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胸腺干扰素:小剂量却功效显著。

Thymic Interferons: A Little Goes a Long Way.

作者信息

Vobořil Matouš, Hogquist Kristin A

机构信息

Department of Lab Medicine and Pathology, Center for Immunology, University of Minnesota Medical School, Minneapolis, Minnesota, USA.

出版信息

Immunol Rev. 2025 Jul;332(1):e70038. doi: 10.1111/imr.70038.

Abstract

Central tolerance is an essential process that protects the mammalian immune system from developing autoimmune reactions by forming a self-tolerant repertoire of T cells. The extent of central tolerance depends on the diversity of self-peptide-major histocompatibility complexes that thymocytes encounter on thymic antigen-presenting cells (APCs). Decades of research have demonstrated that medullary thymic epithelial cells (mTECs), a unique type of APC of stromal origin, possess an extraordinary capacity to produce and present thousands of self-peptides to developing thymocytes. This ability is facilitated by various unconventional mechanisms, including AIRE-regulated promiscuous gene expression, mimicry of peripheral cell types, and cooperative antigen transfer between different thymic APCs. Recently, several studies have reported that mTECs and other thymus-resident cells also produce tonic inflammatory signaling, which shapes the thymic microenvironment and expands the repertoire of presented inflammation-associated self-antigens (ISA). In this review, we focus on thymic interferons (IFNs), pro-inflammatory molecules produced as self-antigens by mTECs. Beyond their role as rare self-antigens critical for tolerance induction, IFNs influence the thymic microenvironment by promoting sterile inflammation, regulating the maturation of thymic APCs, and shaping T cell selection. We will discuss the production and regulation of thymic IFNs and their role in APC maturation and T cell selection.

摘要

中枢耐受是一个重要过程,它通过形成T细胞的自身耐受库来保护哺乳动物免疫系统免受自身免疫反应的影响。中枢耐受的程度取决于胸腺细胞在胸腺抗原呈递细胞(APC)上遇到的自身肽 - 主要组织相容性复合体的多样性。数十年的研究表明,髓质胸腺上皮细胞(mTEC)是一种独特的基质来源的APC,具有非凡的能力,能够产生并向发育中的胸腺细胞呈递数千种自身肽。这种能力由多种非常规机制促成,包括自身免疫调节因子(AIRE)调控的杂乱基因表达、外周细胞类型的模拟以及不同胸腺APC之间的协同抗原转移。最近,多项研究报告称,mTEC和其他胸腺驻留细胞也会产生持续性炎症信号,这种信号塑造了胸腺微环境并扩大了所呈递的炎症相关自身抗原(ISA)的库。在本综述中,我们聚焦于胸腺干扰素(IFN),它是由mTEC作为自身抗原产生的促炎分子。除了作为诱导耐受关键的罕见自身抗原所发挥的作用外,IFN还通过促进无菌性炎症、调节胸腺APC的成熟以及塑造T细胞选择来影响胸腺微环境。我们将讨论胸腺IFN的产生和调控及其在APC成熟和T细胞选择中的作用。

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