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白细胞介素-7受体在记忆性T细胞上的选择性表达确定了不同CD8 +记忆性T细胞亚群早期依赖CD40L的生成。

Selective expression of IL-7 receptor on memory T cells identifies early CD40L-dependent generation of distinct CD8+ memory T cell subsets.

作者信息

Huster Katharina M, Busch Verena, Schiemann Matthias, Linkemann Kathrin, Kerksiek Kristen M, Wagner Hermann, Busch Dirk H

机构信息

Institute for Medical Microbiology, Immunology, and Hygiene, Technical University of Munich, 81675 Munich, Germany.

出版信息

Proc Natl Acad Sci U S A. 2004 Apr 13;101(15):5610-5. doi: 10.1073/pnas.0308054101. Epub 2004 Mar 25.

DOI:10.1073/pnas.0308054101
PMID:15044705
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC397444/
Abstract

Several recent studies have demonstrated that T-helper cell-dependent events during the initial priming period are required for the generation of CD8(+) T cell-mediated protective immunity. The underlying mechanisms of this phenomenon have not yet been determined, mostly because of difficulties in studying memory T cells or their precursor populations at early stages during immune responses. We identified IL-7 receptor (CD127) surface expression as a marker for long-living memory T cells, most importantly allowing the distinction between memory and effector T cells early after in vivo priming. The combination of surface staining for CD127 and CD62L further separates between two functionally distinct memory cell subsets, which are similar (if not identical) to cell subsets recently described as central memory T cells (CD127(high) and CD62L(high)) and peripheral effector memory T cells (CD127(high) and CD62L(low)). Using this new tool of memory T cell analysis, we demonstrate that CD8(+) T cell priming in the absence of T cell help or CD40L specifically alters the generation of the effector memory T cell subset, which appears to be crucial for immediate memory responses and long-term maintenance of effective protective immunity. Our data reveal a unique strategy to obtain information about the quality of long-term protective immunity early during an immune response, a finding that may be applied in a variety of clinical settings, including the rapid monitoring of vaccination success.

摘要

最近的几项研究表明,初始致敏期依赖辅助性T细胞的事件是产生CD8(+) T细胞介导的保护性免疫所必需的。这种现象的潜在机制尚未确定,主要是因为在免疫反应早期研究记忆T细胞或其前体细胞群存在困难。我们将白细胞介素-7受体(CD127)的表面表达确定为长寿记忆T细胞的标志物,最重要的是,它能在体内致敏后早期区分记忆T细胞和效应T细胞。CD127和CD62L的表面染色相结合,进一步区分了两个功能不同的记忆细胞亚群,它们与最近被描述为中枢记忆T细胞(CD127(高)和CD62L(高))和外周效应记忆T细胞(CD127(高)和CD62L(低))的细胞亚群相似(如果不是完全相同的话)。使用这种记忆T细胞分析的新工具,我们证明在没有T细胞辅助或CD40L的情况下,CD8(+) T细胞致敏会特异性改变效应记忆T细胞亚群的产生,这似乎对即时记忆反应和有效保护性免疫的长期维持至关重要。我们的数据揭示了一种在免疫反应早期获取有关长期保护性免疫质量信息的独特策略,这一发现可能应用于各种临床环境,包括快速监测疫苗接种的成功情况。

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本文引用的文献

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Selective expression of the interleukin 7 receptor identifies effector CD8 T cells that give rise to long-lived memory cells.白细胞介素7受体的选择性表达可识别产生长寿记忆细胞的效应性CD8 T细胞。
Nat Immunol. 2003 Dec;4(12):1191-8. doi: 10.1038/ni1009. Epub 2003 Nov 16.
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Defective CD8 T cell memory following acute infection without CD4 T cell help.急性感染后缺乏CD4 T细胞辅助时CD8 T细胞记忆存在缺陷。
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Requirement for CD4 T cell help in generating functional CD8 T cell memory.生成功能性CD8 T细胞记忆对CD4 T细胞辅助的需求。
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CD4+ T cells are required for secondary expansion and memory in CD8+ T lymphocytes.CD4+ T细胞是CD8+ T淋巴细胞二次扩增和记忆所必需的。
Nature. 2003 Feb 20;421(6925):852-6. doi: 10.1038/nature01441. Epub 2003 Feb 9.
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