免疫原性
肠沙门氏菌
微生物学
生物
沙门氏菌
鞭毛蛋白
免疫
血清型
病毒学
病菌
抗原
脾脏
减毒疫苗
毒力
抗体
肠杆菌科
免疫学
基因
细菌
大肠杆菌
生物化学
遗传学
作者
Xinxin Zhao,Xiaoli Zeng,Qinlong Dai,Yulong Hou,Dekang Zhu,Mingshu Wang,Renyong Jia,Shun Chen,Mafeng Liu,Qiao Yang,Ying Wu,Shaqiu Zhang,Juan Huang,Xumin Ou,Sai Mao,Qun Gao,Ling Zhang,Yunya Liu,Yanling Yu,Anchun Cheng
出处
期刊:Vaccine
[Elsevier]
日期:2020-12-17
卷期号:39 (3): 588-595
被引量:11
标识
DOI:10.1016/j.vaccine.2020.12.002
摘要
Salmonella enterica serovar Typhimurium is a major food-borne pathogen that can cause self-limited gastroenteritis or life-threatening invasive diseases in humans. There is no licensed S. Typhimurium vaccine for humans to date. In this study, we attempted to construct a live attenuated vaccine strain of S. Typhimurium based on three genes, namely, the two global regulator genes fnr and arcA and the flagellin subunit gene fliC. The S. Typhimurium three-gene mutant, named SLT39 (ΔfnrΔarcAΔfliC), exhibited a high level of attenuation with a colonization defect in mouse tissues and approximately 104-fold decreased virulence compared with that of the wild-type strain. To evaluate the immunogenicity and protection efficacy of STL39, mice were inoculated twice with a dose of 107 CFU or 108 CFU at a 28-day interval, and the immunized mice were challenged with a lethal dose of the wild-type S. Typhimurium strain one month post second immunization. Compared with mock immunization, SLT39 immunization with either dose elicited significant serum total IgG, IgG1 and IgG2a and faecal IgA responses against inactivated S. Typhimurium antigens at a comparable level post second immunization, whereas the 108 CFU group induced higher levels of duodenal and caecal IgA than the 107 CFU group. Furthermore, the bacterial loads in mouse tissues, including Peyer's patches, spleen and liver, significantly decreased in the two SLT39 immunization groups compared to those in the control group post challenge. Additionally, all mice in the SLT39 (108 CFU) group and 80% of the mice in the SLT39 (107 CFU) group survived the lethal challenge, suggesting full protection and 80% protection efficacy, respectively. Thus, the S. Typhimurium fnr, arcA and fliC mutant proved to be a potential attenuated live vaccine candidate for prevention of homologous infection.
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