Immune responses to the oral administration of recombinant Bacillus subtilis expressing multi-epitopes of foot-and-mouth disease virus and a cholera toxin B subunit |
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Authors: | Hu Bo Li Chang Lu Huijun Zhu Zhanbo Du Shouwen Ye Ming Tan Lei Ren Dayong Han Jiali Kan Shifu Wang Jing Jin Ningyi |
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Affiliation: | a College of Animal Science and Veterinary Medicine, Jilin University, Changchun 130062, China b Genetic Engineering Laboratory of PLA, Academy of Military Medical Sciences of PLA, Changchun 130062, China c College of Animal Science and Veterinary Medicine, HeiLongjiang Bayi Agricultural University, Daqing 163319, China |
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Abstract: | Bacillus subtilis has been engineered successfully to express heterologous antigens for use as a vaccine vehicle that can elicit mucosal and systemic immunity response. In this study, a recombinant B. subtilis expressing the B subunit of cholera toxin (CT-B) and an epitope box constituted with antigen sites from foot-and-mouth disease virus (FMDV) type Asia 1 was constructed and named 1A751/CTB-TEpiAs. Its capability to induce mucosal, humoral, and cellular responses in mice and guinea pigs was evaluated after oral administration with vegetative cells of 1A751/CTB-TEpiAs. In addition, its capability to protect guinea pigs against homologous virus challenge was examined. All animals were given booster vaccination at day 21 after initial inoculation and guinea pigs were challenged 3 weeks after booster vaccination. The control groups were inoculated with a commercial vaccine or administered orally with 1A751/pBC38C or an oral buffer. All animals vaccinated with 1A751/CTB-TEpiAs developed specific anti-FMDV IgA in lung and gut lavage fluid, serum ELISA antibody, neutralizing antibody as well as T lymphocyte proliferation, and IFN-γ secretory responses. Three of the five guinea pigs vaccinated with 1A751/CTB-TEpiAs were protected completely from the viral challenge. The results demonstrate the potential viability of a B. subtilis-based recombinant vaccine for the control and prevention of FMDV infections. |
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Keywords: | Foot-and-mouth disease virus Bacillus subtilis Oral vaccine Immune response |
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