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利用特异性矩阵聚类法定义HLA分子的超型

Definition of supertypes for HLA molecules using clustering of specificity matrices.

作者信息

Lund Ole, Nielsen Morten, Kesmir Can, Petersen Anders Gorm, Lundegaard Claus, Worning Peder, Sylvester-Hvid Christina, Lamberth Kasper, Røder Gustav, Justesen Sune, Buus Søren, Brunak Søren

机构信息

Center for Biological Sequence Analysis, BioCentrum-DTU, Technical University of Denmark, Building 208, 2800 Lyngby, Denmark.

出版信息

Immunogenetics. 2004 Mar;55(12):797-810. doi: 10.1007/s00251-004-0647-4. Epub 2004 Feb 13.

Abstract

Major histocompatibility complex (MHC) proteins are encoded by extremely polymorphic genes and play a crucial role in immunity. However, not all genetically different MHC molecules are functionally different. Sette and Sidney (1999) have defined nine HLA class I supertypes and showed that with only nine main functional binding specificities it is possible to cover the binding properties of almost all known HLA class I molecules. Here we present a comprehensive study of the functional relationship between all HLA molecules with known specificities in a uniform and automated way. We have developed a novel method for clustering sequence motifs. We construct hidden Markov models for HLA class I molecules using a Gibbs sampling procedure and use the similarities among these to define clusters of specificities. These clusters are extensions of the previously suggested ones. We suggest splitting some of the alleles in the A1 supertype into a new A26 supertype, and some of the alleles in the B27 supertype into a new B39 supertype. Furthermore the B8 alleles may define their own supertype. We also use the published specificities for a number of HLA-DR types to define clusters with similar specificities. We report that the previously observed specificities of these class II molecules can be clustered into nine classes, which only partly correspond to the serological classification. We show that classification of HLA molecules may be done in a uniform and automated way. The definition of clusters allows for selection of representative HLA molecules that can cover the HLA specificity space better. This makes it possible to target most of the known HLA alleles with known specificities using only a few peptides, and may be used in construction of vaccines. Supplementary material is available at http://www.cbs.dtu.dk/researchgroups/immunology/supertypes.html.

摘要

主要组织相容性复合体(MHC)蛋白由高度多态性的基因编码,在免疫中起关键作用。然而,并非所有基因不同的MHC分子在功能上都有差异。塞特和西德尼(1999年)定义了9种HLA I类超型,并表明仅9种主要的功能结合特异性就有可能涵盖几乎所有已知HLA I类分子的结合特性。在此,我们以统一且自动化的方式对所有具有已知特异性的HLA分子之间的功能关系进行了全面研究。我们开发了一种用于聚类序列基序的新方法。我们使用吉布斯采样程序为HLA I类分子构建隐马尔可夫模型,并利用这些模型之间的相似性来定义特异性簇。这些簇是先前提出的簇的扩展。我们建议将A1超型中的一些等位基因拆分为一个新的A26超型,将B27超型中的一些等位基因拆分为一个新的B39超型。此外,B8等位基因可能定义它们自己的超型。我们还利用已发表的多种HLA - DR类型的特异性来定义具有相似特异性的簇。我们报告说,先前观察到的这些II类分子的特异性可聚类为9类,这仅部分对应于血清学分类。我们表明,可以以统一且自动化的方式对HLA分子进行分类。簇的定义允许选择能更好地覆盖HLA特异性空间的代表性HLA分子。这使得仅用少数肽就能针对大多数具有已知特异性的已知HLA等位基因,并且可用于疫苗构建。补充材料可在http://www.cbs.dtu.dk/researchgroups/immunology/supertypes.html获取。

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