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胸腺选择决定γδT细胞效应命运:未接触过抗原的细胞产生白细胞介素-17,而接触过抗原的细胞产生干扰素γ。

Thymic selection determines gammadelta T cell effector fate: antigen-naive cells make interleukin-17 and antigen-experienced cells make interferon gamma.

作者信息

Jensen Kirk D C, Su Xiaoqin, Shin Sunny, Li Luke, Youssef Sawsan, Yamasaki Sho, Steinman Lawrence, Saito Takashi, Locksley Richard M, Davis Mark M, Baumgarth Nicole, Chien Yueh-hsiu

机构信息

Department of Microbiology and Immunology, Stanford University, Stanford, CA 94305, USA.

出版信息

Immunity. 2008 Jul 18;29(1):90-100. doi: 10.1016/j.immuni.2008.04.022. Epub 2008 Jun 26.

Abstract

gammadelta T cells uniquely contribute to host immune defense, but how this is accomplished remains unclear. Here, we analyzed the nonclassical major histocompatibility complex class I T10 and T22-specific gammadelta T cells in mice and found that encountering antigen in the thymus was neither required nor inhibitory for their development. But when triggered through the T cell receptor, ligand-naive lymphoid-gammadelta T cells produced IL-17, whereas ligand-experienced cells made IFN-gamma. Immediately after immunization, a large fraction of IL-17(+) gammadelta T cells were found in the draining lymph nodes days before the appearance of antigen-specific IL-17(+) *beta T cells. Thus, thymic selection determines the effector fate of gammadelta T cells rather than constrains their antigen specificities. The swift IL-17 response mounted by antigen-naive gammadelta T cells suggests a critical role for these cells at the onset of an acute inflammatory response to novel antigens.

摘要

γδ T细胞对宿主免疫防御有独特贡献,但具体机制尚不清楚。在此,我们分析了小鼠中I类非经典主要组织相容性复合体T10和T22特异性γδ T细胞,发现胸腺中遇到抗原对其发育既非必需也无抑制作用。但是,当通过T细胞受体触发时,未接触配体的淋巴样γδ T细胞产生白细胞介素-17(IL-17),而接触过配体的细胞则产生干扰素-γ(IFN-γ)。免疫后立即发现,在引流淋巴结中,很大一部分IL-17(+)γδ T细胞在抗原特异性IL-17(+)β T细胞出现前数天就已存在。因此,胸腺选择决定γδ T细胞的效应命运,而非限制其抗原特异性。未接触抗原的γδ T细胞迅速产生IL-17反应,表明这些细胞在对新抗原的急性炎症反应开始时起关键作用。

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