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针对伤寒沙门氏菌的多表位 DnaK 肽疫苗:一种计算机模拟方法。

Multi-epitope DnaK peptide vaccine against S.Typhi: An in silico approach.

机构信息

Defence Institute of Physiology and Allied Sciences, Lucknow Road, Timarpur, Delhi 110054, India.

Institute of Nuclear Medicine and Allied Sciences, Lucknow Road, Timarpur, Delhi 110054, India.

出版信息

Vaccine. 2018 Jun 27;36(28):4014-4022. doi: 10.1016/j.vaccine.2018.05.106. Epub 2018 Jun 1.

DOI:10.1016/j.vaccine.2018.05.106
PMID:29861180
Abstract

Salmonella is one of the key global causes of food and water borne enteric infections, responsible for significant morbidity and mortality worldwide especially in developing countries. Currently available vaccines against typhoid are moderately effective with several side effects and not efficacious against all Salmonella serovars. Due to limitations of these vaccines and emerging threats of multidrug resistance, developing an effective vaccine against these infections has increasingly become a priority. Heat shock proteins (Hsps), being evolutionarily conserved, represent dominant antigens in the host immune response. In continuation of our earlier studies on the development of S. Typhi DnaK and GroEL vaccine candidates, highly efficacious against Salmonella and multiple pathogens, in the present study, we have designed multi-epitope vaccine candidates common to multiple serovars of Salmonella using bioinformatics approach. Implementing various immunoinformatics tools such as IEDB, EpiJen, BCPRED, ElliPro and VaxiJen, led to the identification of many immunogenic B and T cell epitopes. The 3-D structure model of DnaK was generated to predict conformational B-cell epitopes using ElliPro server. Most promising T cell epitopes (29 CTLs, 18 T-helper cells) were selected based on their binding efficiency with commonly occurring MHC alleles. Finally we narrowed down to 5 protective antigenic peptides (PAPs), comprising highly conserved, antigenic and immunogenic B /T cell epitopes, least homologous with human host. These PAPs were predicted to be non-allergenic by allergenicity prediction tools (SORTALLER and AllerHunter). Hence, these immunogenic epitopes can be used for prophylactic or therapeutic usages specifically to defeat antibiotic-resistant Salmonella. These antigens have been reported for the first time and their conserved nature endow them as potential future vaccine candidates against other multiple pathogens as well.

摘要

沙门氏菌是全球引发食源性和水源性肠道感染的主要病原体之一,在世界范围内尤其是在发展中国家造成了大量发病率和死亡率。目前可用的伤寒疫苗具有中等效力,存在多种副作用,并且对所有沙门氏菌血清型均无效。由于这些疫苗存在局限性以及多药耐药性的出现,因此针对这些感染开发有效的疫苗已成为当务之急。热休克蛋白(Hsps)在进化上是保守的,是宿主免疫反应中的主要抗原。在我们之前关于开发 S. Typhi DnaK 和 GroEL 疫苗候选物的研究的基础上,本研究采用生物信息学方法针对多种血清型沙门氏菌设计了共同的多表位疫苗候选物,这些候选物对沙门氏菌和多种病原体均具有高度效力。实施各种免疫信息学工具,例如 IEDB、EpiJen、BCPRED、ElliPro 和 VaxiJen,导致鉴定出许多免疫原性 B 和 T 细胞表位。使用 ElliPro 服务器生成 DnaK 的 3D 结构模型,以预测构象 B 细胞表位。根据与常见 MHC 等位基因的结合效率,选择最有前途的 29 个 CTL 和 18 个 T 辅助细胞 T 细胞表位。最后,我们缩小到 5 个保护性抗原肽(PAPs),包含高度保守、抗原性和免疫原性的 B / T 细胞表位,与人类宿主的同源性最低。这些 PAPs 通过过敏预测工具(SORTALLER 和 AllerHunter)预测为非过敏原。因此,这些免疫原性表位可用于预防或治疗用途,特别是用于对抗抗生素耐药性沙门氏菌。这些抗原是首次报道的,其保守性使它们成为针对其他多种病原体的潜在未来疫苗候选物。

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