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通过计算机模拟鉴定II类主要组织相容性复合体的超级类型

In silico identification of supertypes for class II MHCs.

作者信息

Doytchinova Irini A, Flower Darren R

机构信息

Edward Jenner Institute for Vaccine Research, Compton, Berkshire, UK.

出版信息

J Immunol. 2005 Jun 1;174(11):7085-95. doi: 10.4049/jimmunol.174.11.7085.

Abstract

The development of epitope-based vaccines, which have wide population coverage, is greatly complicated by MHC polymorphism. The grouping of alleles into supertypes, on the basis of common structural and functional features, addresses this problem directly. In the present study we applied a combined bioinformatics approach, based on analysis of both protein sequence and structure, to identify similarities in the peptide binding sites of 2225 human class II MHC molecules, and thus define supertypes and supertype fingerprints. Two chemometric techniques were used: hierarchical clustering using three-dimensional Comparative Similarity Indices Analysis fields and nonhierarchical k-means clustering using sequence-based z-descriptors. An average consensus of 84% was achieved, i.e., 1872 of 2225 class II molecules were classified in the same supertype by both techniques. Twelve class II supertypes were defined: five DRs, three DQs, and four DPs. The HLA class II supertypes and their fingerprints given in parenthesis are DR1 (Trp(9beta)), DR3 (Glu(9beta), Gln(70beta), and Gln/Arg(74beta)), DR4 (Glu(9beta), Gln/Arg(70beta), and Glu/Ala(74beta)), DR5 (Glu(9beta), Asp(70beta)), and DR9 (Lys/Gln(9beta)); DQ1 (Ala/Gly(86beta)), DQ2 (Glu(86beta), Lys(71beta)), and DQ3 (Glu(86beta), Thr/Asp(71beta)); DPw1 (Asp(84beta) and Lys(69beta)), DPw2 (Gly/Val(84beta) and Glu(69beta)), DPw4 (Gly/Val(84beta) and Lys(69beta)), and DPw6 (Asp(84beta) and Glu(69beta)). Apart from the good agreement between known binding motifs and our classification, several new supertypes, and corresponding thematic binding motifs, were also defined.

摘要

基于表位的疫苗具有广泛的人群覆盖率,但其开发因MHC多态性而变得极为复杂。根据共同的结构和功能特征将等位基因分组为超型,可直接解决这一问题。在本研究中,我们应用了一种基于蛋白质序列和结构分析的联合生物信息学方法,以识别2225个人类II类MHC分子的肽结合位点中的相似性,从而定义超型和超型指纹。使用了两种化学计量技术:使用三维比较相似性指数分析字段的层次聚类和使用基于序列的z描述符的非层次k均值聚类。达成了84%的平均一致性,即2225个II类分子中的1872个通过两种技术被分类到同一超型中。定义了12个II类超型:5个DR、3个DQ和4个DP。括号中给出的HLA II类超型及其指纹为DR1(Trp(9β))、DR3(Glu(9β)、Gln(70β)和Gln/Arg(74β))、DR4(Glu(9β)、Gln/Arg(70β)和Glu/Ala(74β))、DR5(Glu(9β)、Asp(70β))和DR9(Lys/Gln(9β));DQ1(Ala/Gly(86β))、DQ2(Glu(86β)、Lys(71β))和DQ3(Glu(86β)、Thr/Asp(71β));DPw1(Asp(84β)和Lys(69β))、DPw2(Gly/Val(84β)和Glu(69β))、DPw4(Gly/Val(84β)和Lys(69β))和DPw6(Asp(84β)和Glu(69β))。除了已知结合基序与我们的分类之间的良好一致性外,还定义了几个新的超型以及相应的主题结合基序。

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