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能否预测用于疫苗接种的、受MHC I类分子限制的细胞毒性T淋巴细胞的抗原肽?

Can one predict antigenic peptides for MHC class I-restricted cytotoxic T lymphocytes useful for vaccination?

作者信息

Calin-Laurens V, Trescol-Biémont M C, Gerlier D, Rabourdin-Combe C

机构信息

Immunobiologie moléculaire, UMR 49, CNRS-ENS-Lyon, France.

出版信息

Vaccine. 1993;11(9):974-8. doi: 10.1016/0264-410x(93)90389-f.

DOI:10.1016/0264-410x(93)90389-f
PMID:7692684
Abstract

The cytotoxic T-lymphocyte (CTL) response can be crucial for efficient immunological control of intracellular pathogens and the MHC class I-restricted CTL have a major role to play in this process. They recognize complexes associating antigen-derived peptides with MHC class I molecules expressed on infected target cells. The characterization of these antigenic peptides is thus a key issue for developing vaccines efficient in inducing specific CTL. Recently, by sequencing the whole set of self-peptides eluted from a given MHC class I molecule, Falk and colleagues have found that they have a homogeneous 8-10 residue length and contain allele-specific peptidic motifs with two conservative dominant anchor residues. The existence of consensus motifs opens the way for a strategy to predict the MHC class I-restricted T-cell epitopes and here we discuss such an approach using hen egg lysozyme (HEL) as an antigenic model. Two HEL peptides corresponding to allele-specific motifs were found, HEL(49-56) and HEL(70-78) peptides, which can associate with MHC class I H-2Kb and H-2Db molecules, respectively. The HEL peptide HEL(70-78) was found to be able to induce HEL-specific CTL in H-2b mice also. Moreover, using an empiricial approach, we have also characterized the N-terminal HEL(1-17) peptide as an immunodominant antigenic peptide in the H-2k haplotype. This peptide presented by H-2Kk molecules neither contained the corresponding allele-specific binding motif nor fitted the expected 8-10 residue length.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

细胞毒性T淋巴细胞(CTL)反应对于细胞内病原体的有效免疫控制至关重要,而MHC I类限制性CTL在此过程中发挥着主要作用。它们识别感染的靶细胞上表达的与MHC I类分子相关联的抗原衍生肽复合物。因此,这些抗原肽的表征是开发有效诱导特异性CTL的疫苗的关键问题。最近,通过对从给定的MHC I类分子洗脱的整套自身肽进行测序,福尔克及其同事发现它们具有均一的8至10个残基长度,并包含具有两个保守显性锚定残基的等位基因特异性肽基序。共有基序的存在为预测MHC I类限制性T细胞表位的策略开辟了道路,在此我们讨论一种使用鸡蛋清溶菌酶(HEL)作为抗原模型的方法。发现了两条与等位基因特异性基序相对应的HEL肽,即HEL(49 - 56)肽和HEL(70 - 78)肽,它们分别可与MHC I类H - 2Kb和H - 2Db分子结合。还发现HEL肽HEL(70 - 78)在H - 2b小鼠中也能够诱导HEL特异性CTL。此外,通过经验方法,我们还将N端HEL(1 - 17)肽鉴定为H - 2k单倍型中的免疫显性抗原肽。由H - 2Kk分子呈递的该肽既不包含相应的等位基因特异性结合基序,也不符合预期的8至10个残基长度。(摘要截短于250字)

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