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TCR/自身抗原相互作用驱动双阴性T细胞在外周扩增并分化为抑制性细胞。

TCR/self-antigen interactions drive double-negative T cell peripheral expansion and differentiation into suppressor cells.

作者信息

Priatel J J, Utting O, Teh H S

机构信息

Department of Microbiology and Immunology, University of British Columbia, Vancouver, Canada.

出版信息

J Immunol. 2001 Dec 1;167(11):6188-94. doi: 10.4049/jimmunol.167.11.6188.

Abstract

Mature CD4-CD8- alphabeta+ T cells (DNTC) in the periphery of TCR transgenic mice are resistant to clonal deletion in cognate Ag-expressing (Ag+) mice. Previously, we have characterized DNTC populations bearing the alloreactive 2C TCR in Ag-free (Ag-) and Ag+ mice. Despite appearing functionally anergic when challenged with cognate Ag in vitro, Ag-experienced DNTC exhibit markers of activation/memory, a lowered threshold of activation, ex vivo cytolytic activity, and the ability to rapidly secrete IFN-gamma. Remarkably, these memory-like DNTC also possess potent immunoregulatory properties, competing effectively for bystander-produced IL-2 and suppressing autoreactive CD8+ T cell proliferation via a Fas/FasL-dependent cytolytic mechanism. The fact that DNTC recovered from Ag+ mice possess markers and attributes characteristic of naive CD8+ T cells that have undergone homeostasis-induced proliferation suggested that they may be derived from a similar peripheral expansion process. Naive DNTC adoptively transferred into Ag-bearing hosts rapidly acquire markers and functional attributes of DNTC that have continually developed in the presence of Ag. Thus, the peripheral selection and maintenance of such autoreactive cells may serve to negatively regulate potential autoimmune T cell responses.

摘要

TCR转基因小鼠外周的成熟CD4-CD8-αβ+ T细胞(双阴性T细胞,DNTC)对表达同源抗原(Ag+)的小鼠中的克隆清除具有抗性。此前,我们已对无菌(Ag-)和Ag+小鼠中携带同种异体反应性2C TCR的DNTC群体进行了表征。尽管在体外受到同源抗原刺激时表现出功能无反应性,但经历过抗原刺激的DNTC表现出激活/记忆标记、降低的激活阈值、体外细胞溶解活性以及快速分泌IFN-γ的能力。值得注意的是,这些类似记忆的DNTC还具有强大的免疫调节特性,能有效竞争旁观者产生的IL-2,并通过Fas/FasL依赖性细胞溶解机制抑制自身反应性CD8+ T细胞增殖。从Ag+小鼠中回收的DNTC具有经历稳态诱导增殖的初始CD8+ T细胞的标记和特征,这一事实表明它们可能源自类似的外周扩增过程。过继转移到携带抗原的宿主中的初始DNTC会迅速获得在抗原存在下持续发育的DNTC的标记和功能特性。因此,此类自身反应性细胞的外周选择和维持可能有助于对潜在的自身免疫性T细胞反应进行负调节。

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