期刊论文详细信息
Journal of Veterinary Medical Science
A Fusion Protein of IgG Fc and Mouse-Derived Antigen on the Surface of Pseudorabies Virus Particles Does Not Accelerate Production of Harmful Auto-Reactive Antibodies
Haruko OTA1  Yasunobu MATSUMOTO1  Yoshihiro HAYASHI1  Yasuhiro TAKASHIMA2 
[1] Department of Global Agricultural Science, Graduate School of Agricultural and Life Sciences, the University of Tokyo;Department of Veterinary Parasitological Diseases, Faculty of Applied Biological Sciences, Gifu University
关键词: chimeric IgG1 Fc;    Fc;    PRV;   
DOI  :  10.1292/jvms.68.1179
学科分类:兽医学
来源: Japanese Society of Veterinary Science
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【 摘 要 】

References(11)Cited-By(1)Previously we reported that immunization with pseudorabies virus (PRV), harboring chimeric Fc on the surface of the virus particles (PRV/Fc), induced higher immune responses than normal PRV particles. The chimeric Fc was fused with mouse transferrin receptor of transmembrane domain (mTR) and the Fc region of immunoglobulin G1. Since it has been reported that some chimeric protein of Fc and self-antigen induce auto-reactive antibodies, in this present study, we examined whether PRV/Fc induces auto-reactive antibodies that react with mTR. PRV/Fc immunized mice produced higher levels of anti-PRV antibodies and antibodies that reacted with mouse-derived 3T3/A31 cells (A31 cell), compared to normal PRV immunized mice. However, antibodies that reacted with mTR in A31 cells were not detected in both Western blot analyses and indirect immunofluorescence assay. The antibodies reacted with an antigen of approximately 16 kDa in A31 cells, but this antigen has a different molecular mass from that of mTR. The antibody also reacted with the antigen of approximately 16 kDa in RK13 cells in which the virus had been propagated. In addition, antibodies induced by immunization with normal PRV also reacted with the same antigen in A31 and RK13 cells. Moreover, neither kidney disorders, in which high levels of mTR were expressed, nor clinical symptoms of autoimmune diseases were observed in mice immunized with either PRV or PRV/Fc. These results indicated that the antibodies were not induced by mTR-Fc, but were instead induced by trace amounts of RK13 derived antigens contained in PRV or PRV/Fc preparations, and cross-reacted with equivalent molecules in mouse derived A31 cells. Therefore, this study confirmed that immunization with PRV/Fc did not induce harmful auto-reactive antibodies.

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