Immunogenicity of recombinantLactobacillus casei-expressing F4 (K88) fimbrial adhesin FaeG in conjunction with a heat-labile enterotoxin A (LTAK63) and heat-labile enterotoxin B (LTB) of enterotoxigenicEscherichia colias an oral adjuvant in mice

产肠毒素大肠杆菌 免疫原性 细菌粘附素 肠毒素 微生物学 耐热肠毒素 大肠杆菌 重组DNA 干酪乳杆菌 生物 化学 抗原 免疫学 细菌 基因 生物化学 遗传学
作者
Mei Yu,Ruomei Qi,Cheng Chen,Jiechao Yin,Shining Ma,Wen Shi,Yuhong Wu,Junwei Ge,Yanping Jiang,Lijie Tang,Yongping Xu,Y. Li
出处
期刊:Journal of Applied Microbiology [Oxford University Press]
卷期号:122 (2): 506-515 被引量:40
标识
DOI:10.1111/jam.13352
摘要

The aims of this study were to develop an effective oral vaccine against enterotoxigenic Escherichia coli (ETEC) infection and to design new and more versatile mucosal adjuvants.Genetically engineered Lactobacillus casei strains expressing F4 (K88) fimbrial adhesin FaeG (rLpPG-2-FaeG) and either co-expressing heat-labile enterotoxin A (LTA) subunit with an amino acid mutation associated with reduced virulence (LTAK63) and a heat-labile enterotoxin B (LTB) subunit of E. coli (rLpPG-2-LTAK63-co-LTB) or fused-expressing LTAK63 and LTB (rLpPG-2-LTAK63-fu-LTB) were constructed. The immunogenicity of rLpPG-2-FaeG in conjunction with rLpPG-2-LTAK63-co-LTB or rLpPG-2-LTAK63-fu-LTB as an orally administered mucosal adjuvant in mice was evaluated. Results showed that the levels of FaeG-specific serum IgG and mucosal sIgA, as well as the proliferation of lymphocytes, were significantly higher in mice orally co-administered rLpPG-2-FaeG and rLpPG-2-LTAK63-fu-LTB compared with those administered rLpPG-2-FaeG alone, and were lower than those co-administered rLpPG-2-FaeG and rLpPG-2-LTAK63-co-LTB. Moreover, effective protection was observed after challenge with F4+ ETEC strain CVCC 230 in mice co-administered rLpPG-2-FaeG and rLpPG-2-LTAK63-co-LTB or rLpPG-2-FaeG and rLpPG-2-LTAK63-fu-LTB group compared with those that received rLpPG-2-FaeG alone.rLpPG-2-FaeG showed greater immunogenicity in combination with LTAK63 and LTB as molecular adjuvants.Recombinant Lactobacillus provides a promising platform for the development of vaccines against F4+ ETEC infection.
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