在小鼠模型中研究硅学设计的 FepA 肽疫苗对柔性志贺氏菌的疫苗潜力

IF 2.7 Q3 IMMUNOLOGY
Md. Rayhan Ali , Shahin Mahmud , Md. Omar Faruque , Md. Imam Hossain , Mohammed Akhter Hossain , K.M. Kaderi Kibria
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引用次数: 0

摘要

背景志贺氏杆菌病是孟加拉国腹泻的主要原因之一。这是一个全球性的健康问题,每年约有 130 万人死于志贺氏菌病。目前使用不同抗生素治疗志贺氏杆菌病的方法效果不佳。在本研究中,我们用化学方法合成了 FepA 肽。结果免疫学分析表明,所有接种疫苗的小鼠都得到了免疫增强,与对照小鼠相比,差异有统计学意义(P 值为 0.0325)。细菌中和试验结果的免疫学分析也有统计学意义(P 值为 0.0468)。用 1 × 1012 个 S. flexneri 细胞对接种疫苗的小鼠和对照组小鼠进行的挑战测试表明,37.5% 的对照组(未接种疫苗)小鼠在接受挑战后的七天内死亡,而 100%的接种疫苗的小鼠仍然强壮有力。对小鼠挑战后体重减轻情况的分析也显示,对照组小鼠体重减轻的百分比远高于接种疫苗的小鼠(P 值为 0.0367)。疫苗接种小鼠的病理和表型与对照组小鼠相比也有明显差异。因此,所有这些免疫学分析和病理学表现都直接支持我们的 FepA 肽是一种潜在的免疫增强剂。因此,这些研究结果为今后评估该候选疫苗是否适用于志贺氏菌病的试验提供了启发。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Investigation of the vaccine potential of an in silico designed FepA peptide vaccine against Shigella flexneri in mice model

Background

Shigellosis is one of the significant causes of diarrhea in Bangladesh. It is a global health problem; approximately 1.3 million people die yearly from Shigellosis. The current treatment method, using different antibiotics against Shigellosis is ineffective. Moreover, it becomes a worrying situation due to the emergence of antibiotic-resistant pathogenic microbes responsible for these diarrheal diseases.

Methodology

Previous immunoinformatics study predicted a potential peptide from the Ferric enterobactin protein (FepA) of Shigella spp. In this study, we have chemically synthesized the FepA peptide. As a highly immunogenic, FepA peptide conjugated with KLH has been tested in mice model with complete and incomplete adjuvants as a vaccine candidate.

Results

Immunological analysis showed that all vaccinated mice were immunologically boosted, which was statistically significant (P-value 0.0325) compared to control mice. Immunological analysis for bacterial neutralization test result was also statistically significant (P-value 0.0468), where each ELISA plate was coated with 1 × 107 S. flexneri cells. The Challenge test with 1 × 1012 S. flexneri cells to each vaccinated and controlled mice showed that 37.5 % of control (non-vaccinated) mice died within seven days after the challenge was given while 100 % of vaccinated mice remained strong and stout. The analyses of the post-challenge weight loss of the mice were also significant (P-value 0.0367) as the weight loss percentage in control mice was much higher than in the vaccinated mice. The pathological and phenotypic appearances of vaccinated mice were also clearly differentiable compared with control mice. Thus all these immunological analysis and pathological appearances directly supported our FepA peptide as a potential immune booster.

Conclusion

This study provides evidence that the FepA peptide is a highly immunogenic vaccine candidate against S. flexneri. Therefore, these findings inspire future trials for the evaluation of the suitability of this vaccine candidate against Shigellosis.

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来源期刊
Vaccine: X
Vaccine: X Multiple-
CiteScore
2.80
自引率
2.60%
发文量
102
审稿时长
13 weeks
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