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[Aire在中枢和外周免疫耐受中的作用]

[Function of Aire in central and peripheral immune tolerance].

作者信息

Hanafusa Takaaki

机构信息

Postdoctoral Fellow, Laboratory of Dr. Mark S Anderson, Diabetes Center, University of California, San Francisco.

出版信息

Nihon Rinsho Meneki Gakkai Kaishi. 2014;37(3):133-8. doi: 10.2177/jsci.37.133.

Abstract

Negative selection induces central tolerance in which self-reactive T cells are deleted by medullary thymic epithelial cells (mTECs) to prevent autoimmunity. The transcriptional factor, autoimmune regulator (Aire), controls the expression of tissue-specific antigens (TSAs) by mTECs for negative selection. The mechanisms by which Aire targets loci which encode TSAs are unknown in detail; recently, however, the ATF7ip-MBD1 complex was identified as an Aire-interacting transcriptional protein complex required for its targeting the loci. Lineage tracing of Aire(+) mTECs identified that mTECs have a post-Aire stage during the development, where they lost maturation markers but maintained intermediate TSA expression, and Aire is required for the terminal differentiation of mTEC's. Extrathymic Aire-expressing cells (eTACs) are identified in murine and human secondary lymphoid organs. eTACs express major histocompatibility complex class II(hi), CD80(lo), CD86(lo), epithelial cell adhesion molecule(hi), CD45(lo) bone marrow-derived peripheral antigen-presenting cell population, which is distinct from mTECs and dendritic cells. They can induce activation-induced cell death of self-reactive CD8(+) T cells and unresponsiveness of self-reactive CD4(+) T cells through a mechanism that does not require regulatory T cells, suggesting that peripheral Aire plays a complementary role for central tolerance.

摘要

阴性选择诱导中枢耐受,其中自身反应性T细胞被髓质胸腺上皮细胞(mTECs)清除以预防自身免疫。转录因子自身免疫调节因子(Aire)控制mTECs表达组织特异性抗原(TSAs)以进行阴性选择。Aire靶向编码TSAs的基因座的详细机制尚不清楚;然而,最近,ATF7ip-MBD1复合物被鉴定为一种与Aire相互作用的转录蛋白复合物,是其靶向这些基因座所必需的。对Aire(+) mTECs的谱系追踪表明,mTECs在发育过程中有一个Aire后阶段,在此阶段它们失去了成熟标志物,但维持中等水平的TSA表达,并且Aire是mTECs终末分化所必需的。在小鼠和人类的二级淋巴器官中鉴定出胸腺外表达Aire的细胞(eTACs)。eTACs表达主要组织相容性复合体II类(高)、CD80(低)、CD86(低)、上皮细胞粘附分子(高)、CD45(低),是骨髓来源的外周抗原呈递细胞群体,与mTECs和树突状细胞不同。它们可以通过一种不需要调节性T细胞的机制诱导自身反应性CD8(+) T细胞的活化诱导细胞死亡和自身反应性CD4(+) T细胞的无反应性,这表明外周Aire对中枢耐受起补充作用。

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