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Identification of a novel epitope in the C terminus of hepatitis C virus-E2 protein that induces potent and cross-reactive neutralizing antibodies

机译:在丙型肝炎病毒E2蛋白C末端新表位的鉴定,该表位诱导有效和交叉反应的中和抗体

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摘要

Hepatitis C virus (HCV) is a leading cause of chronic viral hepatitis, but an effective vaccine is still not available to prevent infection. Use of neutralizing antibodies could be a potential therapeutic option. In this study, the presence of anti-HCV antibodies in HCV-infected patients was assessed from 50 patients and the presence of neutralizing antibodies was examined using `hepatitis C virus-like particles'. Antibodies from two samples exhibited significant inhibitory activity, suggesting that these may neutralize viral infection. Antigenic determinants generating the neutralizing antibodies from these two samples were delineated by epitope mapping using the core, E1 and E2 regions and a stretch of 45 amino acid peptide (E2C45) derived from the C-terminal region of HCV-E2 protein (aa 634-679) was designed. Results suggest that this hitherto uncharacterized region has the potential to generate neutralizing antibodies against HCV and thus be effective in preventing virus entry into liver cells. Computational analysis of the structure of the modelled peptide (E2C45) suggested high conformational entropy for this region. Furthermore, E2C45 peptide-generated antibodies could block virus entry and monoclonal antibodies generated against this peptide could also significantly reduce virus replication in a cell culture system. It is possible that the inhibition could be partly due to a conformational alteration of the CD81-binding region, preventing virus attachment to liver cells. In conclusion, this work focused on the discovery of a novel epitope at the C terminus of E2 that induces potent neutralizing antibodies in HCV-infected patients.
机译:丙型肝炎病毒(HCV)是导致慢性病毒性肝炎的主要原因,但仍没有有效的疫苗来预防感染。使用中和抗体可能是潜在的治疗选择。在这项研究中,从50位患者中评估了HCV感染患者中抗HCV抗体的存在,并使用“丙型肝炎病毒样颗粒”检查了中和抗体的存在。来自两个样品的抗体表现出显着的抑制活性,表明它们可以中和病毒感染。使用抗原表位,E1和E2区域以及源自HCV-E2蛋白C末端区域的45个氨基酸肽段(E2C45),通过表位作图来描述从这两个样品中产生中和抗体的抗原决定簇。 679)的设计。结果表明,该迄今未鉴定的区域具有产生针对HCV的中和抗体的潜力,因此可有效防止病毒进入肝细胞。对建模肽(E2C45)结构的计算分析表明,该区域具有很高的构象熵。此外,E2C45肽生成的抗体可能会阻止病毒进入,针对该肽生成的单克隆抗体也可能会大大减少病毒在细胞培养系统中的复制。抑制作用可能部分是由于CD81结合区的构象改变,从而阻止了病毒附着在肝细胞上。总之,这项工作的重点是在E2的C末端发现一个新的表位,该表位在HCV感染的患者中诱导有效的中和抗体。

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