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新型多表位混合疫苗对抗猴痘病毒的设计与计算评估:大流行防范的潜在靶标和免疫原性评估。

Design and computational evaluation of a novel multi-epitope hybrid vaccine against monkeypox virus: Potential targets and immunogenicity assessment for pandemic preparedness.

机构信息

School of Biological Sciences, Faculty of Life Sciences, University of the Punjab, Lahore, 54590, Pakistan.

School of Biochemistry and Biotechnology, University of the Punjab, Lahore, 54590, Pakistan.

出版信息

Biologicals. 2024 May;86:101770. doi: 10.1016/j.biologicals.2024.101770. Epub 2024 May 14.

DOI:10.1016/j.biologicals.2024.101770
PMID:38749079
Abstract

Monkeypox is a type of DNA-enveloped virus that belongs to the orthopoxvirus family, closely related to the smallpox virus. It can cause an infectious disease in humans known as monkeypox disease. Although there are multiple drugs and vaccines designed to combat orthopoxvirus infections, with a primary focus on smallpox, the recent spread of the monkeypox virus to over 50 countries have ignited a mounting global concern. This unchecked viral proliferation has raised apprehensions about the potential for a pandemic corresponding to the catastrophic impact of COVID-19. This investigation explored the structural proteins of monkeypox virus as potential candidates for designing a novel hybrid multi-epitope vaccine. The epitopes obtained from the selected proteins were screened to ensure their non-allergenicity, non-toxicity, and antigenicity to trigger T and B-cell responses. The interaction of the vaccine with toll-like receptor-3 (TLR-3) and major histocompatibility complexes (MHCs) was assessed using Cluspro 2.0. To establish the reliability of the docked complexes, a comprehensive evaluation was conducted using Immune and MD Simulations and Normal Mode Analysis. However, to validate the computational results of this study, additional in-vitro and in-vivo research is essential.

摘要

猴痘是一种 DNA 包膜病毒,属于正痘病毒科,与天花病毒密切相关。它可导致一种人类传染病,称为猴痘病。虽然有多种针对正痘病毒感染的药物和疫苗,主要针对天花,但最近猴痘病毒在 50 多个国家的传播引起了全球越来越多的关注。这种不受控制的病毒增殖引发了人们对可能出现类似于 COVID-19 灾难性影响的大流行的担忧。本研究探讨了猴痘病毒的结构蛋白作为设计新型混合多表位疫苗的潜在候选物。从选定的蛋白质中筛选出的表位,以确保它们无过敏原性、无毒性和抗原性,以触发 T 和 B 细胞反应。使用 Cluspro 2.0 评估疫苗与 toll 样受体-3(TLR-3)和主要组织相容性复合物(MHCs)的相互作用。为了建立对接复合物的可靠性,使用免疫和 MD 模拟和正常模式分析进行了全面评估。然而,要验证本研究的计算结果,还需要进行额外的体外和体内研究。

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