Tamiris Silva Lopes, Brenda Picoli Gheno, Luiza Dos Santos Miranda, Joana Detofano, Md Anik Ashfaq Khan, André Felipe Streck
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Commercial vaccines are formulated with strains that usually do not match those currently circulating in the field. To address this, the study aimed to investigate CPV-2 variants in Brazil, predict epitopes, and design an in silico vaccine tailored to local variants employing reverse vaccinology. The methodology involved data collection, genetic sequence analysis, and amino acid comparison between field strains and vaccines, followed by the prediction of B and T cell epitope regions. The predicted epitopes were evaluated for antigenicity, allergenicity and toxicity. The final vaccine construct consisted of selected epitopes linked to an adjuvant and optimized for expression in Escherichia coli. Structural predictions confirmed the stability and antigenicity of the vaccine, while molecular docking demonstrated interaction with the canine toll-like receptor 4. Molecular dynamics simulations indicated a stable complex formation. In silico immune simulations demonstrated a progressive immune response post-vaccination, including increased antibody production and T-helper cell activity. The multi-epitope vaccine design targeted prevalent CPV-2 variants in Brazil and potentially other regions globally. 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引用次数: 0
摘要
犬细小病毒(CPV-2)是一种传染性极强的病毒,影响着全世界的犬只,对人类构成了严重威胁。VP2 蛋白是 CPV-2 的主要和高免疫原性结构成分。CPV-2 出现后不久就被称为 CPV-2a、2b 和 2c 的变种所取代,其特征是 VP2 的氨基酸残基 426 发生了变化。在 VP2 中还发现了更多的氨基酸变化,某些变化可作为新变种的特征。在巴西,CPV-2疫情持续爆发,VP2特征各不相同。接种疫苗是预防该病毒的主要措施。然而,变异株的出现给传统疫苗接种方法带来了挑战。商用疫苗所使用的毒株通常与目前在野外流行的毒株不匹配。为解决这一问题,该研究旨在调查巴西的 CPV-2 变异株,预测表位,并利用反向疫苗学设计出适合当地变异株的硅学疫苗。研究方法包括数据收集、基因序列分析、实地菌株与疫苗之间的氨基酸比较,然后预测 B 细胞和 T 细胞表位区。对预测的表位进行抗原性、过敏性和毒性评估。最终的疫苗结构包括与佐剂相连的选定表位,并在大肠杆菌中进行了优化表达。结构预测证实了疫苗的稳定性和抗原性,而分子对接则证明了疫苗与犬收费样受体 4 的相互作用。分子动力学模拟显示了稳定的复合物形成。硅学免疫模拟显示,疫苗接种后会产生渐进的免疫反应,包括抗体生成和 T 辅助细胞活性的增加。多表位疫苗设计针对的是巴西以及可能的全球其他地区流行的 CPV-2 变异株。然而,实验验证对于证实我们的硅学研究结果至关重要。
In silico designing of multi-epitope vaccine against canine parvovirus using reverse vaccinology.
Canine parvovirus (CPV-2) is a highly contagious virus affecting dogs worldwide, posing a significant threat. The VP2 protein stands out as the predominant and highly immunogenic structural component of CPV-2. Soon after its emergence, CPV-2 was replaced by variants known as CPV-2a, 2b and 2c, marked by changes in amino acid residue 426 of VP2. Additional amino acid alterations have been identified within VP2, with certain modifications serving as signatures of emerging variants. In Brazil, CPV-2 outbreaks persist with diverse VP2 profiles. Vaccination is the main preventive measure against the virus. However, the emergence of substitutions presents challenges to conventional vaccine methods. Commercial vaccines are formulated with strains that usually do not match those currently circulating in the field. To address this, the study aimed to investigate CPV-2 variants in Brazil, predict epitopes, and design an in silico vaccine tailored to local variants employing reverse vaccinology. The methodology involved data collection, genetic sequence analysis, and amino acid comparison between field strains and vaccines, followed by the prediction of B and T cell epitope regions. The predicted epitopes were evaluated for antigenicity, allergenicity and toxicity. The final vaccine construct consisted of selected epitopes linked to an adjuvant and optimized for expression in Escherichia coli. Structural predictions confirmed the stability and antigenicity of the vaccine, while molecular docking demonstrated interaction with the canine toll-like receptor 4. Molecular dynamics simulations indicated a stable complex formation. In silico immune simulations demonstrated a progressive immune response post-vaccination, including increased antibody production and T-helper cell activity. The multi-epitope vaccine design targeted prevalent CPV-2 variants in Brazil and potentially other regions globally. However, experimental validation is essential to confirm our in silico findings.
期刊介绍:
The Brazilian Journal of Microbiology is an international peer reviewed journal that covers a wide-range of research on fundamental and applied aspects of microbiology.
The journal considers for publication original research articles, short communications, reviews, and letters to the editor, that may be submitted to the following sections: Biotechnology and Industrial Microbiology, Food Microbiology, Bacterial and Fungal Pathogenesis, Clinical Microbiology, Environmental Microbiology, Veterinary Microbiology, Fungal and Bacterial Physiology, Bacterial, Fungal and Virus Molecular Biology, Education in Microbiology. For more details on each section, please check out the instructions for authors.
The journal is the official publication of the Brazilian Society of Microbiology and currently publishes 4 issues per year.
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