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基于免疫信息学从志贺氏菌属的麦芽糖孔蛋白、铁摄取外膜蛋白A和外膜孔蛋白W中鉴定基于表位的候选疫苗,并进行分子对接确认。

Immunoinformatic identification of the epitope-based vaccine candidates from Maltoporin, FepA and OmpW of Shigella Spp, with molecular docking confirmation.

作者信息

Ullah Hedayet, Mahmud Shahin, Hossain Md Jakir, Islam Md Shaid Bin, Kibria K M Kaderi

机构信息

Department of Biotechnology and Genetic Engineering, Faculty of Life Science, Mawlana Bhashani Science and Technology University, Tangail 1902, Bangladesh.

Department of Biotechnology and Genetic Engineering, Faculty of Life Science, Mawlana Bhashani Science and Technology University, Tangail 1902, Bangladesh.

出版信息

Infect Genet Evol. 2021 Dec;96:105129. doi: 10.1016/j.meegid.2021.105129. Epub 2021 Nov 2.

Abstract

Shigella is a bacterial pathogen that causes shigellosis, fatal bacillary dysentery, responsible for a higher level of mortality worldwide. We adopted a number of computational approaches to predict potential epitope-based vaccine candidates of immunogenic proteins of Shigella spp. We selected three cell surface proteins of the bacterium according to their antigenicity using the VaxiJen server, including, FepA, Maltoporin, and OmpW. The sequence analyses by the IEDB server resulted in three 15-mer peptides of the core epitope, FTAEHTQSV, FLVNQTLTL, and MRAGSATVR from FepA, Maltoporin, and OmpW, respectively, as the most potential epitopes that have an affinity with both cytotoxic and helper T-cells. Moreover, the epitopes showed 73.76%, 99.0%, and 93.07% world population coverage, along with 100% conservancy among the Shigella subspecies. The molecular docking simulation studies were performed to verify the interactions between the peptides and the respective HLAs. Docking analyses showed that the Epitope-MHC complexes had a higher level of global energy score dictating strong binding. We have also predicted B-cell epitopes from the sequences of these three proteins. In vivo study of the proposed epitope might contribute to the development of a functional and efficient vaccine, which might be an effective way to elude dysentery from the world.

摘要

志贺氏菌是一种导致志贺氏菌病(致命性细菌性痢疾)的细菌病原体,在全球造成较高的死亡率。我们采用了多种计算方法来预测志贺氏菌属免疫原性蛋白基于表位的潜在疫苗候选物。我们使用VaxiJen服务器根据其抗原性选择了该细菌的三种细胞表面蛋白,包括FepA、麦芽糖孔蛋白和OmpW。通过IEDB服务器进行的序列分析分别从FepA、麦芽糖孔蛋白和OmpW中得到了三个核心表位的15肽,即FTAEHTQSV、FLVNQTLTL和MRAGSATVR,作为与细胞毒性T细胞和辅助性T细胞都具有亲和力的最具潜力的表位。此外,这些表位在世界人口中的覆盖率分别为73.76%、99.0%和93.07%,并且在志贺氏菌亚种中具有100%的保守性。进行了分子对接模拟研究以验证肽与各自的人类白细胞抗原(HLA)之间的相互作用。对接分析表明,表位 - 主要组织相容性复合体(MHC)复合物具有较高的全局能量得分,表明结合力强。我们还从这三种蛋白质的序列中预测了B细胞表位。对所提出表位的体内研究可能有助于开发一种功能性和高效的疫苗,这可能是在全球范围内避免痢疾的有效方法。

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