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Expression of the S glycoprotein of transmissible gastroenteritis virus (TGEV) in transgenic potato and its immunogenicity in mice
2013
Ahn, D.J., KRIBB, Daejeon, Republic of Korea | Youm, J.W., KRIBB, Ochang, Republic of Korea | Kim, S.W., KRIBB, Ochang, Republic of Korea | Yoon, W.K., KRIBB, Daejeon, Republic of Korea | Kim, H.C., KRIBB, Daejeon, Republic of Korea | Hur, T.Y., RDA, Cheonan, Republic of Korea | Joung, Y.H., Chonnam National University, Gwangju, Republic of Korea. | Jeon, J.H., KRIBB, Daejeon, Republic of Korea | Kim, H.S., KRIBB, Daejeon, Republic of Korea
Transgenic plants have been tested as an alternative host for the production and delivery of experimental oral vaccines. Here, we developed transgenic potatoes that express the major antigenic sites A and D of the glycoprotein S from transmissible gastroenteritis coronavirus (TGEV-S0.7) under three expression vector systems. The DNA integration and mRNA expression level of the TGEV-S0.7 gene were confirmed in transgenic plants by PCR and northern blot analysis. Antigen protein expression in transgenic potato was determined by western blot analysis. Enzyme-linked immunosorbent assay results revealed that based on a dilution series of Escherichia coli-derived antigen, the transgenic line P-2 had TGEV-S0.7 protein at levels that were 0.015% of total soluble proteins. We then examined the immunogenicity of potato-derived TGEV-S0.7 antigen in mice. Compared with the wild-type potato treated group and synthetic antigen treated group, mice treated with the potato-derived antigen showed significantly higher levels of immunoglobulin (Ig) G and IgA responses.
Afficher plus [+] Moins [-]Effect of chicken egg yolk antibody on canine parvoviral enteritis in pups
2014
Oh, K.E., Kangwon National University, Chuncheon, Republic of Kroea | Jeoung, S.Y., Gangnam Animal Clinics, Chunchon, Republic of Korea | Kim, B.M., ADBIOTECH Co., Ltd., Chunchon, Republic, of Korea | Jang, S.H., ADBIOTECH Co., Ltd., Chunchon, Republic, of Korea | Lee, N.H., ADBIOTECH Co., Ltd., Chunchon, Republic, of Korea | Cho, Y.J., Kangwon National University, Chuncheon, Republic of Kroea | Kim, D., Kangwon National University, Chuncheon, Republic of Kroea | Choi, J.H., Kangwon National University, Chuncheon, Republic of Kroea | Hahn, T.W., Kangwon National University, Chuncheon, Republic of Kroea
Preventive and therapeutic effects of egg yolk antibody, immunoglobulin Y (IgY), against canine parvovirus (CPV) was evaluated in 25 pups orally challenged with CPV-2a. Oral administration of IgY using powder, paste and coated paste delivery systems was compared. Each type of IgY was administered orally for 17 days from 3 days before challenge. The group of pups administered coated IgY showed mild symptoms such as a moderate decrease in total white blood cell count, no depression, vomiting and diarrhea when compared with other groups. The overall clinical score of the group of pups administered coated IgY was significantly lower than that of the challenge control group. However, mortality did not differ among groups because not all pups received symptomatic treatment. These results implied that oral treatment of coated IgY could improve therapeutic effects against CPV challenge if pups received symptomatic treatment.
Afficher plus [+] Moins [-]Comparative pharmacokinetics of norfloxacin-glycine acetate after single oral administration and medication with drinking water in broilers
Lim, J.H.;Lim, B.Y.;Park, B.K.;Kim, M.S.;Jang, B.S.;Yun, H.I.(Chungnam National University, Daejeon, Republic of Korea)E-mail:hiyun@cnu.ac.kr | Park, S.C.(Kyungpook National University, Daegu, Republic of Korea)
Norfloxacin (NFX) is a fluorquinolone antibacterial agent with a high antimicrobial activity and might have great potential for treating common infections in poultry. The objective of this study was to obtain comparative pharmacokinetic data after a single oral administration and medication with drinking water of norfloxacin-glycine acetate (NFX-GA) at the dose rate of 10 mg/kg bw in broilers. Fifty minutes following oral administration of NFX-GA, serum concentrations peaked at 1.32 ㎍/mL (range 1.03-1.45 ㎍/mL).
Afficher plus [+] Moins [-]Preliminary studies on the effects of orally-administered transforming growth factor-beta on protozoan diseases in mice
2009
Namangala, B.(Obihiro Univ. of Agriculture and Veterinary Medicine, Hokkaido (Japan)) | Inoue, N. | Sugimoto, C.
Transforming growth factor beta-1 (TGF-beta1) is a pleiotropic cytokine with both pro- and antiinflammatory properties, depending on its environment and concentration. The present study evaluated the effects of orally-delivered TGF-beta1 on mice parenterally-infected with various protozoan parasites. We report that while orally-administered TGF-beta1 seems to confer partial protection against murine chronic babesiosis and acute trypanosomosis, no beneficial clinical effects were observed against acute babesiosis, malaria or toxoplasmosis. Taken together, these preliminary data suggest that the systemic effects conferred by exogenous TGF-beta1 could be parasite species-specific. The variations in different parasitic infections could be due to (i) intrinsic differences between parasite species and/or strains in their ability to induce production of immunosuppressive molecules and/or (ii) differences in mechanisms governing host protection against different parasitic infections.
Afficher plus [+] Moins [-]Alymphoplasia mice are resistant to prion infection via oral route
2006
Horiuchi, M.(Hokkaido Univ., Sapporo (Japan)) | Furuoka, H. | Kitamura, N. | Shinagawa, M.
The major cause of infection in animal prion diseases is thought to be consumption of prion-contaminated stuff. There is evidence that the enteric nerve system (ENS) and gut-associated lymphoid tissues (GATL) are involved in the establishment of prion infection through alimentary tract. To elucidate the initial entry port for prion, we inoculated prion to alymphoplasia (aly) mice showing a deficiency in systemic lymph nodes and Peyer's patches. The aly/aly mice were susceptible to prion infection by intra-cranial inoculation and there were no differences in incubation periods between aly/aly mice and wild-type C57BL/6J mice. Incubation periods in aly/aly mice were about 20 days longer than those in C57BL/6J mice with the intra-peritoneal inoculation. The aly/aly mice were completely resistant to prion infection by per os administration, while C57BL/6J mice were sensitive as they entered the terminal stage of disease around 300 days post inoculation. PrPsup(sc) were detected in the intestine and spleen of C57BL/6J mice inoculated with prion intra-peritoneally or orally; however PrPsup(sc) was not detected in the spleen and intestine of aly/aly mice. Prion infectivity was detected in the intestines and spleens of prion-inoculated C57BL/6J mice, even after the early stages of ex-posure, while no infectivity was detected in these tissues of prion-inoculated aly/aly mice. No apparent differences were observed in the organization of the enteric nerve system between wild-type and aly/aly mice. These results indicate that GALT rather than ENS acts as the primary entry port for prion after oral exposure.
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