Computer-Aided Multi-Epitope Based Vaccine Design Against Monkeypox Virus Surface Protein A30L: An Immunoinformatics Approach

IF 1.9 4区 生物学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY The Protein Journal Pub Date : 2023-08-24 DOI:10.1007/s10930-023-10150-4
S. V. Ramprasadh, Santhosh Rajakumar, S. Srinivasan, D. Susha, Sameer Sharma, Rajan Chourasiya
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引用次数: 1

Abstract

Monkeypox, a viral zoonotic disease resembling smallpox, has emerged as a significant national epidemic primarily in Africa. Nevertheless, the recent global dissemination of this pathogen has engendered apprehension regarding its capacity to metamorphose into a sweeping pandemic. To effectively combat this menace, a multi-epitope vaccine has been meticulously engineered with the specific aim of targeting the cell envelope protein of Monkeypox virus (MPXV), thereby stimulating a potent immunological response while mitigating untoward effects. This new vaccine uses T-cell and B-cell epitopes from a highly antigenic, non-allergenic, non-toxic, conserved, and non-homologous A30L protein to provide protection against the virus. In order to ascertain the vaccine design with the utmost efficacy, protein–protein docking methodologies were employed to anticipate the intricate interactions with Toll-like receptors (TLR) 2, 3, 4, 6, and 8. This meticulous approach led the researchers to discern an optimal vaccine architecture, bolstered by affirmative prognostications derived from both molecular dynamics (MD) simulations and immune simulations. The current research findings indicate that the peptides ATHAAFEYSK, FFIVVATAAV, and MNSLSIFFV exhibited antigenic properties and were determined to be non-allergenic and non-toxic. Through the utilization of codon optimization and in-silico cloning techniques, our investigation revealed that the prospective vaccine exhibited a remarkable expression level within Escherichia coli. Moreover, upon conducting immune simulations, we observed the induction of a robust immune response characterized by elevated levels of both B-cell and T-cell mediated immunity. Moreover, as the initial prediction with in-silico techniques has yielded promising results these epitope-based vaccines can be recommended to in vitro and in silico studies to validate their immunogenic properties.

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猴痘病毒表面蛋白A30L的计算机辅助多表位疫苗设计:一种免疫信息学方法。
猴痘是一种类似天花的病毒性人畜共患疾病,已成为主要在非洲流行的一种重要的全国性流行病。尽管如此,这种病原体最近在全球的传播引起了人们对其转变为全面流行病的能力的担忧。为了有效对抗这一威胁,我们精心设计了一种多表位疫苗,其特定目的是靶向猴痘病毒(MPXV)的细胞包膜蛋白,从而刺激强大的免疫反应,同时减轻不良反应。这种新疫苗使用来自高度抗原性、非致敏性、无毒、保守和非同源A30L蛋白的T细胞和B细胞表位来提供对病毒的保护。为了确定具有最大效力的疫苗设计,采用蛋白质-蛋白质对接方法来预测与Toll样受体(TLR)2、3、4、6和8的复杂相互作用。这种细致的方法使研究人员在分子动力学(MD)模拟和免疫模拟的肯定预测的支持下,发现了最佳的疫苗结构。目前的研究结果表明,肽ATHAAFEYSK、FFIVATAAV和MNSLSIFFV表现出抗原特性,并被确定为非致敏性和无毒性。通过利用密码子优化和计算机克隆技术,我们的研究表明,该疫苗在大肠杆菌中表现出显著的表达水平。此外,在进行免疫模拟时,我们观察到了以B细胞和T细胞介导的免疫水平升高为特征的强大免疫反应的诱导。此外,由于计算机技术的初步预测已经产生了有希望的结果,这些基于表位的疫苗可以推荐用于体外和计算机研究,以验证其免疫原性。
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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来源期刊
The Protein Journal
The Protein Journal 生物-生化与分子生物学
CiteScore
5.20
自引率
0.00%
发文量
57
审稿时长
12 months
期刊介绍: The Protein Journal (formerly the Journal of Protein Chemistry) publishes original research work on all aspects of proteins and peptides. These include studies concerned with covalent or three-dimensional structure determination (X-ray, NMR, cryoEM, EPR/ESR, optical methods, etc.), computational aspects of protein structure and function, protein folding and misfolding, assembly, genetics, evolution, proteomics, molecular biology, protein engineering, protein nanotechnology, protein purification and analysis and peptide synthesis, as well as the elucidation and interpretation of the molecular bases of biological activities of proteins and peptides. We accept original research papers, reviews, mini-reviews, hypotheses, opinion papers, and letters to the editor.
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