登革热病毒2型多聚表位肽疫苗的免疫信息学设计

Q3 Medicine Vacunas Pub Date : 2023-10-01 DOI:10.1016/j.vacun.2023.04.001
Mohamed Sheik Tharik Abdul Azeeze , Rajaguru Arivuselvam
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引用次数: 0

摘要

登革热病毒感染影响全球约130个国家。根据世卫组织的报告,全球40%的人口生活在农村地区,感染登革热的风险很高。科学家已经确定了登革热病毒的四种远源毒株,一种疫苗并不能永久地控制所有四种远源毒株的出现。因此,需要为这四种毒株中的每一种都接种一种疫苗,以应对目前的情况。本研究的目的是为登革热病毒2株设计一种基于多表位的疫苗,该疫苗可引起强大的免疫反应,同时具有安全性和非过敏性。结果首先分析了包膜蛋白的理化性质和抗原性。接下来,我们高精度地预测MHC I、MHC II和b细胞表位,并评估它们的性质。然后,选用合适的佐剂和连接剂构建疫苗,预测疫苗的二级和三级结构,并对三级结构进行验证。在与toll样受体进行分子对接后,我们利用最佳对接结果进行分子刺激。最后,我们分析了对疫苗的免疫刺激,结果显示巨噬细胞、DC细胞、t细胞和b细胞的免疫反应呈阳性。此外,我们发现疫苗可以从人体排出。结论利用免疫信息学工具和免疫学知识设计基于多表位的登革病毒2株疫苗是可行的。这种方法可以应用于设计其他疾病的疫苗,需要进一步的研究来验证其在体内的有效性。
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Immuno-informatics design of a multimeric epitope peptide-based vaccine against dengue virus serotype-2

Introduction

Dengue viral infection affects approximately 130 countries worldwide. According to WHO reports, 40% of the global population lives in rural areas with a high risk of contracting dengue. Researchers have identified four distant strains of the dengue virus, and a single vaccine has not permanently controlled the emergence of all four distant strains. Therefore, a vaccine is required for each of the four strains to address the current situation.

Objectives

The objective of this study was to design a multi-epitope-based vaccine for the dengue virus-2 strain that elicits a robust immune response while being safe and non-allergenic.

Results

Firstly, we analyzed the envelope protein for its physicochemical and antigenic properties. Next, we predicted MHC I, MHC II, and B-cell epitopes with high accuracy and evaluated their properties. Then, we constructed a vaccine using a suitable adjuvant and linkers, and predicted the secondary and tertiary structure of the vaccine, and the tertiary structure was validated. After conducting molecular docking with toll-like receptors, we utilized the best-docked result for molecular stimulation. Finally, we analyzed the immune stimulation against the vaccine, and the results showed positive immune responses from macrophages, DC cells, T-cells, and B-cells. Additionally, we found that the vaccine was excreted from the human body.

Conclusions

Our study demonstrates the potential of using immunoinformatic tools and immunological knowledge to design a multi-epitope-based vaccine for the dengue virus-2 strain. This approach could be applied to designing vaccines for other diseases, and further studies are required to validate its effectiveness in vivo.

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来源期刊
Vacunas
Vacunas Medicine-Infectious Diseases
CiteScore
3.90
自引率
0.00%
发文量
138
审稿时长
62 days
期刊介绍: Sin duda una de las mejores publicaciones para conocer los avances en el campo de las vacunaciones preventivas, tanto en el ámbito de la investigación básica como aplicada y en la evaluación de programas de vacunaciones. Su alta calidad y utilidad la ha llevado a estar indexada en los prestigiosos índices IME y SCOPUS.
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