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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Characterization of HLA class II/peptide-TCR interactions of the immunodominant T cell epitope in Art v 1, the major mugwort pollen allergen.
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Characterization of HLA class II/peptide-TCR interactions of the immunodominant T cell epitope in Art v 1, the major mugwort pollen allergen.

机译:主要艾蒿花粉过敏原Art v 1中免疫优势T细胞表位的HLA II类/肽-TCR相互作用的表征。

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摘要

More than 95% of mugwort pollen-allergic individuals are sensitized to Art v 1, the major allergen in mugwort pollen. Interestingly, the CD4 T cell response to Art v 1 involves only one single immunodominant peptide, Art v 1(25-36) (KCIEWEKAQHGA), and is highly associated with the expression of HLA-DR1. Therefore, we investigated the molecular basis of this unusual immunodominance among allergens. Using artificial APC expressing exclusively HLA-DRB1*0101 and HLA-DRA*0101, we formally showed that DR1 acts as restriction element for Art v 1(25-36)-specific T cell responses. Further assessment of binding of Art v 1(25-36) to artificial HLA-DR molecules revealed that its affinity was high for HLA-DR1. Amino acid I27 was identified as anchor residue interacting with DR molecules in pocket P1. Additionally, Art v 1(25-36) bound with high affinity to HLA-DRB1*0301 and *0401, moderately to HLA-DRB1*1301 and HLA-DRB5*0101, and weakly to HLA-DRB1*1101 and *1501. T cell activation was also inducible by Art v 1(25-36)-loaded, APC-expressing HLA molecules other than DR1, indicating degeneracy of peptide binding and promiscuity of TCR recognition. Specific binding of HLA-DRB1*0101 tetramers containing Art v 1(19-36) allowed the identification of Art v 1(25-36)-specific T cells by flow cytometry. In summary, the immunodominance of Art v 1(25-36) relies on its affinity to DR1, but is not dictated by it. Future investigations at the molecular HLA/peptide/TCR and cellular level using mugwort pollen allergy as a disease model may allow new insights into tolerance and pathomechanisms operative in type I allergy, which may instigate new, T cell-directed strategies in specific immunotherapy.
机译:超过95%的艾蒿花粉过敏个人对艾蒿花粉中的主要过敏原Art v 1敏感。有趣的是,对Art v 1的CD4 T细胞应答仅涉及一种单一的免疫优势肽Art v 1(25-36)(KCIEWEKAQHGA),并且与HLA-DR1的表达高度相关。因此,我们调查了变应原之间这种异常的免疫优势的分子基础。使用专门表达HLA-DRB1 * 0101和HLA-DRA * 0101的人工APC,我们正式表明DR1充当Art v 1(25-36)特异性T细胞反应的限制元件。进一步评估Art v 1(25-36)与人工HLA-DR分子的结合,发现其对HLA-DR1的亲和力很高。氨基酸I27被鉴定为与口袋P1中的DR分子相互作用的锚残基。此外,Art v 1(25-36)与HLA-DRB1 * 0301和* 0401具有高亲和力,与HLA-DRB1 * 1301和HLA-DRB5 * 0101具有中等亲和力,而与HLA-DRB1 * 1101和* 1501具有弱亲和力。 T细胞活化还可以通过Art v 1(25-36)加载的,表达DRC以外的表达APC的HLA分子诱导,这表明肽结合的变性和TCR识别的混杂。包含Art v 1(19-36)的HLA-DRB1 * 0101四聚体的特异性结合可以通过流式细胞术鉴定Art v 1(25-36)特异性T细胞。总之,Art v 1(25-36)的免疫优势取决于其对DR1的亲和力,但不受它的支配。使用艾蒿花粉变态反应作为疾病模型的分子HLA /肽/ TCR和细胞水平的未来研究可能会为I型变态反应的耐受性和致病机理提供新见解,这可能会激发针对特定免疫疗法的新的T细胞定向策略。

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