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表达“AIRE”和外周组织特异性抗原的小鼠胸腺上皮细胞系在体外复制 T 细胞阴性选择。

Mouse thymic epithelial cell lines expressing "Aire" and peripheral tissue-specific antigens reproduce in vitro negative selection of T cells.

机构信息

Advanced Research Center for Genome Super Power, Keio University, 2 Okubo, Tsukuba, Ibaraki 300-2611, Japan.

出版信息

Exp Cell Res. 2011 Aug 15;317(14):2019-30. doi: 10.1016/j.yexcr.2011.05.002. Epub 2011 Jun 15.

Abstract

In the human thymus, AIRE (autoimmune regulator) gene is expressed in a very limited type of medullary thymic epithelial cells (mTECs) and no cognate cell lines are available, hence the molecular analysis of AIRE gene function has been difficult. To improve this situation, we attempted to isolate Aire-expressing cells and established three cell lines (Aire⁺TEC1, Aire⁺TEC2, Aire⁺DC) from the abnormally enlarged thymus, which was developed in the transgenic mice expressing SV40 T-antigen driven by the mouse Aire gene promoter. When these Aire⁺ cell lines were co-cultured with fresh thymocytes, they adhered to the majority of thymocytes and induced apoptosis as if negative selection of T-cells in the thymus is occurring in vitro. Further analysis revealed that these Aire⁺ cell lines are derived from mTECs and exhibit characteristic natures of "antigen presenting cells" including several distinct abilities: to express a variety of peripheral tissue-specific antigens, to produce immunoproteasome and immunological synapse, and to express some of TNFSFs (tumor necrosis factor super families). Thus, the newly established Aire⁺ cell lines will be invaluable for the further detailed analysis of AIRE gene function in the central tolerance of immunity and autoimmune disease.

摘要

在人类胸腺中,AIRE(自身免疫调节因子)基因在非常有限类型的髓质胸腺上皮细胞(mTEC)中表达,并且没有同源细胞系可用,因此 AIRE 基因功能的分子分析一直很困难。为了改善这种情况,我们试图分离表达 Aire 的细胞,并从异常增大的胸腺中建立了三个细胞系(Aire⁺TEC1、Aire⁺TEC2、Aire⁺DC),这些细胞系是在表达 SV40 T 抗原的转基因小鼠中建立的,该抗原由小鼠 Aire 基因启动子驱动。当这些 Aire⁺细胞系与新鲜的胸腺细胞共培养时,它们与大多数胸腺细胞黏附,并诱导凋亡,就好像在体外发生了胸腺 T 细胞的阴性选择。进一步的分析表明,这些 Aire⁺细胞系来源于 mTEC,并表现出“抗原提呈细胞”的特征性质,包括几种不同的能力:表达各种外周组织特异性抗原,产生免疫蛋白酶体和免疫突触,并表达一些 TNFSFs(肿瘤坏死因子超家族)。因此,新建立的 Aire⁺细胞系将对进一步详细分析 AIRE 基因在免疫中枢耐受和自身免疫性疾病中的功能非常有价值。

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