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首页> 外文期刊>International immunology. >The MHC class II ligand lymphocyte activation gene-3 is co-distributed with CD8 and CD3-TCR molecules after their engagement by mAb or peptide-MHC class I complexes.
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The MHC class II ligand lymphocyte activation gene-3 is co-distributed with CD8 and CD3-TCR molecules after their engagement by mAb or peptide-MHC class I complexes.

机译:MHC II类配体淋巴细胞活化基因3与CD8和CD3-TCR分子通过mAb或肽-MHC I类复合物结合后共同分布。

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摘要

Previous studies indicated that signaling through lymphocyte activation gene-3 (LAG-3), a MHC class II ligand, induced by multivalent anti-receptor antibodies led to unresponsiveness to TCR stimulation. Here, lateral distribution of the LAG-3 molecules and its topological relationship (mutual proximity) to the TCR, CD8, CD4, and MHC class I and II molecules were studied in the plasma membrane of activated human T cells in co-capping experiments and conventional fluorescence microscopy. Following TCR engagement by either TCR-specific mAb or MHC-peptide complex recognition in T-B cell conjugates, LAG-3 was found to be specifically associated with the CD3-TCR complex. Similarly, following CD8 engagement LAG-3 and CD8 were co-distributed on the cell surface while only a low percentage of CD4-capped cells displayed LAG-3 co-caps. In addition, LAG-3 was found to be associated with MHC class II (i.e. DR, DP and DQ) and partially with MHC class I molecules. The supramolecular assemblies described here between LAG-3, CD3, CD8 and MHC class II molecules may result from an organization in raft microdomains, a phenomenon known to regulate early events of T cell activation.
机译:先前的研究表明,由多价抗受体抗体诱导的淋巴细胞活化基因3(LAG-3)(一种MHC II类配体)发出的信号导致对TCR刺激无反应。在这里,LAG-3分子的横向分布及其与TCR,CD8,CD4和MHC I类和II类分子的拓扑关系(相互接近)在共封盖实验中研究了活化的人类T细胞的质膜,并常规荧光显微镜。在T-B细胞偶联物中通过TCR特异性mAb或MHC肽复合物识别进行TCR结合后,发现LAG-3与CD3-TCR复合物特异性结合。类似地,在CD8参与之后,LAG-3和CD8共分布在细胞表面,而只有很少百分比的CD4封端的细胞显示出LAG-3共帽。另外,发现LAG-3与II类MHC分子(即DR,DP和DQ)有关,并且部分与I类MHC分子有关。本文所述的LAG-3,CD3,CD8和MHC II类分子之间的超分子组装可能是由筏微域中的组织导致的,这种现象已知是调节T细胞活化的早期事件。

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