Identification of T-cell epitopes using allele-specific ligand motifs.

Behring Institute Mitteilungen Pub Date : 1994-12-01
S Stevanović, H G Rammensee
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Abstract

In order to facilitate the identification of T-cell epitopes as useful components of synthetic vaccines, we investigated the role of MHC molecules as the restriction element for the recognition of epitopes by the alpha beta receptor of T cells. MHC molecules are able to present thousands of different peptides to T cells, with all the peptides presented by one distinct type of MHC sharing common structural features. Our group analyzed these common characteristics concerning peptide length (only MHC I ligands) and anchor positions (MHC I and II ligands) occupied by a small set of closely related amino acids. Until now, for more than fifty MHC proteins allele-specific "peptide motifs" have been defined. The exact knowledge of MHC I peptide motifs allows for a prediction of CTL epitopes, and this kind of prediction has been successful in many cases over the last three years.

利用等位基因特异性配体基序鉴定t细胞表位。
为了方便鉴定T细胞表位作为合成疫苗的有用成分,我们研究了MHC分子作为T细胞α - β受体识别表位的限制性元件的作用。MHC分子能够将数千种不同的肽呈现给T细胞,而一种不同类型的MHC所呈现的所有肽都具有共同的结构特征。我们的研究小组分析了这些共同的特征,包括肽长度(只有MHC I配体)和锚位(MHC I和II配体)被一小组密切相关的氨基酸占据。到目前为止,已经确定了50多个MHC蛋白的等位基因特异性“肽基序”。MHC I肽基序的确切知识允许预测CTL表位,这种预测在过去三年中在许多情况下都是成功的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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