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效应性CD4 T细胞在生化特性上与记忆亚群不同:效应细胞在体内长期持续存在的证据。

Effector CD4 T cells are biochemically distinct from the memory subset: evidence for long-term persistence of effectors in vivo.

作者信息

Ahmadzadeh M, Hussain S F, Farber D L

机构信息

Department of Cell Biology and Molecular Genetics, University of Maryland, College Park, MD 20742, USA.

出版信息

J Immunol. 1999 Sep 15;163(6):3053-63.

Abstract

Memory T cell responses are believed to be mediated by long-lived memory T cells that arise directly from a subset of short-lived, activated effector T cells that have reverted to the resting state. Although widely accepted, definitive proof that memory T cells arise from effectors is lacking because of the inability to reliably distinguish these subsets based on known phenotypic or functional parameters. We have used a biochemical approach to distinguish effector and memory CD4 T cell subsets and follow the differentiative fate of effector cells in vivo. When examined biochemically, effector and memory CD4 T cells are strikingly distinct and exhibit qualitative and quantitative differences in tyrosine phosphorylation. These effector-specific patterns were identical in effectors derived either from naive CD4 T cells (primary effectors) or memory CD4 T cells (memory effectors). To monitor the fate of effector cells in vivo, Ag-activated CD4+ TCR-transgenic T cells were transferred into irradiated BALB/c mice. These TCR-transgenic CD4 T cells persisted in adoptive hosts for several months, gave a recall response to Ag, yet exhibited effector-specific biochemical profiles. These results suggest that a subset of effector CD4 T cells can persist in vivo and contribute to long-term immunity by mediating secondary immune responses.

摘要

记忆性T细胞反应被认为是由长寿命记忆性T细胞介导的,这些长寿命记忆性T细胞直接来源于一部分已恢复到静止状态的短寿命活化效应T细胞。尽管这一观点已被广泛接受,但由于无法基于已知的表型或功能参数可靠地区分这些亚群,因此缺乏记忆性T细胞来源于效应T细胞的确切证据。我们采用了一种生化方法来区分效应性和记忆性CD4 T细胞亚群,并在体内追踪效应细胞的分化命运。当进行生化检测时,效应性和记忆性CD4 T细胞表现出显著差异,在酪氨酸磷酸化方面存在质和量的不同。这些效应细胞特异性模式在源自初始CD4 T细胞的效应细胞(初始效应细胞)或记忆性CD4 T细胞的效应细胞(记忆效应细胞)中是相同的。为了在体内监测效应细胞的命运,将抗原激活的CD4+ TCR转基因T细胞转移到经照射的BALB/c小鼠体内。这些TCR转基因CD4 T细胞在过继宿主中持续存在数月,对抗原产生回忆反应,但表现出效应细胞特异性的生化特征。这些结果表明,一部分效应性CD4 T细胞能够在体内持续存在,并通过介导二次免疫反应对长期免疫作出贡献。

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