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Tax and M1 Peptide/HLA-A2-Specific Fabs and T Cell Receptors Recognize Nonidentical Structural Features on Peptide/HLA-A2 Complexes

机译:Tax和M1肽/ HLA-A2特异的Fab和T细胞受体识别肽/ HLA-A2络合物的结构特征不同

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Both TCRs and Ab molecules are capable of MHC-restricted recognition of peptide/MHC complexes. However, such MHC restriction is the predominant mode of recognition by T cells, but is extremely rare for B cells. The present study asks whether the dichotomy in Ag recognition modes of T and B cells could be due to fundamental differences in the methods by which TCRs and Abs recognize peptide/MHC complexes. We have compared MHC and peptide recognition by panels of CTL lines specific for the Tax and M1 peptides presented by HLA-A2 plus Tax and M1 peptide/HLA-A2-specific human Fabs that were selected from a naive phage display library. Collectively, the results indicate both striking similarities and important differences between Fab and TCR recognition of MHC and peptide components of the Tax and M1/HLA-A2 complexes. These findings suggest that these two classes of immunoreceptors have solved the problem of specific recognition of peptide/MHC complexes by nonidentical mechanisms. This conclusion is important in part because it indicates that Ab engineering approaches could produce second-generation Ab molecules that more closely mimic TCR fine specificity. Such efforts may produce more efficacious diagnostic and therapeutic agents.
机译:TCR和Ab分子均能够通过MHC限制识别肽/ MHC复合物。但是,这种MHC限制是T细胞识别的主要方式,但对于B细胞却极为罕见。本研究问T和B细胞的Ag识别模式的二分法是否可能是由于TCR和Abs识别肽/ MHC复合物的方法的根本差异。我们已经比较了通过对HLA-A2加上Tax和M1肽/ HLA-A2特异性人类Fabs提呈的Tax和M1肽特异的CTL品系的MHC和肽的识别,这些人Fabs是从天然噬菌体展示库中选择的。总体而言,结果表明Fab和TCR对MHC的识别以及Tax和M1 / HLA-A2复合物的肽成分之间的惊人相似性和重要区别。这些发现表明这两类免疫受体已经通过不同的机制解决了肽/ MHC复合物的特异性识别问题。该结论之所以重要,部分是因为它表明Ab工程方法可以产生更紧密地模仿TCR精细特异性的第二代Ab分子。这样的努力可以产生更有效的诊断和治疗剂。

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