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首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Regulation Of Cd8~+ Regulatory T Cells: Interruption Of The Nkg2a-qa-1 Interaction Allows Robust Suppressive Activity And Resolution Of Autoimmune Disease
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Regulation Of Cd8~+ Regulatory T Cells: Interruption Of The Nkg2a-qa-1 Interaction Allows Robust Suppressive Activity And Resolution Of Autoimmune Disease

机译:调节Cd8〜+调节性T细胞:Nkg2a-qa-1相互作用的中断使鲁棒的抑制活性和自身免疫性疾病的解决

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摘要

Regulation of autoreactive CD4 T cells is essential to maintain self-tolerance and prevent autoimmune disease. Although CD8 T regulatory (Treg) cells that recognize self-peptides restricted by Qa-1 (HLA-E in humans) inhibit autoreactive CD4 cells and attenuate experimental autoimmune encephalomyelitis (EAE), the mechanism of this interaction is unclear. We generated Qa-1 mutant knock-in mice that impair Qa-1 binding to the T cell receptor (TCR) and CD94/NKG2A receptors. Analysis of these mice showed that TCR-dependent recognition of Qa-1-peptide complexes on target CD4 cells is essential for suppression by CD8 Treg cells. Further analysis revealed that genetic disruption of the Qa-1-CD94/NKG2A interaction unleashes robust CD8 Treg cell activity that completely abolishes development of EAE.
机译:调节自身反应性CD4 T细胞对于维持自我耐受和预防自身免疫性疾病至关重要。尽管识别受Qa-1限制的自身肽的CD8 T调节(Treg)细胞(人类中的HLA-E)会抑制自身反应性CD4细胞并减弱实验性自身免疫性脑脊髓炎(EAE),但这种相互作用的机制尚不清楚。我们生成了Qa-1突变型敲入小鼠,这些小鼠损害Qa-1与T细胞受体(TCR)和CD94 / NKG2A受体的结合。对这些小鼠的分析表明,靶CD4细胞上Qa-1肽复合物的TCR依赖性识别对于CD8 Treg细胞的抑制至关重要。进一步的分析表明,Qa-1-CD94 / NKG2A相互作用的遗传破坏释放出强大的CD8 Treg细胞活性,从而完全消除了EAE的发展。

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