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鉴定和回顾性验证丙型肝炎病毒 4 型蛋白组中的 T 细胞表位:一种加速表位驱动疫苗开发的方法。

Identification and retrospective validation of T-cell epitopes in the hepatitis C virus genotype 4 proteome: an accelerated approach toward epitope-driven vaccine development.

机构信息

a Department of Chemistry; School of Sciences and Engineering; The American University in Cairo; New Cairo, Egypt.

出版信息

Hum Vaccin Immunother. 2014;10(8):2366-77. doi: 10.4161/hv.29177.

DOI:10.4161/hv.29177
PMID:25424944
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4896781/
Abstract

With over 150 million people chronically infected worldwide and millions more infected annually, hepatitis C continues to pose a burden on the global healthcare system. The standard therapy of hepatitis C remains expensive, with severe associated side effects and inconsistent cure rates. Vaccine development against the hepatitis C virus has been hampered by practical and biological challenges posed by viral evasion mechanisms. Despite these challenges, HCV vaccine research has presented a number of candidate vaccines that progressed to phase II trials. However, those efforts focused mainly on HCV genotypes 1 and 2 as vaccine targets and barely enough attention was given to genotype 4, the variant most prevalent in the Middle East and central Africa. We describe herein the in silico identification of highly conserved and immunogenic T-cell epitopes from the HCV genotype 4 proteome, using the iVAX immunoinformatics toolkit, as targets for an epitope-driven vaccine. We also describe a fast and inexpensive approach for results validation using the empirical data on the Immune Epitope Database (IEDB) as a reference. Our analysis identified 90 HLA class I epitopes of which 20 were found to be novel and 19 more had their binding predictions retrospectively validated; empirical data for the remaining 51 epitopes was insufficient to validate their binding predictions. Our analysis also identified 14 HLA class II epitopes, of which 8 had most of their binding predictions validated. Further investigation is required regarding the efficacy of the identified epitopes as vaccine targets in populations where HCV genotype 4 is most prevalent.

摘要

全球有超过 1.5 亿人慢性感染,每年还有数百万人新感染,丙型肝炎继续给全球医疗保健系统带来负担。丙型肝炎的标准治疗仍然昂贵,存在严重的相关副作用和不一致的治愈率。由于病毒逃避机制带来的实际和生物学挑战,丙型肝炎病毒的疫苗开发一直受到阻碍。尽管存在这些挑战,但 HCV 疫苗研究已经提出了许多候选疫苗,这些疫苗已经进入 II 期临床试验。然而,这些努力主要集中在 HCV 基因型 1 和 2 作为疫苗靶点上,对基因型 4 几乎没有足够的关注,基因型 4 是中东和中非最常见的变异。我们在此描述了使用 iVAX 免疫信息学工具包,从 HCV 基因型 4 蛋白质组中鉴定高度保守和免疫原性 T 细胞表位的计算方法,作为基于表位的疫苗的靶点。我们还描述了一种快速且廉价的方法,使用免疫表位数据库(IEDB)上的经验数据作为参考来验证结果。我们的分析确定了 90 个 HLA Ⅰ类表位,其中 20 个是新的,19 个更多的是回顾性验证了它们的结合预测;对于其余 51 个表位的经验数据不足以验证它们的结合预测。我们的分析还确定了 14 个 HLA Ⅱ类表位,其中 8 个的结合预测得到了大部分验证。需要进一步研究在丙型肝炎基因型 4 最流行的人群中,鉴定的表位作为疫苗靶点的功效。

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