Institute for Immunology, Ludwig-Maximilians-Universität, Munich, Germany.
Nat Immunol. 2010 Jun;11(6):512-9. doi: 10.1038/ni.1874. Epub 2010 May 2.
Medullary thymic epithelial cells (mTECs) serve an essential function in central tolerance by expressing peripheral-tissue antigens. These antigens may be transferred to and presented by dendritic cells (DCs). Therefore, it is unclear whether mTECs, in addition to being an antigen reservoir, also serve a mandatory function as antigen-presenting cells. Here we diminished major histocompatibility complex (MHC) class II on mTECs through transgenic expression of a 'designer' microRNA specific for the MHC class II transactivator CIITA (called 'C2TA' here). This resulted in an enlarged polyclonal CD4(+) single-positive compartment and, among thymocytes specific for model antigens expressed in mTECs, enhanced selection of regulatory T cells (T(reg) cells) at the expense of deletion. Our data document an autonomous contribution of mTECs to both dominant and recessive mechanisms of CD4(+) T cell tolerance and support an avidity model of T(reg) cell development versus deletion.
髓质胸腺上皮细胞 (mTECs) 通过表达外周组织抗原在中枢耐受中发挥重要作用。这些抗原可能被树突状细胞 (DC) 摄取并呈递。因此,目前尚不清楚 mTECs 是否除了作为抗原储存库之外,还作为抗原呈递细胞发挥强制性功能。在这里,我们通过转基因表达针对 MHC II 类转录激活物 CIITA 的“设计” microRNA(称为“C2TA”)来减少 mTECs 中的 MHC 类 II。这导致多克隆 CD4(+)单阳性区扩大,并且在针对 mTEC 中表达的模型抗原特异的胸腺细胞中,以牺牲删除为代价增强了调节性 T 细胞 (T(reg) 细胞)的选择。我们的数据证明了 mTECs 对 CD4(+) T 细胞耐受的显性和隐性机制的自主贡献,并支持 T(reg) 细胞发育与删除的亲和力模型。
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