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丙型肝炎病毒包膜2蛋白的抗原结构

Antigenic structure of the hepatitis C virus envelope 2 protein.

作者信息

Zhang Z X, Sönnerborg A, Sällberg M

机构信息

Division of Clinical Virology, Karolinska Institute at Huddinge Hospital, Sweden.

出版信息

Clin Exp Immunol. 1994 Dec;98(3):382-7. doi: 10.1111/j.1365-2249.1994.tb05501.x.

Abstract

The antigenic structure of the envelope 2 (e2) protein of the hepatitis C virus (HCV) was characterized by the use of 70 synthetic peptides and 131 human sera from persons with antibodies to HCV. Among 34 overlapping peptides spanning the e2 protein of HCV, two major antigenic regions were located to residues 484-499 and residues 554-569. The sequence of the two major antigenic regions of the e2 protein are partly well conserved within the described types of HCV. Both regions contain two Cys residues in close proximity, and the region at residues 554-569 contains a putative N-glycosylation site, which are factors that previously have been suggested to affect the immune recognition of the e2 protein. Using substitution peptide analogues where each position within residues 484-499 and 554-569 were sequentially substituted by Ala or Gly, the most essential residues for antibody binding were found to be the Pro-498, Ala-499, Ala-566, Pro-567, and Pro-568. All of these, except for the Pro-498 and Ala-566, are conserved among different HCV strains. Also, according to previous studies, position 496 often shows variations, which could be explained by position 496 being contained within the antigenic region at residues 484-499. Interestingly, none of the Cys residues at positions 486, 494, 564 and 569 were found to be essential for antibody binding, indicating that these are not essential in maintaining the e2 antigenicity of the peptides. In a material of 114 confirmed anti-HCV positive sera, derived from patients during the acute or the chronic phase of HCV infection, the prevalence of antibodies to the two major linear antigenic regions of the e2 protein was found to be 55% among HCV RNA-positive sera, and 53% among HCV RNA-negative sera. In conclusion, we have identified and characterized two major linear antigenic regions outside the two hypervariable regions of the e2 protein. Since these regions are accessible to the B cells of the infected host, these two regions are likely to be surface exposed either on the precursor polyprotein or the native e2 protein. Also, we could confirm that antibodies to the e2 protein co-exist with HCV viraemia.

摘要

通过使用70种合成肽和131份来自丙型肝炎病毒(HCV)抗体阳性者的人血清,对HCV包膜2(E2)蛋白的抗原结构进行了表征。在跨越HCV E2蛋白的34种重叠肽中,两个主要抗原区域位于第484 - 499位残基和第554 - 569位残基处。E2蛋白的两个主要抗原区域的序列在所描述的HCV类型中部分保守。两个区域都紧邻两个半胱氨酸残基,并且第554 - 569位残基区域包含一个推定的N - 糖基化位点,这些都是先前已被认为会影响E2蛋白免疫识别的因素。使用替代肽类似物,其中第484 - 499位残基和第554 - 569位残基内的每个位置依次被丙氨酸或甘氨酸取代,发现抗体结合的最关键残基是Pro - 498、Ala - 499、Ala - 566、Pro - 567和Pro - 568。除Pro - 498和Ala - 566外,所有这些残基在不同的HCV毒株中都是保守的。此外,根据先前的研究,第496位经常出现变异,这可以解释为第496位包含在第484 - 499位残基的抗原区域内。有趣的是,发现第486、494、564和569位的半胱氨酸残基对于抗体结合都不是必需的,这表明这些残基对于维持肽的E2抗原性不是必需的。在114份确诊为抗HCV阳性血清的材料中,这些血清来自HCV感染急性期或慢性期的患者,发现E2蛋白的两个主要线性抗原区域的抗体在HCV RNA阳性血清中的流行率为55%,在HCV RNA阴性血清中的流行率为53%。总之,我们已经鉴定并表征了E2蛋白两个高变区之外的两个主要线性抗原区域。由于这些区域可被受感染宿主的B细胞识别,这两个区域可能在前体多蛋白或天然E2蛋白上暴露于表面。此外,我们可以确认E2蛋白抗体与HCV病毒血症共存。

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