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慢性感染和康复感染之间假定的2型丙型肝炎病毒F蛋白的差异反应性。

Differential reactivity of putative genotype 2 hepatitis C virus F protein between chronic and recovered infections.

作者信息

Chuang Wing Chia-Ming, Allain Jean-Pierre

机构信息

Department of Haematology, Division of Transfusion Medicine, Cambridge Blood Centre, University of Cambridge, Long Road, Cambridge CB2 2PT, UK.

出版信息

J Gen Virol. 2008 Aug;89(Pt 8):1890-1900. doi: 10.1099/vir.0.83677-0.

Abstract

To date, all studies regarding hepatitis C virus (HCV) F protein have been based on expression in vitro/in vivo of recombinant protein or monoclonal antibodies derived from genotype 1a or 1b sequences, but not from other genotypes. The objective of this study was to prepare a putative genotype 2 recombinant F protein and evaluate its reactivity in plasma from individuals with chronic HCV infection or who had recovered from infection. One genotype 2 strain was selected for F protein (F-2) and core expression in bacterial culture. An ELISA was developed and applied to samples from patients with chronic infection or recovered infection of various genotypes. The anti-F-2 response in 117 samples showed a significantly higher reactivity in chronic than in recovered HCV-infected blood donors (P<0.001), but no difference was found among genotypes. However, the correlation between anti-F and anti-core was more significant in genotypes 1 and 2 than in genotype 3. Anti-F-2 titres were also significantly higher in chronic than in recovered individuals (P<0.0001). Antibody titres to recombinant genotype 2 core protein or to genotype 1 multiple proteins used in commercial anti-HCV assays paralleled the anti-F-2 end-point antibody titre. This study thus demonstrated the antigenicity of genotype 2 HCV F protein, although the exact location of the natural frameshift position remains unknown. The difference in anti-F-2 response between chronic and recovered infection, the cross-reactivity irrespective of genotype and the correlation of antibody response with structural and non-structural antigens suggest that the immune response to F protein is an integral part of the natural HCV infection.

摘要

迄今为止,所有关于丙型肝炎病毒(HCV)F蛋白的研究均基于重组蛋白或源自1a或1b基因型序列而非其他基因型的单克隆抗体的体外/体内表达。本研究的目的是制备一种假定的2型重组F蛋白,并评估其在慢性HCV感染个体或已从感染中康复个体的血浆中的反应性。选择了一个2型毒株用于在细菌培养物中表达F蛋白(F-2)和核心蛋白。开发了一种酶联免疫吸附测定(ELISA)并应用于来自各种基因型慢性感染或已康复感染患者的样本。117份样本中的抗F-2反应显示,慢性HCV感染献血者的反应性显著高于康复者(P<0.001),但各基因型之间未发现差异。然而,1型和2型中抗F与抗核心之间的相关性比3型更显著。慢性个体的抗F-2滴度也显著高于康复个体(P<0.0001)。商业抗HCV检测中使用的重组2型核心蛋白或1型多种蛋白的抗体滴度与抗F-2终点抗体滴度平行。因此,本研究证明了2型HCV F蛋白的抗原性,尽管自然移码位置的确切位置仍然未知。慢性感染和康复感染之间抗F-2反应的差异、不考虑基因型的交叉反应性以及抗体反应与结构和非结构抗原的相关性表明,对F蛋白的免疫反应是自然HCV感染的一个组成部分。

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