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Autoantigen-specific interactions with CD4+ thymocytes control mature medullary thymic epithelial cell cellularity.

机译:与CD4 +胸腺细胞的自身抗原特异性相互作用可控制成熟的髓样胸腺上皮细胞的细胞性。

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摘要

Medullary thymic epithelial cells (mTECs) are specialized for inducing central immunological tolerance to self-antigens. To accomplish this, mTECs must adopt a mature phenotype characterized by expression of the autoimmune regulator Aire, which activates the transcription of numerous genes encoding tissue-restricted self-antigens. The mechanisms that control mature Aire(+) mTEC development in the postnatal thymus remain poorly understood. We demonstrate here that, although either CD4(+) or CD8(+) thymocytes are sufficient to sustain formation of a well-defined medulla, expansion of the mature mTEC population requires autoantigen-specific interactions between positively selected CD4(+) thymocytes bearing autoreactive T cell receptor (TCR) and mTECs displaying cognate self-peptide-MHC class II complexes. These interactions also involve the engagement of CD40 on mTECs by CD40L induced on the positively selected CD4(+) thymocytes. This antigen-specific TCR-MHC class II-mediated crosstalk between CD4(+) thymocytes and mTECs defines a unique checkpoint in thymic stromal development that is pivotal for generating a mature mTEC population competent for ensuring central T cell tolerance.
机译:髓样胸腺上皮细胞(mTECs)专门用于诱导对自身抗原的中央免疫耐受。为此,mTEC必须采用以自身免疫调节剂Aire为特征的成熟表型,该表型激活众多编码组织限制性自身抗原的基因的转录。控制产后胸腺中成熟的Aire(+)mTEC发育的机制仍知之甚少。我们在这里证明,尽管CD4(+)或CD8(+)胸腺细胞足以维持定义良好的延髓的形成,但成熟的mTEC群体的扩展需要在带有自身反应性的阳性选择的CD4(+)胸腺细胞之间进行自身抗原特异性相互作用T细胞受体(TCR)和mTECs显示相关的自身肽-MHC II类复合物。这些相互作用还涉及在阳性选择的CD4(+)胸腺细胞上诱导的CD40L诱导CD40在mTECs上的参与。 CD4(+)胸腺细胞和mTEC之间的这种抗原特异性TCR-MHC II类介导的串扰在胸腺基质发育中定义了一个独特的检查点,这对于产生能够确保中央T细胞耐受性的成熟mTEC种群至关重要。

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