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New Promising Targets for Synthetic Omptin-Based Peptide Vaccine against Gram-Negative Pathogens

机译:针对革兰氏阴性病原体的基于合成蛋白的肽疫苗的新有希望的目标

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摘要

Omptins represent a family of proteases commonly found in various Gram-negative pathogens. These proteins play an important role in host–pathogen interaction and have been recognized as key virulence factors, highlighting the possibility of developing an omptin-based broad-spectrum vaccine. The prototypical omptin, His-tagged recombinant Pla, was used as a model target antigen. In total, 46 linear and 24 conformational epitopes for the omptin family were predicted by the use of ElliPro service. Among these we selected highly conserved, antigenic, non-allergenic, and immunogenic B-cell epitopes. Five epitopes (2, 6, 8, 10, and 11 corresponding to Pla regions 52–60, 146–150, 231–234, 286–295, and 306–311, respectively) could be the first choice for the development of the new generation of target-peptide-based vaccine against plague. The partial residues of omptin epitopes 6, 8, and 10 (regions 136–145, 227–230, and 274–285) could be promising targets for the multi-pathogen vaccine against a group of enterobacterial infections. The comparative analysis and 3D modeling of amino acid sequences of several omptin family proteases, such as Pla (Yersinia pestis), PgtE (Salmonella enterica), SopA (Shigella flexneri), OmpT, and OmpP (Escherichia coli), confirmed their high cross-homology with respect to the identified epitope clusters and possible involvement of individual epitopes in host–pathogen interaction.
机译:Omptins代表通常在各种革兰氏阴性病原体中发现的蛋白酶家族。这些蛋白质在宿主与病原体的相互作用中起着重要作用,并已被认为是关键的毒力因子,突显了开发基于omptin的广谱疫苗的可能性。原型的omptin,His标记的重组Pla,被用作模型靶抗原。通过使用ElliPro服务,可以预测出针对omptin家族的46个线性和24个构象表位。在这些中,我们选择了高度保守的,抗原性,非过敏性和免疫原性的B细胞表位。五个抗原决定簇(分别对应于Pla区域52-60、146-150、231-234、286-295和306-311的2个,6个,8个,10个和11个)可能是开发该抗原决定簇的首选。新一代针对鼠疫的基于靶标肽的疫苗。 omptin表位6、8和10的部分残基(区域136-145、227-230和274-285)可能是针对一组肠道细菌感染的多病原体疫苗的有希望的靶标。对几种omptin家族蛋白酶(例如瘟疫耶尔森氏菌,PgtE(肠炎沙门氏菌),SopA(志贺氏志贺氏菌),OmpT和OmpP(大肠杆菌))的氨基酸序列进行比较分析和3D建模,证实了它们的高交叉关于已鉴定的表位簇的同源性以及单个表位可能参与宿主与病原体的相互作用。

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