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模拟戊型肝炎病毒衣壳表位的噬菌体展示肽。

Phage-displayed peptides that mimic epitopes of hepatitis E virus capsid.

作者信息

Larralde Osmany, Petrik Juraj

机构信息

Microbiology RDI, Scottish National Blood Transfusion Service, NHS National Services Scotland, 21 Ellen's Glen Road, Edinburgh, EH17 7QT, UK.

出版信息

Med Microbiol Immunol. 2017 Aug;206(4):301-309. doi: 10.1007/s00430-017-0507-0. Epub 2017 Apr 22.

DOI:10.1007/s00430-017-0507-0
PMID:28434129
Abstract

Hepatitis E is an emerging zoonotic infection of increasing public health threat for the UK, especially for immunosuppressed individuals. A human recombinant vaccine has been licensed only in China and is not clear whether it protects against hepatitis E virus (HEV) genotype 3, the most prevalent in Europe. The aim of this study was to use phage display technology as a tool to identify peptides that mimic epitopes of HEV capsid (mimotopes). We identified putative linear and conformational mimotopes using sera from Scottish blood donors that have the immunological imprint of past HEV infection. Four mimotopes did not have homology with the primary sequence of HEV ORF2 capsid but competed effectively with a commercial HEV antigen for binding to anti-HEV reference serum. When the reactivity profile of each mimotope was compared with Wantai HEV-IgG ELISA, the most sensitive HEV immunoassay, mimotopes showed 95.2-100% sensitivity while the specificity ranged from 81.5 to 95.8%. PepSurf algorithm was used to map affinity-selected peptides onto the ORF2 crystal structure of HEV genotype 3, which predicted that these four mimototopes are clustered in the P domain of ORF2 capsid, near conformational epitopes of anti-HEV neutralising monoclonal antibodies. These HEV mimotopes may have potential applications in the design of structural vaccines and the development of new diagnostic tests.

摘要

戊型肝炎是一种新出现的人畜共患感染病,对英国的公共卫生威胁日益增加,对免疫抑制个体尤其如此。一种重组人疫苗仅在中国获得许可,尚不清楚它是否能预防戊型肝炎病毒(HEV)3型,这是欧洲最常见的基因型。本研究的目的是利用噬菌体展示技术作为工具,鉴定模拟HEV衣壳表位的肽(模拟表位)。我们使用来自苏格兰献血者的血清鉴定出推定的线性和构象模拟表位,这些血清具有过去HEV感染的免疫印记。四个模拟表位与HEV ORF2衣壳的一级序列没有同源性,但能与一种商业HEV抗原有效竞争,以结合抗HEV参考血清。当将每个模拟表位的反应性谱与最灵敏的HEV免疫测定法——万泰HEV-IgG ELISA进行比较时,模拟表位的灵敏度为95.2-100%,而特异性范围为81.5至95.8%。使用PepSurf算法将亲和选择的肽映射到HEV 3型的ORF2晶体结构上,预测这四个模拟表位聚集在ORF2衣壳的P结构域中,靠近抗HEV中和单克隆抗体的构象表位。这些HEV模拟表位可能在结构疫苗设计和新诊断测试开发中具有潜在应用。

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Hepatitis E: Discovery, global impact, control and cure.戊型肝炎:发现、全球影响、控制与治愈
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