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针对树突状细胞的 HIV-1 疫苗改进策略。

Targeting dendritic cells for improved HIV-1 vaccines.

机构信息

Department of Microbiology, Tumor, and Cell Biology, Karolinska Institutet, Stockholm, Sweden.

出版信息

Adv Exp Med Biol. 2013;762:263-88. doi: 10.1007/978-1-4614-4433-6_10.

DOI:10.1007/978-1-4614-4433-6_10
PMID:22975879
Abstract

As dendritic cells (DCs) have the unique capacity to activate antigen-naive T cells they likely play a critical role in eliciting immune responses to vaccines. DCs are therefore being explored as attractive targets for vaccines, but understanding the interaction of DCs and clinically relevant vaccine antigens and adjuvants is a prerequisite. The HIV-1/AIDS epidemic continues to be a significant health problem, and despite intense research efforts over the past 30 years a protective vaccine has not yet been developed. A common challenge in vaccine design is to find a vaccine formulation that best shapes the immune response to protect against and/or control the given pathogen. Here, we discuss the importance of understanding the diversity, anatomical location and function of different human DC subsets in order to identify the optimal target cells for an HIV-1 vaccine. We review human DC interactions with some of the HIV-1 vaccine antigen delivery vehicles and adjuvants currently utilized in preclinical and clinical studies. Specifically, the effects of distinctly different vaccine adjuvants in terms of activation of DCs and improving DC function and vaccine efficacy are discussed. The susceptibility and responses of DCs to recombinant adenovirus vectors are reviewed, as well as the strategy of directly targeting DCs by using DC marker-specific monoclonal antibodies coupled to an antigen.

摘要

树突状细胞(DCs)具有激活抗原初始 T 细胞的独特能力,因此它们可能在引发疫苗免疫反应中发挥关键作用。因此,DCs 被探索作为疫苗的有吸引力的靶点,但理解 DCs 与临床相关的疫苗抗原和佐剂的相互作用是先决条件。HIV-1/AIDS 疫情仍然是一个重大的健康问题,尽管过去 30 年来进行了密集的研究,但仍未开发出保护性疫苗。疫苗设计的一个共同挑战是找到最佳的疫苗配方,以塑造免疫反应,从而预防和/或控制给定的病原体。在这里,我们讨论了了解不同人类 DC 亚群的多样性、解剖位置和功能的重要性,以确定 HIV-1 疫苗的最佳靶细胞。我们回顾了人类 DC 与目前在临床前和临床研究中使用的一些 HIV-1 疫苗抗原传递载体和佐剂的相互作用。具体讨论了不同疫苗佐剂在激活 DCs 以及改善 DC 功能和疫苗疗效方面的作用。还回顾了 DCs 对重组腺病毒载体的易感性和反应,以及使用与抗原偶联的 DC 标记物特异性单克隆抗体直接靶向 DCs 的策略。

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Targeting dendritic cells for improved HIV-1 vaccines.针对树突状细胞的 HIV-1 疫苗改进策略。
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Increased generation of HIV-1 gp120-reactive CD8+ T cells by a DNA vaccine construct encoding the chemokine CCL3.通过编码趋化因子CCL3的DNA疫苗构建体增加HIV-1 gp120反应性CD8 + T细胞的生成。
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