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小鼠(CD8 +)CD27 - T细胞的特性。

Properties of murine (CD8+)CD27- T cells.

作者信息

Baars Paul A, Sierro Sophie, Arens Ramon, Tesselaar Kiki, Hooibrink Berend, Klenerman Paul, van Lier René A W

机构信息

Department of Experimental Immunology, Academic Medical Center, Amsterdam, The Netherlands.

出版信息

Eur J Immunol. 2005 Nov;35(11):3131-41. doi: 10.1002/eji.200425770.

Abstract

In humans, loss of CD27 expression is associated with the stable acquisition of effector functions by CD8+ T cells. We found that murine (CD8+)CD27- T cells were confined to the primed CD62L(dull/-)CD44(bright)CCR7- T cell population. (CD8+)CD27- T cells were absent from lymph nodes but could be found in blood, spleen and in non-lymphoid organs such as lung and liver. Late after primary influenza virus infection, low percentages of antigen-specific CD27- cells emerged in the lung and spleen. After recovery from secondary influenza virus infection, high percentages of influenza-specific CD27- T cells were found in the lung and the loss of CD27 on lung CD8+ T cells coincided with high granzyme B expression. After murine cytomegalovirus infection, loss of CD27 expression on virus-specific CD8+ T cell populations was sustained and especially marked in liver and lung. We suggest that in mice, CD27 is lost from CD8+ T cells only after repetitive antigenic stimulation. Moreover, the high expression of both granzyme B and perforin in the CD27- T cells suggests that the lack of CD27 on murine CD8+ T cells can be used to identify memory T cells with expression of cytotoxic effector molecules.

摘要

在人类中,CD27表达缺失与CD8⁺T细胞效应功能的稳定获得相关。我们发现,小鼠(CD8⁺)CD27⁻T细胞局限于初始CD62L(低表达/阴性)CD44(高表达)CCR7⁻T细胞群体。淋巴结中不存在(CD8⁺)CD27⁻T细胞,但可在血液、脾脏以及肺和肝脏等非淋巴器官中发现。初次感染流感病毒后晚期,肺和脾脏中出现低比例的抗原特异性CD27⁻细胞。二次感染流感病毒恢复后,肺中发现高比例的流感特异性CD27⁻T细胞,且肺CD8⁺T细胞上CD27的缺失与颗粒酶B的高表达同时出现。感染小鼠巨细胞病毒后,病毒特异性CD8⁺T细胞群体上CD27表达的缺失持续存在,在肝脏和肺中尤为明显。我们认为,在小鼠中,CD8⁺T细胞仅在反复抗原刺激后才会丢失CD27。此外,CD27⁻T细胞中颗粒酶B和穿孔素的高表达表明,小鼠CD8⁺T细胞上CD27的缺失可用于识别表达细胞毒性效应分子的记忆T细胞。

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