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用于肠胃外和粘膜疫苗的佐剂的选择与设计

Choice and Design of Adjuvants for Parenteral and Mucosal Vaccines.

作者信息

Savelkoul Huub F J, Ferro Valerie A, Strioga Marius M, Schijns Virgil E J C

机构信息

Cell Biology and Immunology, Wageningen University, Wageningen, P.O. Box 338, 6700 AH Wageningen, The Netherlands.

Strathclyde Institute of Pharmacy and Biomedical Sciences, University of Strathclyde, 161 Cathedral Street, Glasgow G4 0RE, UK.

出版信息

Vaccines (Basel). 2015 Mar 5;3(1):148-71. doi: 10.3390/vaccines3010148.

Abstract

The existence of pathogens that escape recognition by specific vaccines, the need to improve existing vaccines and the increased availability of therapeutic (non-infectious disease) vaccines necessitate the rational development of novel vaccine concepts based on the induction of protective cell-mediated immune responses. For naive T-cell activation, several signals resulting from innate and adaptive interactions need to be integrated, and adjuvants may interfere with some or all of these signals. Adjuvants, for example, are used to promote the immunogenicity of antigens in vaccines, by inducing a pro-inflammatory environment that enables the recruitment and promotion of the infiltration of phagocytic cells, particularly antigen-presenting cells (APC), to the injection site. Adjuvants can enhance antigen presentation, induce cytokine expression, activate APC and modulate more downstream adaptive immune reactions (vaccine delivery systems, facilitating immune Signal 1). In addition, adjuvants can act as immunopotentiators (facilitating Signals 2 and 3) exhibiting immune stimulatory effects during antigen presentation by inducing the expression of co-stimulatory molecules on APC. Together, these signals determine the strength of activation of specific T-cells, thereby also influencing the quality of the downstream T helper cytokine profiles and the differentiation of antigen-specific T helper populations (Signal 3). New adjuvants should also target specific (innate) immune cells in order to facilitate proper activation of downstream adaptive immune responses and homing (Signal 4). It is desirable that these adjuvants should be able to exert such responses in the context of mucosal administered vaccines. This review focuses on the understanding of the potential working mechanisms of the most well-known classes of adjuvants to be used effectively in vaccines.

摘要

一些病原体能够逃避特定疫苗的识别,同时需要改进现有疫苗,以及治疗性(非感染性疾病)疫苗的可及性增加,这些都使得基于诱导保护性细胞介导免疫反应来合理开发新型疫苗概念成为必要。对于初始T细胞的激活,需要整合先天和适应性相互作用产生的多种信号,而佐剂可能会干扰其中一些或所有信号。例如,佐剂通过诱导促炎环境来促进疫苗中抗原的免疫原性,这种环境能够促使吞噬细胞,特别是抗原呈递细胞(APC)募集并促进其向注射部位浸润。佐剂可以增强抗原呈递、诱导细胞因子表达、激活APC并调节更多下游适应性免疫反应(疫苗递送系统,促进免疫信号1)。此外,佐剂可以作为免疫增强剂(促进信号2和3),在抗原呈递过程中通过诱导APC上共刺激分子的表达发挥免疫刺激作用。这些信号共同决定了特定T细胞激活的强度,从而也影响下游T辅助细胞因子谱的质量以及抗原特异性T辅助细胞群体的分化(信号3)。新型佐剂还应靶向特定的(先天)免疫细胞,以促进下游适应性免疫反应的适当激活和归巢(信号4)。理想的情况是,这些佐剂应能够在黏膜给药疫苗的背景下发挥此类反应。本综述着重于理解最知名的几类佐剂在疫苗中有效使用的潜在作用机制。

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本文引用的文献

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Unleashing the potential of NOD- and Toll-like agonists as vaccine adjuvants.释放NOD样和Toll样激动剂作为疫苗佐剂的潜力。
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Systemic immunotoxicity reactions induced by adjuvanted vaccines.佐剂疫苗引起的全身性免疫毒性反应。
Int Immunopharmacol. 2014 May;20(1):170-80. doi: 10.1016/j.intimp.2014.02.033. Epub 2014 Mar 6.

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