胸腺选择中的特异性与灵活性。
Specificity and flexibility in thymic selection.
作者信息
Jameson S C, Hogquist K A, Bevan M J
机构信息
Howard Hughes Medical Institute, Department of Immunology, University of Washington, Seattle 98195.
出版信息
Nature. 1994 Jun 30;369(6483):750-2. doi: 10.1038/369750a0.
Abstract
During positive selection, developing thymocytes are rescued from programmed cell death by T-cell receptor (TCR)-mediated recognition of major histocompatibility complex (MHC) molecules. MHC-bound peptides contribute to this process. Recently we identified individual MHC-binding peptides which can induce positive selection of a single TCR. Here we examine peptide fine specificity in positive selection. These data suggest that a direct TCR-peptide interaction occurs during this event, and strengthens the correlation between selecting peptides and TCR antagonists. Certain positively selecting peptides are weakly antigenic. We demonstrate that thymocytes 'educated' on such a peptide are specifically non-responsive to it and have decreased CD8 expression levels. Similar reduction of CD8 expression on mature T cells converts a TCR agonist into a TCR antagonist. These data indicate that thymocytes may maintain self-tolerance towards a positively selecting ligand by regulating co-receptor expression.
摘要
在阳性选择过程中,发育中的胸腺细胞通过T细胞受体(TCR)介导的对主要组织相容性复合体(MHC)分子的识别,从程序性细胞死亡中被拯救出来。与MHC结合的肽参与了这一过程。最近,我们鉴定出了能够诱导单一TCR阳性选择的单个MHC结合肽。在此,我们研究了阳性选择中的肽精细特异性。这些数据表明,在这一事件中发生了直接的TCR-肽相互作用,并加强了选择肽与TCR拮抗剂之间的相关性。某些阳性选择肽具有弱抗原性。我们证明,在这样一种肽上“受教育”的胸腺细胞对其具有特异性无反应性,并且CD8表达水平降低。成熟T细胞上CD8表达的类似降低会将TCR激动剂转化为TCR拮抗剂。这些数据表明,胸腺细胞可能通过调节共受体表达来维持对阳性选择配体的自身耐受性。
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