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首页> 外文期刊>Immunity >Thymic selection determines gammadelta T cell effector fate: antigen-naive cells make interleukin-17 and antigen-experienced cells make interferon gamma.
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Thymic selection determines gammadelta T cell effector fate: antigen-naive cells make interleukin-17 and antigen-experienced cells make interferon gamma.

机译:胸腺的选择决定了γ-T细胞效应子的命运:抗原初生细胞产生白介素17,而抗原经历细胞产生干扰素γ。

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摘要

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.
机译:γT细胞可以独特地促进宿主的免疫防御,但如何实现尚不清楚。在这里,我们分析了小鼠中非经典的主要组织相容性复合体I类T10和T22特异性的Gammadelta T细胞,发现在胸腺中遇到抗原既不需要也不抑制它们的发育。但是,当通过T细胞受体触发时,未配体的淋巴样-γT细胞产生IL-17,而经历配体的细胞则产生IFN-γ。免疫后立即在抗原特异性IL-17(+)βT细胞出现前几天在引流淋巴结中发现很大一部分IL-17(γ)γT细胞。因此,胸腺选择决定了γT细胞的效应命运,而不是限制了它们的抗原特异性。初生抗原的γ-T细胞对IL-17的迅速反应表明,这些细胞在对新抗原的急性炎症反应开始时起着至关重要的作用。

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