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庚型肝炎病毒(GB-C病毒)颗粒的特性:核衣壳的证据及E1蛋白上游序列的表达

Characterization of hepatitis G virus (GB-C virus) particles: evidence for a nucleocapsid and expression of sequences upstream of the E1 protein.

作者信息

Xiang J, Klinzman D, McLinden J, Schmidt W N, LaBrecque D R, Gish R, Stapleton J T

机构信息

Department of Internal Medicine, Iowa City Veterans Administration Medical Center, and The University of Iowa College of Medicine 52242, USA.

出版信息

J Virol. 1998 Apr;72(4):2738-44. doi: 10.1128/JVI.72.4.2738-2744.1998.

Abstract

Hepatitis G virus (HGV or GB-C virus) is a newly described virus that is closely related to hepatitis C virus (HCV). Based on sequence analysis and by evaluation of translational initiation codon preferences utilized during in vitro translation, HGV appears to have a truncated or absent core protein at the amino terminus of the HGV polyprotein. Consequently, the biophysical properties of HGV may be very different from those of HCV. To characterize HGV particle types, we evaluated plasma from chronically infected individuals with and without concomitant HCV infection by using sucrose gradient centrifugation, isopycnic banding in cesium chloride, and saline density flotation centrifugation. Similar to HCV, HGV particles included an extremely-low-density virion particle (1.07 to 1.09 g/ml) and a nucleocapsid of approximately 1.18 g/ml. One major difference between the particle types was that HGV was consistently more stable in cesium chloride than HCV. Plasma samples from chronically HGV-infected individuals and controls were assessed by a synthetic peptide-based immunoassay to determine if they contained HGV antibody specific for a conserved region in the coding region upstream of the E1 protein. Chronically HGV-infected individuals contained antibody to the HGV core protein peptide, whereas no binding to a hepatitis A virus peptide control was observed. Competitive inhibition of binding to the HGV peptide confirmed the specificity of the assay. These data indicate that HGV has a nucleocapsid and that at least part of the putative core region of HGV is expressed in vivo.

摘要

庚型肝炎病毒(HGV或GB-C病毒)是一种新发现的病毒,与丙型肝炎病毒(HCV)密切相关。基于序列分析以及对体外翻译过程中使用的翻译起始密码子偏好性的评估,HGV在其多聚蛋白的氨基末端似乎有一个截短的或缺失的核心蛋白。因此,HGV的生物物理特性可能与HCV有很大不同。为了表征HGV颗粒类型,我们通过蔗糖梯度离心、氯化铯等密度区带离心和盐水密度浮选离心,对伴有或不伴有HCV感染的慢性感染个体的血浆进行了评估。与HCV相似,HGV颗粒包括极低密度的病毒粒子(1.07至1.09克/毫升)和大约1.18克/毫升的核衣壳。颗粒类型之间的一个主要差异是,HGV在氯化铯中始终比HCV更稳定。通过基于合成肽的免疫测定法对慢性HGV感染个体和对照的血浆样本进行评估,以确定它们是否含有针对E1蛋白上游编码区保守区域的HGV抗体。慢性HGV感染个体含有针对HGV核心蛋白肽的抗体,而未观察到与甲型肝炎病毒肽对照的结合。对与HGV肽结合的竞争性抑制证实了该测定法的特异性。这些数据表明HGV有一个核衣壳,并且HGV假定的核心区域至少有一部分在体内表达。

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