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某些氨基酸取代的进化意义及其对HIV-1针对HLA的A*0201和B*27免疫原性的影响。

The evolutionary significance of certain amino acid substitutions and their consequences for HIV-1 immunogenicity toward HLA's A*0201 and B*27.

作者信息

Hecht Luke, Dormer Anton

机构信息

Institute of Evolutionary Biology, The University of Edinburgh, Kings Buildings, Ashworth Laboratories, West Mains Road, Edinburgh EH9 3JT.

出版信息

Bioinformation. 2013 Mar 19;9(6):315-20. doi: 10.6026/97320630009315. Print 2013.

DOI:10.6026/97320630009315
PMID:23745018
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3607191/
Abstract

In silico tools are employed to examine the evolutionary relationship to possible vaccine peptide candidates' development. This perspective sheds light on the proteomic changes affecting the creation of HLA specific T-cell stimulating peptide vaccines for HIV. Full-length sequences of the envelope protein of the HIV subtypes A, B, C and D were obtained through the NCBI Protein database were aligned using CLUSTALW. They were then analyzed using RANKPEP specific to Human Leukocyte Antigen A02 and B27. Geneious was used to catalogue the collected gp160 sequences and to construct a phylogenic tree. Mesquite was employed for ancestral state reconstruction to infer the order of amino acid substitutions in the epitopes examined. The results showed that consensus peptide identified SLAEKNITI had changes that indicated predicted escape mutation in strains of HIV responding to pressure exerted by CD8+ cells expressing HLA A02. The predominating 9-mers IRIGPGQAF of gp120 are significantly less immunogenic toward HLA B27 than to HLA A02. The data confirms previous findings on the importance for efficacious binding, of an arginine residue at the 2(nd) position of the gag SL9 epitope, and extends this principle to other epitopes which interacts with HLA B27. This study shows that the understanding of viral evolution relating T-cell peptide vaccine design is a development that has much relevance for the creation of personalized therapeutics for HIV treatment.

摘要

利用计算机工具来研究与可能的疫苗肽候选物开发的进化关系。这一观点揭示了影响针对HIV的HLA特异性T细胞刺激肽疫苗创建的蛋白质组学变化。通过NCBI蛋白质数据库获得HIV A、B、C和D亚型包膜蛋白的全长序列,使用CLUSTALW进行比对。然后使用针对人类白细胞抗原A02和B27的RANKPEP进行分析。使用Geneious对收集的gp160序列进行编目并构建系统发育树。使用Mesquite进行祖先状态重建,以推断所检查表位中氨基酸取代的顺序。结果表明,鉴定出的共有肽SLAEKNITI发生了变化,表明在对表达HLA A02的CD8 +细胞施加的压力作出反应的HIV毒株中存在预测的逃逸突变。gp120中占主导地位的9聚体IRIGPGQAF对HLA B27的免疫原性明显低于对HLA A02的免疫原性。数据证实了先前关于gag SL9表位第2位精氨酸残基对有效结合重要性的发现,并将这一原则扩展到与HLA B27相互作用的其他表位。这项研究表明,对与T细胞肽疫苗设计相关的病毒进化的理解对于创建用于HIV治疗的个性化疗法具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9dc7/3607191/d9bbf82acdde/97320630009315F4.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9dc7/3607191/6fcc992b7d81/97320630009315F1.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9dc7/3607191/0d03cd697f9d/97320630009315F2.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9dc7/3607191/3a41c5e8c4c5/97320630009315F3.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9dc7/3607191/d9bbf82acdde/97320630009315F4.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9dc7/3607191/6fcc992b7d81/97320630009315F1.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9dc7/3607191/0d03cd697f9d/97320630009315F2.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9dc7/3607191/3a41c5e8c4c5/97320630009315F3.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9dc7/3607191/d9bbf82acdde/97320630009315F4.jpg

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