首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Dissociation of peripheral T cell responses from thymocyte negative selection by weak agonists supports a spare receptor model of T cell activation
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Dissociation of peripheral T cell responses from thymocyte negative selection by weak agonists supports a spare receptor model of T cell activation

机译:弱激动剂从胸腺细胞阴性选择中分离外周T细胞反应支持T细胞活化的备用受体模型

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摘要

We have focused on stability of the peptide-MHC complex as a determining factor of ligand potency for thymocytes and peripheral CD4+ T cell responses. MHC variant peptides that have low affinities and fast dissociation rates are different in that they stimulate proliferation and cytolysis of mature T cells (classifying the variant peptides as weak agonists) but do not induce thymocyte negative selection. The MHC variant weak agonists require significant receptor reserve, because decreasing the level of T cell receptor on mature T cells blocks the proliferative response. These results demonstrate that peripheral T cells are more sensitive to MHC variant ligands by virtue of increased T cell receptor expression; in addition, the data support a T cell model of the spare receptor theory.
机译:我们以肽-MHC复合物的稳定性作为胸腺细胞和外周CD4 + T细胞应答配体效能的决定因素。具有低亲和力和快速解离速率的MHC变体肽的不同之处在于,它们刺激成熟T细胞的增殖和细胞溶解(将变体肽分类为弱激动剂),但不会诱导胸腺细胞阴性选择。 MHC变体弱激动剂需要大量的受体储备,因为降低成熟T细胞上T细胞受体的水平会阻止增殖反应。这些结果表明,由于增加的T细胞受体表达,外周T细胞对MHC变体配体更敏感。此外,数据支持备用受体理论的T细胞模型。

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