结核分枝杆菌感染期间抗原特异性CD8 + T细胞与中央记忆的形成

Antigen-specific CD8+ T cells and the development of central memory during Mycobacterium tuberculosis infection.

作者信息

Kamath Arati, Woodworth Joshua S M, Behar Samuel M

机构信息

Division of Rheumatology, Immunology, and Allergy, Brigham and Women's Hospital and Harvard Medical School, One Jimmy Fund Way, Boston, MA 02115, USA.

出版信息

J Immunol. 2006 Nov 1;177(9):6361-9. doi: 10.4049/jimmunol.177.9.6361.

DOI:10.4049/jimmunol.177.9.6361

PMID:17056567

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3133654/

Abstract

Whether true memory T cells develop in the face of chronic infection such as tuberculosis remains controversial. To address this question, we studied CD8+ T cells specific for the Mycobacterium tuberculosis ESAT6-related Ags TB10.3 and TB10.4. The shared epitope TB10.3/10.4(20-28) is presented by H-2 K(d), and 20-30% of the CD8+ T cells in the lungs of chronically infected mice are specific for this Ag following respiratory infection with M. tuberculosis. These TB10.3/10.4(20-28)-specific CD8+ T cells produce IFN-gamma and TNF and express CD107 on their cell surface, which indicates their likely role as CTL in vivo. Nearly all of the Ag-specific CD8+ T cells in the lungs of chronically infected mice had a T effector cell phenotype based on their low expression of CD62L and CD45RB. In contrast, a population of TB10.3/10.4(20-28)-specific CD8+ T cells was identified in the lymphoid organs that express high levels of CD62L and CD45RB. Antibiotic treatment to resolve the infection led to a contraction of the Ag-specific CD8+ T cell population and was accompanied by an increase in the proportion of CD8+ T cells with a central memory phenotype. Finally, challenge of memory-immune mice with M. tuberculosis was accompanied by significant expansion of TB10.3/10.4(20-28)-specific CD8+ T cells, which suggests that these cells are in fact functional memory T cells.

摘要

在诸如结核病等慢性感染情况下，真正的记忆性T细胞是否会产生仍存在争议。为解决这个问题，我们研究了针对结核分枝杆菌ESAT6相关抗原TB10.3和TB10.4的CD8+ T细胞。共同表位TB10.3/10.4(20 - 28)由H-2 K(d)呈递，在结核分枝杆菌呼吸道感染后，慢性感染小鼠肺部20 - 30%的CD8+ T细胞针对该抗原具有特异性。这些TB10.3/10.4(20 - 28)特异性CD8+ T细胞产生干扰素-γ和肿瘤坏死因子，并在其细胞表面表达CD107，这表明它们在体内可能作为细胞毒性T淋巴细胞发挥作用。基于其低水平表达CD62L和CD45RB，慢性感染小鼠肺部几乎所有的抗原特异性CD8+ T细胞都具有效应T细胞表型。相比之下，在淋巴器官中鉴定出一群表达高水平CD62L和CD45RB的TB10.3/10.4(20 - 28)特异性CD8+ T细胞。用于消除感染的抗生素治疗导致抗原特异性CD8+ T细胞群体收缩，并伴随着具有中央记忆表型的CD8+ T细胞比例增加。最后，用结核分枝杆菌攻击具有记忆免疫的小鼠伴随着TB10.3/10.4(20 - 28)特异性CD8+ T细胞的显著扩增，这表明这些细胞实际上是功能性记忆T细胞

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