B Georges, H Gras-Masse, P Maes, A Capron, A Tartar, C Auriault
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引用次数: 0
摘要
为了表征MHC II类分子HLA-DR3的肽结合基序,我们对从结合槽中洗脱的肽池或单肽进行了测序。鉴定的锚定残基与不同小组报告的肽结合和测序研究一致。4个位置似乎占主导地位(i, i + 3, i + 5, i + 8),而2个次要位置(i + 1, i + 2)可以合作以促进结合。根据本文定义的所有标准和文献,我们提出了DR3特异性的锚定基序,并在曼氏血吸虫抗原的序列上进行了测试。鉴定的6个假定表位中有3个与在人类和动物模型中通过实验性免疫确定的免疫优势区具有共同序列。扩展到其他等位基因,这种方法可以适用于确定潜在的免疫优势肽疫苗有用。
[Analysis of peptides associated with class II MHC molecules, HLA-DR3: implication for the prediction of peptides useful for vaccines].
In order to characterize peptide binding motifs of MHC class II molecules HLA-DR3, we have sequenced pool or single peptides eluted from the binding groove. Anchor residues identified are in agreement with peptide binding and sequencing studies reported by different groups. Four positions seem to be dominant (i, i + 3, i + 5, i + 8) while 2 secondary positions (i + 1, i + 2) could cooperate to facilitate binding. According to all the criteria define here and the literature, we propose an anchor motif specific for DR3, which has been tested on the sequence of an antigen from Schistosoma mansoni. Three out of 6 putative epitopes identified share common sequences with immunodominant regions determined in humans and by experimental immunizations in animal models. Extended to other alleles, this approach could be suitable to define potentially immunodominant peptides useful for vaccines.