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细胞因子诱导的分泌白细胞介素-10的CD8 T细胞代表一种表型独特的抑制性T细胞谱系。

Cytokine-induced IL-10-secreting CD8 T cells represent a phenotypically distinct suppressor T-cell lineage.

作者信息

Noble Alistair, Giorgini Angela, Leggat Jamie A

机构信息

Medical Research Council, King's College London, UK.

出版信息

Blood. 2006 Jun 1;107(11):4475-83. doi: 10.1182/blood-2005-10-3994. Epub 2006 Feb 7.

DOI:10.1182/blood-2005-10-3994
PMID:16467201
Abstract

Populations of regulatory T cells (Tregs) control autoimmune and allergic immunopathology induced by self or foreign antigens. Several types of CD4(+) MHC class II-restricted Treg populations have been characterized, but the biology of CD8(+), MHC class I-restricted Tregs is less understood. We show here that CD8(+) Tregs are rapidly generated in the presence of IL-4 and IL-12, produce IL-10, and exhibit a unique cell-surface phenotype with coexpression of activation and naive cell-associated markers. They block activation of naive or effector T cells and suppress IgG/IgE antibody responses and graft-versus-host disease in vivo. Suppression is dependent on cell contact and mediated by direct T-cell-T-cell interaction that antagonizes T-cell-receptor (TCR) signals. The data establish the existence of a CD8 T-cell suppressor effector subset distinct in both phenotype and function from T cytotoxic 1 (Tc1) and Tc2 cells. Production of such CD8 Tregs has potential for cell-based therapy of CD4 or CD8 T-cell-mediated disease.

摘要

调节性T细胞(Tregs)群体可控制由自身或外来抗原诱导的自身免疫和过敏性免疫病理。已对几种CD4(+) MHC II类限制性Treg群体进行了表征,但对CD8(+) MHC I类限制性Tregs的生物学特性了解较少。我们在此表明,CD8(+) Tregs在IL-4和IL-12存在的情况下迅速产生,产生IL-10,并表现出独特的细胞表面表型,同时表达激活相关和幼稚细胞相关标志物。它们可阻断幼稚或效应T细胞的激活,并在体内抑制IgG/IgE抗体反应和移植物抗宿主病。抑制作用依赖于细胞接触,并由拮抗T细胞受体(TCR)信号的直接T细胞-T细胞相互作用介导。这些数据证实了存在一个CD8 T细胞抑制效应亚群,其在表型和功能上均不同于细胞毒性T细胞1(Tc1)和Tc2细胞。此类CD8 Tregs的产生具有用于基于细胞的CD4或CD8 T细胞介导疾病治疗的潜力。

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