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基于聚合物的微粒疫苗佐剂的合理设计。

Rational design of polymer-based particulate vaccine adjuvants.

机构信息

Adjuvant Research Group, School of Biochemistry and Immunology, Trinity Biomedical Sciences Institute, Trinity College Dublin, Dublin, Ireland.

Centre for Research on Adaptive Nanostructures and Nanodevices (CRANN) & Advanced Materials Bio-Engineering Research Centre (AMBER), Trinity College Dublin, Dublin, Ireland.

出版信息

Eur J Immunol. 2024 Feb;54(2):e2350512. doi: 10.1002/eji.202350512. Epub 2023 Dec 3.

DOI:10.1002/eji.202350512
PMID:37994660
Abstract

Vaccination is considered one of the major milestones in modern medicine, facilitating the control and eradication of life-threatening infectious diseases. Vaccine adjuvants are a key component of many vaccines, serving to steer antigen-specific immune responses and increase their magnitude. Despite major advances in the field of adjuvant research over recent decades, our understanding of their mechanism of action remains incomplete. This hinders our capacity to further improve these adjuvant technologies, so addressing how adjuvants induce and control the induction of innate and adaptive immunity is a priority. Investigating how adjuvant physicochemical properties, such as size and charge, exert immunomodulatory effects can provide valuable insights and serve as the foundation for the rational design of vaccine adjuvants. Most clinically applied adjuvants are particulate in nature and polymeric particulate adjuvants present advantages due to stability, biocompatibility profiles, and flexibility in terms of formulation. These properties can impact on antigen release kinetics and biodistribution, cellular uptake and targeting, and drainage to the lymphatics, consequently dictating the induction of innate, cellular, and humoral adaptive immunity. A current focus is to apply rational design principles to the development of adjuvants capable of eliciting robust cellular immune responses including CD8 cytotoxic T-cell and Th1-biased CD4 T-cell responses, which are required for vaccines against intracellular pathogens and cancer. This review highlights recent advances in our understanding of how particulate adjuvants, especially polymer-based particulates, modulate immune responses and how this can be used as a guide for improved adjuvant design.

摘要

疫苗接种被认为是现代医学的主要里程碑之一,有助于控制和消灭危及生命的传染病。疫苗佐剂是许多疫苗的关键组成部分,用于引导抗原特异性免疫反应并增加其规模。尽管近几十年来在佐剂研究领域取得了重大进展,但我们对其作用机制的理解仍然不完整。这阻碍了我们进一步改进这些佐剂技术的能力,因此,了解佐剂如何诱导和控制先天免疫和适应性免疫的诱导是当务之急。研究佐剂的物理化学特性(如大小和电荷)如何发挥免疫调节作用,可以提供有价值的见解,并为疫苗佐剂的合理设计提供基础。大多数临床应用的佐剂都是颗粒状的,而聚合颗粒佐剂由于其稳定性、生物相容性和制剂方面的灵活性而具有优势。这些特性可以影响抗原释放动力学和生物分布、细胞摄取和靶向以及向淋巴引流,从而决定先天、细胞和体液适应性免疫的诱导。目前的重点是应用合理设计原则来开发能够引发强大细胞免疫反应的佐剂,包括 CD8 细胞毒性 T 细胞和 Th1 偏向性 CD4 T 细胞反应,这是针对细胞内病原体和癌症疫苗所必需的。本文综述了我们对颗粒佐剂(特别是基于聚合物的颗粒)如何调节免疫反应的理解的最新进展,以及如何将其用于指导改进佐剂设计。

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