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CD4 T细胞介导曲霉病疫苗的保护作用。

CD4 T Cells Mediate Aspergillosis Vaccine Protection.

作者信息

Diaz-Arevalo Diana, Kalkum Markus

机构信息

Fundación Instituto de Inmunología de Colombia, FIDIC, Carrera 50, #26-20, Bogotá, 111321, Colombia.

Universidad de Ciencias Aplicadas y Ambientales, U.D.C.A,, Bogotá, Colombia.

出版信息

Methods Mol Biol. 2017;1625:281-293. doi: 10.1007/978-1-4939-7104-6_19.

DOI:10.1007/978-1-4939-7104-6_19
PMID:28584997
Abstract

Adaptive effector CD4 T cells play essential roles in the defense against fungal infections, especially against invasive aspergillosis (IA). Such protective CD4 T cells can be generated through immunization with specialized antifungal vaccines, as has been demonstrated for pulmonary Aspergillus fumigatus infections in mouse experiments. Adaptive transfer of fungal antigen-specific CD4 T cells conferred protection onto non-immunized naive mice, an experimental approach that could potentially become a future treatment option for immunosuppressed IA patients, focusing on the ultimate goal to improve their otherwise dim chances for survival. Here, we describe the different techniques to analyze CD4 T cell immune responses after immunization with a recombinant fungal protein. We present three major methods that are used to analyze the role of CD4 T cells in protection against A. fumigatus challenge. They include (1) transplantation of CD4 T cells from vaccinated mice into immunosuppressed naive mice, observing increasing protection of the cell recipients, (2) depletion of CD4 T cells from vaccinated mice, which abolishes vaccine protection, and (3) T cell proliferation studies following stimulation with overlapping synthetic peptides or an intact protein vaccine. The latter can be used to validate immunization status and to identify protective T cell epitopes in vaccine antigens. In the methods detailed here, we used versions of the well-studied Asp f3 protein expressed in a bacterial host, either as the intact full length protein or its N-terminally truncated version, comprised of residues 15-168. However, these methods are generally applicable and can well be adapted to study other protein-based subunit vaccines.

摘要

适应性效应CD4 T细胞在抵御真菌感染,尤其是侵袭性曲霉病(IA)中发挥着重要作用。通过用专门的抗真菌疫苗进行免疫接种,可以产生这种保护性CD4 T细胞,这在小鼠实验中针对肺部烟曲霉感染已得到证实。真菌抗原特异性CD4 T细胞的适应性转移赋予未免疫的幼稚小鼠保护作用,这种实验方法有可能成为免疫抑制IA患者未来的一种治疗选择,其最终目标是改善他们原本渺茫的生存机会。在此,我们描述了用重组真菌蛋白免疫后分析CD4 T细胞免疫反应的不同技术。我们介绍了三种主要方法,用于分析CD4 T细胞在抵御烟曲霉攻击中的作用。它们包括:(1)将接种疫苗小鼠的CD4 T细胞移植到免疫抑制的幼稚小鼠中,观察细胞受体的保护作用增强;(2)从接种疫苗的小鼠中去除CD4 T细胞,这会消除疫苗保护作用;(3)用重叠合成肽或完整蛋白疫苗刺激后进行T细胞增殖研究。后者可用于验证免疫状态并鉴定疫苗抗原中的保护性T细胞表位。在本文详述的方法中,我们使用了在细菌宿主中表达的经过充分研究的Asp f3蛋白的不同版本,要么是完整的全长蛋白,要么是其N端截短版本,由15 - 168位残基组成。然而,这些方法普遍适用,并且可以很好地适用于研究其他基于蛋白的亚单位疫苗。

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