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HLA-A*3001的肽结合特异性表明其属于HLA-A3超型。

The peptide-binding specificity of HLA-A*3001 demonstrates membership of the HLA-A3 supertype.

作者信息

Lamberth Kasper, Røder Gustav, Harndahl Mikkel, Nielsen Morten, Lundegaard Claus, Schafer-Nielsen Claus, Lund Ole, Buus Soren

机构信息

Laboratory of Experimental Immunology, Faculty of Health Sciences, University of Copenhagen, Panum 18.3.12, Blegdamsvej 3B, 2200, Copenhagen, Denmark.

出版信息

Immunogenetics. 2008 Nov;60(11):633-43. doi: 10.1007/s00251-008-0317-z. Epub 2008 Sep 4.

DOI:10.1007/s00251-008-0317-z
PMID:18769915
Abstract

Human leukocyte antigen class I (HLA-I) molecules are highly polymorphic peptide receptors, which select and present endogenously derived peptide epitopes to CD8+ cytotoxic T cells (CTL). The specificity of the HLA-I system is an important component of the overall specificity of the CTL immune system. Unfortunately, the large and rapidly increasing number of known HLA-I molecules seriously complicates a comprehensive analysis of the specificities of the entire HLA-I system (as of June 2008, the international HLA registry holds >1,650 unique HLA-I protein entries). In an attempt to reduce this complexity, it has been suggested to cluster the different HLA-I molecules into "supertypes" of largely overlapping peptide-binding specificities. Obviously, the HLA supertype concept is only valuable if membership can be assigned with reasonable accuracy. The supertype assignment of HLA-A3001, a common HLA haplotype in populations of African descent, has variously been assigned to the A1, A3, or A24 supertypes. Using a biochemical HLA-A3001 binding assay, and a large panel of nonamer peptides and peptide libraries, we here demonstrate that the specificity of HLA-A*3001 most closely resembles that of the HLA-A3 supertype. We discuss approaches to supertype assignment and underscore the importance of experimental verification.

摘要

人类白细胞抗原 I 类(HLA-I)分子是高度多态的肽受体,其选择内源性衍生的肽表位并将其呈递给 CD8+ 细胞毒性 T 细胞(CTL)。HLA-I 系统的特异性是 CTL 免疫系统整体特异性的重要组成部分。不幸的是,已知的 HLA-I 分子数量庞大且迅速增加,这使得对整个 HLA-I 系统特异性的全面分析变得极为复杂(截至 2008 年 6 月,国际 HLA 登记处拥有超过 1650 个独特的 HLA-I 蛋白条目)。为了降低这种复杂性,有人建议将不同的 HLA-I 分子聚类为肽结合特异性基本重叠的“超型”。显然,只有能够以合理的准确性进行成员分配时,HLA 超型概念才具有价值。HLA-A3001 是非洲裔人群中常见的 HLA 单倍型,其超型分配在不同情况下被归为 A1、A3 或 A24 超型。通过生化 HLA-A3001 结合试验以及大量九肽和肽库,我们在此证明 HLA-A*3001 的特异性与 HLA-A3 超型最为相似。我们讨论了超型分配的方法,并强调了实验验证的重要性。

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