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在流感特异性CD8 + T细胞记忆的早期建立过程中,位置而非CD62L表型至关重要。

Location rather than CD62L phenotype is critical in the early establishment of influenza-specific CD8+ T cell memory.

作者信息

Kedzierska Katherine, Stambas John, Jenkins Misty R, Keating Rachael, Turner Stephen J, Doherty Peter C

机构信息

Department of Microbiology and Immunology, University of Melbourne, Parkville, Melbourne 3010, Australia.

出版信息

Proc Natl Acad Sci U S A. 2007 Jun 5;104(23):9782-7. doi: 10.1073/pnas.0703699104. Epub 2007 May 23.

Abstract

The rapid recall of influenza virus-specific CD8(+) T cell effector function is protective, although our understanding of T cell memory remains incomplete. Recent debate has focused particularly on the CD62L lymph node homing receptor. The present analysis shows that although functional memory can be established from both CD62L(hi) and CD62L(lo) CD8(+) T cell subsets soon after initial encounter between naïve precursors and antigen, the optimal precursors are CD8(+)CD44(hi)CD25(lo) immune lymphocytes isolated from draining lymph nodes on day 3.5 after influenza virus infection. Analysis of primed T cells at different times after challenge indicates that the capacity to transfer memory is diminished at the peak of the primary cytotoxic T lymphocyte response, challenging speculations that the transition to memory first requires full differentiation to effector status. It seems that location rather than CD62Lhi/lo phenotype may be the more profitable focus for further dissection of the early establishment of T cell memory.

摘要

流感病毒特异性CD8(+) T细胞效应功能的快速恢复具有保护作用,尽管我们对T细胞记忆的理解仍不完整。最近的争论尤其集中在CD62L淋巴结归巢受体上。目前的分析表明,虽然在初始幼稚前体细胞与抗原接触后不久,CD62L(hi)和CD62L(lo) CD8(+) T细胞亚群都可以建立功能性记忆,但最佳前体细胞是在流感病毒感染后3.5天从引流淋巴结中分离出的CD8(+)CD44(hi)CD25(lo)免疫淋巴细胞。对攻击后不同时间的致敏T细胞进行分析表明,在初次细胞毒性T淋巴细胞反应的高峰期,记忆传递能力会下降,这对认为向记忆的转变首先需要完全分化为效应状态的推测提出了挑战。似乎位置而非CD62Lhi/lo表型可能是进一步剖析T细胞记忆早期建立过程中更值得关注的重点。

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