Development of a Multiple-Epitope-Based Vaccine for Hepatitis C Virus Genotypes 1a and 1b: an in-silico reverse vaccinology approach.

In silico pharmacology Pub Date : 2024-11-09 eCollection Date: 2024-01-01 DOI:10.1007/s40203-024-00275-4

Enakshi Das, Mahesh Samantaray, Kajal Abrol, Jayarani Basumatari, Shilpa Sri Pushan, Amutha Ramaswamy

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Abstract

The Hepatitis C virus (HCV) is a blood-transmitted virus responsible for persistent inflammation, presenting a substantial worldwide health challenge. HCV, characterized by a positive-stranded ribonucleic acid genome, possesses an intricate genetic makeup encoding both structural and non-structural proteins, crucial for sustaining its life cycle. The Direct Acting Antivirals have revolutionized the treatment landscape of HCV promoting higher Sustained Virological Response rates. Despite significant advancements in treatment, no vaccines are currently available against HCV. The development of effective HCV vaccines becomes challenging as the genetic diversity of HCV virus and its complex nature of the immune response required for protection. In this work, the immunoinformatics methods were utilized to develop a multiple-epitope-based vaccine towards an effective treatment against the viral HCV polyprotein. The vaccine was constructed by T-cell epitopes extracted from the viral polyprotein of HCV genotypes 1a and 1b. The vaccine was highly antigenic, non-toxic, and non-allergenic. Effective binding of the designed vaccine construct was studied by forming complexes with the human immune Toll-Like Receptors; TLR3 and TLR8. The MD simulation of these receptor-vaccine complexes were performed for 50ns and the immunological simulation of modeled vaccine in presence of receptors for 365 days timeline validated the stability of the constructed vaccine. The in-silico vaccine construct developed from this work might be beneficial as prophylactic measures against the HCV variants, if explored further in in vivo and in vitro methods. Consequently, this research outcome is presumed to have implications in the development of safer and more efficient vaccines for lethal diseases.

Graphical abstract:

Supplementary information: The online version contains supplementary material available at 10.1007/s40203-024-00275-4.

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针对丙型肝炎病毒基因 1a 型和 1b 型开发基于多表的疫苗：硅内反向疫苗学方法。

丙型肝炎病毒（HCV）是一种血液传播病毒，可导致持续性炎症，给全世界的健康带来巨大挑战。丙型肝炎病毒（HCV）以正链核糖核酸基因组为特征，拥有复杂的基因组成，编码结构蛋白和非结构蛋白，对维持其生命周期至关重要。直接作用抗病毒药物彻底改变了 HCV 的治疗格局，提高了持续病毒学应答率。尽管在治疗方面取得了重大进展，但目前还没有针对 HCV 的疫苗。由于 HCV 病毒的遗传多样性及其保护所需的免疫反应的复杂性，开发有效的 HCV 疫苗变得极具挑战性。在这项工作中，我们利用免疫信息学方法开发了一种基于多表位的疫苗，以有效治疗病毒性 HCV 多蛋白。该疫苗由从 HCV 基因型 1a 和 1b 的病毒多聚蛋白中提取的 T 细胞表位构建而成。该疫苗具有高抗原性、无毒性和无过敏性。通过与人体免疫 Toll-Like 受体（TLR3 和 TLR8）形成复合物，研究了所设计疫苗构建体的有效结合。对这些受体-疫苗复合物进行了 50ns 的 MD 模拟，并对模型疫苗在受体存在下进行了 365 天的免疫学模拟，验证了所构建疫苗的稳定性。如果在体内和体外方法中进行进一步探索，这项工作中开发出的硅内疫苗构建物可能有利于作为针对 HCV 变体的预防措施。因此，这项研究成果被认为对开发更安全、更有效的致命疾病疫苗具有重要意义：在线版本包含补充材料，可查阅 10.1007/s40203-024-00275-4。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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In silico pharmacology

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