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基于表位的多价和多病原体疫苗蓝图:针对登革热和寨卡病毒。

Blueprint of epitope-based multivalent and multipathogenic vaccines: targeted against the dengue and zika viruses.

机构信息

Department of Biotechnology and Genetic Engineering, Faculty of Biological Sciences, Jahangirnagar University, Dhaka, Bangladesh.

Department of Genetic Engineering and Biotechnology, School of Life Sciences, Shahjalal University of Science and Technology, Sylhet, Bangladesh.

出版信息

J Biomol Struct Dyn. 2021 Nov;39(18):6882-6902. doi: 10.1080/07391102.2020.1804456. Epub 2020 Aug 8.

DOI:10.1080/07391102.2020.1804456
PMID:32772811
Abstract

Both dengue virus (DENV) and zika virus (ZIKV) belong to the highly infectious family that has already caused several outbreaks and epidemics in many countries. DENV and ZIKV cause two of the most wide spread mosquito-borne viral diseases in the world, dengue fever (DENF) and zika fever (ZIKF), respectively. In many regions around the world, both of these diseases can outbreak together and can be lethal as well as life-threatening. Unfortunately, there is no functional and satisfactory vaccine available to combat these viruses. Therefore, in this study, we have attempted to design a blue print of potential multivalent and multipathogenic vaccines using immunoinformatics approach, which can combat both the DENV and ZIKV infections, simultaneously. Initially, three vaccines were designed; containing highly antigenic, non-allergenic, and non-toxic epitopes of T-cell (100% conserved) and B-cell from all the four DENV serotypes and ZIKV. In total, nine cytotoxic T-lymphocytic (CTL), nine helper T-lymphocytic (HTL), and seven B-cell lymphocytic (BCL) epitopes were used to construct three vaccines using three different adjuvants, designated as 'V1', 'V2', and 'V3'. Later, V3 was found to be the best vaccine construct, determined by molecular docking analysis. Thereafter, several validation studies including molecular dynamics simulation and immune simulation were performed which indicated that V3 might be quite stable and should generate substantial immune response in the biological environment. However, further and validation might be required to finally confirm the safety and efficacy of our suggested vaccine constructs.Communicated by Ramaswamy H. Sarma.

摘要

登革热病毒(DENV)和寨卡病毒(ZIKV)都属于高度传染性的病毒家族,该家族已经在许多国家引发了多次暴发和流行。DENV 和 ZIKV 分别导致世界上两种最广泛传播的蚊媒病毒性疾病,即登革热(DENF)和寨卡热(ZIKF)。在世界上许多地区,这两种疾病可能同时暴发,并且可能是致命的和危及生命的。不幸的是,目前还没有功能和令人满意的疫苗来对抗这些病毒。因此,在这项研究中,我们试图使用免疫信息学方法设计潜在的多价和多病原体疫苗蓝图,以同时对抗 DENV 和 ZIKV 感染。最初设计了三种疫苗,其中包含来自所有四种 DENV 血清型和 ZIKV 的 T 细胞(100%保守)和 B 细胞的高度抗原性、非变应原性和非毒性表位。总共使用了九个细胞毒性 T 淋巴细胞(CTL)、九个辅助 T 淋巴细胞(HTL)和七个 B 细胞淋巴细胞(BCL)表位,使用三种不同的佐剂构建了三种疫苗,分别命名为“V1”、“V2”和“V3”。后来,通过分子对接分析发现 V3 是最好的疫苗构建体。此后,进行了几项验证研究,包括分子动力学模拟和免疫模拟,表明 V3 可能相当稳定,并且应该在生物环境中产生大量免疫反应。然而,可能需要进一步和临床验证来最终确认我们建议的疫苗构建体的安全性和有效性。由 Ramaswamy H. Sarma 传达。

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