生产高免疫原性和安全的Triton X-100生产的针对福氏志贺氏菌2b血清型的细菌幽灵疫苗。

IF 4.3 3区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
Amany Abdelfattah, Reham Samir, Heba M Amin
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引用次数: 0

摘要

背景:细菌鬼细胞(BGCs)是一种被抽干其遗传成分和细胞质成分的细胞。本工作旨在利用bgc方法开发针对福氏志贺氏菌(S. flexneri) 2b血清型的候选疫苗。首次用Triton X-100 (TX100)孵育12 h制备了(S. flexneri) 2b血清型BGCs疫苗,并与先前使用表面活性剂Tween 80 (TW80)制备的疫苗进行了安全性和免疫原性比较。扫描电镜(SEM)、细胞DNA、蛋白质含量测定和鬼影细胞再培养证实了bgc的成功产生。免疫原性通过小鼠腹腔免疫后感染弗氏单胞菌ATCC 12022进行评估。最后进行组织病理学检查。结果:在未免疫挑战组的粪便样本和均质结肠组织中均可计数到富氏沙门氏菌的活菌落形成单位(CFUs)。免疫小鼠血清中两种制剂(TX100 = 40%, TW80 = 56%)的杀菌活性均显著高于未免疫小鼠(阳性对照)。与阳性对照相比,接种TX100和TW80幽灵疫苗的细菌幽灵疫苗组的IgG水平分别高出4倍和3倍;根据安全性检查试验和组织病理学分析结果,两种细菌幽灵疫苗(BGVs)都是安全有效的。结论:通过比较TX100和TW80制备的BGVs, TX100作为一种新的化学处理剂用于BGC的生产,在与靶细胞的培养时间较短,并且在IP攻击试验中对S. flexneri 2b血清型ATCC 12022具有较强的免疫应答。然而,这种新型疫苗的有效性和总体安全性还需要临床研究来证实。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Production of highly immunogenic and safe Triton X-100 produced bacterial ghost vaccine against Shigella flexneri 2b serotype.

Production of highly immunogenic and safe Triton X-100 produced bacterial ghost vaccine against Shigella flexneri 2b serotype.

Production of highly immunogenic and safe Triton X-100 produced bacterial ghost vaccine against Shigella flexneri 2b serotype.

Production of highly immunogenic and safe Triton X-100 produced bacterial ghost vaccine against Shigella flexneri 2b serotype.

Background: Bacterial ghost cells (BGCs) are cells were drained of their genetic and cytoplasmic components. This work aimed to develop vaccine candidates against the Shigella flexneri (S. flexneri) 2b serotype using the BGCs approach. For the first time, (S. flexneri) 2b serotype BGCs vaccine was prepared by incubation with Triton X-100 (TX100) for only 12 h. Its safety and immunogenicity were compared to another vaccine produced using a previously used surfactant, namely Tween 80 (TW80). Scanning electron microscopy (SEM), cellular DNA, protein contents measurements, and ghost cell re-cultivation were used to confirm the successful generation of the BGCs. Immunogenicity was assessed through mice's intraperitoneal (IP) immunization followed by infection with S. flexneri ATCC 12022. Finally, histopathological examination was carried out.

Results: Viable colony forming units (CFUs) of S. flexneri were counted from stool samples as well as homogenized colon tissues of the non-immunized challenged group. Immunized mice sera showed a significant increase in serum bactericidal activity of both preparations (TX100 = 40% and TW80 = 56%) compared to the non-immunized challenged group (positive control). The IgG levels of the bacterial ghost-vaccinated groups were four and three times greater for the TX100 and TW80 ghost vaccines, respectively, compared to that of the positive control; both bacterial ghost vaccines (BGVs) were safe and effective, according to the results of the safety check tests and histopathological analysis.

Conclusions: When comparing the BGVs prepared using TX100 and TW80 methods, the use of TX100 as a new chemical treating agent for BGC production attained robust results in terms of shorter incubation time with the targeted cells and a strong immune response against S. flexneri 2b serotype ATCC 12022 in the IP challenge test. However, a clinical study is needed to confirm the efficacy and total safety of this novel vaccine.

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来源期刊
Gut Pathogens
Gut Pathogens GASTROENTEROLOGY & HEPATOLOGY-MICROBIOLOGY
CiteScore
7.70
自引率
2.40%
发文量
43
期刊介绍: Gut Pathogens is a fast publishing, inclusive and prominent international journal which recognizes the need for a publishing platform uniquely tailored to reflect the full breadth of research in the biology and medicine of pathogens, commensals and functional microbiota of the gut. The journal publishes basic, clinical and cutting-edge research on all aspects of the above mentioned organisms including probiotic bacteria and yeasts and their products. The scope also covers the related ecology, molecular genetics, physiology and epidemiology of these microbes. The journal actively invites timely reports on the novel aspects of genomics, metagenomics, microbiota profiling and systems biology. Gut Pathogens will also consider, at the discretion of the editors, descriptive studies identifying a new genome sequence of a gut microbe or a series of related microbes (such as those obtained from new hosts, niches, settings, outbreaks and epidemics) and those obtained from single or multiple hosts at one or different time points (chronological evolution).
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