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基于纳米颗粒的治疗性疫苗中不同的细胞内抗原运输促进了细胞和体液反应的协调。

The orchestration of cellular and humoral responses is facilitated by divergent intracellular antigen trafficking in nanoparticle-based therapeutic vaccine.

机构信息

National Key Laboratory of Biochemical Engineering, Institute of Process Engineering, Chinese Academy of Sciences, Beijing, PR China.

出版信息

Pharmacol Res. 2012 Feb;65(2):189-97. doi: 10.1016/j.phrs.2011.09.008. Epub 2011 Oct 1.

DOI:10.1016/j.phrs.2011.09.008
PMID:21983005
Abstract

Therapeutic vaccination for the treatment of chronic hepatitis B is promising but has so far shown limited clinical efficacy. Herein, we employ polylactide nanoparticles (NPs) as the vaccine adjuvant and systematically explore their effect on activation of specific immunity and the underlying theoretical mechanisms. In vitro studies show that hepatitis B surface antigen (HBsAg) accumulates in antigen-presenting cells (APCs) to a larger content (270%) with the assistant of NP in comparison with the pure-antigen group. Besides the elevated costimulators (CD80/86) and increased major histocompatibility complex (MHC) II molecules, the MHC I molecules are also found upregulated. This result is mostly owing to the divergent antigen trafficking ways of NP-antigen in APCs, especially for the escape of exogenous HBsAg from the lysosomes to the cytosol. Interestingly, the MHC I level is downregulated in alum-antigen group, indicating a possible reason for its inefficiency in priming cellular response. Further in vivo experiments establish that NP-antigen group indeed enhances the CD8(+) CTL cytotoxicity and IFN-γ cytokine secretion. Meanwhile, specific antibody titer is also upregulated, and even surpasses that of the commercialized alum-antigen. All these results strongly support that NP-based antigen promotes an orchestration of cellular and humoral immune response, exhibiting favorable intrinsic properties to be applied in therapeutic vaccines.

摘要

治疗性乙型肝炎疫苗治疗具有广阔的前景,但迄今为止,其临床疗效有限。本研究采用聚乳酸纳米颗粒(NPs)作为疫苗佐剂,系统地研究了其对特异性免疫激活的作用及其潜在的理论机制。体外研究表明,与纯抗原组相比,HBsAg 在 NP 辅助下在抗原呈递细胞(APCs)中积累的含量更高(270%)。除了共刺激分子(CD80/86)和主要组织相容性复合物(MHC)II 分子的增加外,还发现 MHC I 分子也上调。这一结果主要归因于 NP-抗原在 APCs 中不同的抗原运输途径,特别是外源性 HBsAg 从溶酶体逃逸到细胞质。有趣的是,铝佐剂-抗原组中 MHC I 水平下调,表明其在刺激细胞反应方面效率低下的可能原因。进一步的体内实验证实,NP-抗原组确实增强了 CD8(+)CTL 的细胞毒性和 IFN-γ细胞因子的分泌。同时,特异性抗体滴度也上调,甚至超过了商品化的铝佐剂。所有这些结果都有力地支持了基于 NP 的抗原能够促进细胞和体液免疫反应的协调,具有良好的内在特性,可应用于治疗性疫苗。

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