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通过抗原识别非依赖和体液因子依赖的机制激活调节性 T 细胞来精细调节抗原特异性免疫反应。

Fine-tuning of antigen-specific immune responses by regulatory T cells activated via antigen recognition-independent and humoral factor-dependent mechanisms.

机构信息

Department of Immunology, Dokkyo Medical University School of Medicine, Tochigi, Japan.

Division of Host Defense, Research Center for Advanced Medical Science, Dokkyo Medical University School of Medicine, Tochigi, Japan.

出版信息

Scand J Immunol. 2021 Jun;93(6):e13020. doi: 10.1111/sji.13020. Epub 2021 Jan 12.

DOI:10.1111/sji.13020
PMID:33393095
Abstract

CD4 CD25 Foxp3 regulatory T cells (Tregs) are highly sensitive to IL-2, one of the many cytokines produced during immune responses, for their development, survival and functions. Although the effects of IL-2 administration on Tregs in vivo are well characterized, the effects on Tregs elicited by IL-2 produced during an immune response have not been elucidated. Hence, in this study, Treg behaviour during IL-2-producing immune responses was explored using in vivo and in vitro murine systems. The use of murine mixed lymphocyte culture (MLC) revealed that a large proportion of Tregs increased in size, accompanied by both cell death and proliferation status. Further, these large Tregs, which were found to not recognize specific antigens, were observed in MLCs as being functionally activated by various cytokines, including IL-2, produced by antigen-specific T cells. This 'bystander Treg activation' was also observed in mice with graft-versus-host reactions (GvHRs). Alternatively, effector cells from Treg-depleted MLCs exhibited lower antigen-specific responses or higher cross-reactivity as compared to control MLCs with Tregs. Taken together, these results suggest that Tregs are activated by cytokines, mainly IL-2, released from T cells that are activated by a specific antigen. Subsequently, these activated bystander Tregs contribute to the fine-tuning of highly antigen-specific immune responses.

摘要

CD4 CD25 Foxp3 调节性 T 细胞(Tregs)对 IL-2 非常敏感,IL-2 是免疫反应中产生的众多细胞因子之一,对其发育、存活和功能至关重要。尽管 IL-2 给药对体内 Tregs 的影响已得到很好的描述,但对免疫反应中产生的 IL-2 诱导的 Tregs 的影响尚未阐明。因此,在这项研究中,使用体内和体外小鼠系统探索了 Tregs 在产生 IL-2 的免疫反应期间的行为。使用小鼠混合淋巴细胞培养(MLC)发现,很大一部分 Tregs 体积增大,同时伴有细胞死亡和增殖状态。此外,这些发现不识别特定抗原的大 Tregs 在 MLC 中被观察到被各种细胞因子(包括由抗原特异性 T 细胞产生的 IL-2)激活。这种“旁观者 Treg 激活”也在移植物抗宿主反应(GvHR)的小鼠中观察到。或者,与含有 Tregs 的对照 MLC 相比,来自 Treg 耗尽的 MLC 的效应细胞表现出较低的抗原特异性反应或较高的交叉反应性。综上所述,这些结果表明 Tregs 被由特定抗原激活的 T 细胞释放的细胞因子(主要是 IL-2)激活。随后,这些被激活的旁观者 Tregs 有助于高度抗原特异性免疫反应的精细调节。

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