首页> 外文期刊>European Journal of Immunology >Functional and biophysical characterization of an HLA-A*6801-restricted HIV-specific T cell receptor.
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Functional and biophysical characterization of an HLA-A*6801-restricted HIV-specific T cell receptor.

机译:功能和生物物理特性6801 -限制HIV-specific T细胞抗原*受体。

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摘要

HLA-A*6801 exhibits several unusual features. First, it is known to bind weakly to CD8 due to the presence of an A245V substitution in the alpha3 domain. Second, it is able to accommodate unusually long peptides as a result of peptide 'kinking' in the binding groove. Third, CD8+ cytotoxic T lymphocytes that recognise HLA-A*6801-restricted antigens can tolerate substantial changes in the peptide sequence without apparent loss of recognition. In addition, it has been suggested that HLA-A68-restricted TCR might bind with higher affinity than other TCR due to their selection in the presence of a decreased contribution from CD8. Here we (1) examine monoclonal T cell recognition of an HLA-A*6801-restricted HIV-1 Tat-derived 11-amino acid peptide (ITKGLGISYGR) and natural variant sequences thereof; (2) measure the affinity and kinetics of a TCR/pHLA-A68 interaction biophysically for the first time, showing that equilibrium binding occurs within the range previously determined for non-HLA-A68-restricted TCR (KD approx. 7 microM); and (3) show that "normalization" of the non-canonical HLA-A*6801 CD8-binding domain enhances recognition of agonist peptides without inducing non-specific activation. This latter effect may provide a fundamental new mechanism with which to enhance T cell immunity to specific antigens.
机译:于* 6801展示一些不同寻常的特性。首先,它绑定弱CD8由于A245V替换的alpha3域。异常长肽的肽“扭结”绑定槽。细胞毒性T淋巴细胞识别于* 6801 -限制抗原可以容忍大量的肽序列的变化没有明显的识别。另外,建议HLA-A68-restricted TCR可能结合更高亲和力比其他细胞由于他们的选择的存在减少的贡献CD8。识别的抗原* 6801 -限制hiv - 1Tat-derived 11-amino酸肽(ITKGLGISYGR)和自然变异序列;测量的亲和力和动力学识别/ pHLA-A68交互的生物物理第一次,表明平衡绑定发生在先前确定的经营范围内non-HLA-A68-restricted TCR (KD约。(3)显示的“正常化”非规范于* 6801 CD8-binding域提高识别受体激动剂肽诱导非特异性激活。效果可能会提供一个基本的新机制具体来增强T细胞免疫力抗原。

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