection against a model bacterial antigen. Immunization with poly(lactide-co-glycolide) (PLGA) nanoparticles elicited prolonged antibody titers compared to liposomes and alum. The magnitude of the cellular immune response was also highest in mice vaccinated with PLGA, which also showed a higher frequency of effector-like memory T cell phenotype, leading to an effective clearance of intracellular bacteria. The difference in performance of these two common particulate platforms is shown not to be due to material differences but appears to be connected to the kinetics of antigen delivery. Thus, this study highlights the importance of sustained antigen release mediated by particulate platforms and its role in the long-term appearance of effector memory cellular response.

摘要

微粒疫苗是一种新兴的有前途的技术,可用于针对多种疾病定制预防性疫苗。囊泡和固体可生物降解聚合物平台,分别以脂质体和聚酯为例,是疫苗输送研究中最常见的两种平台。在这里,我们在一项长期免疫研究中直接比较了每种平台的功效,并比较了它们在预防模型细菌抗原方面的效果。与脂质体和铝佐剂相比,聚(乳酸-共-乙醇酸)(PLGA)纳米颗粒的免疫接种可引起长期的抗体滴度升高。用 PLGA 接种疫苗的小鼠中的细胞免疫应答的幅度也最高,并且还显示出更高频率的效应样记忆 T 细胞表型,从而有效地清除了细胞内细菌。这两种常见的微粒平台的性能差异不是由于材料差异引起的,而似乎与抗原传递的动力学有关。因此,这项研究强调了微粒平台介导的持续抗原释放的重要性及其在效应记忆细胞反应的长期出现中的作用。

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