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Two potential recombinant rabies vaccines expressing canine parvovirus virion protein 2 induce immunogenicity to canine parvovirus and rabies virus

机译:表达犬细小病毒毒粒蛋白2的两种潜在重组狂犬病疫苗可诱导对犬细小病毒和狂犬病病毒的免疫原性

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Both rabies virus (RABV) and canine parvovirus (CPV) cause lethal diseases in dogs. In this study, both high egg passage Flury (HEP-Flury) strains of RABV and recombinant RABV carrying double RABV glycoprotein (G) gene were used to express the CPV virion protein 2 (VP2) gene, and were designated rHEP-VP2 and, rHEP-dG-VP2 respectively. The two recombinant RABVs maintained optimal virus titration according to their viral growth kinetics assay compared with the parental strain HEP-Flury. Western blotting indicated that G protein and VP2 were expressed in vitro. The expression of VP2 in Crandell feline kidney cells post-infection by rHEP-VP2 and rHEP-dG-VP2 was confirmed by indirect immunofluorescence assay with antibody against VP2. Immunogenicity of recombinant rabies viruses was tested in Kunming mice. Both rHEP-VP2 and rHEP-dG-VP2 induced high levels of rabies antibody compared with HEP-Flury. Mice immunized with rHEP-VP2 and rHEP-dG-VP2 both had a high level of antibodies against VP2, which can protect against CPV infection. A challenge experiment indicated that more than 80% mice immunized with recombinant RABVs survived after infection of challenge virus standard 24 (CVS-24). Together, this study showed that recombinant RABVs expressing VP2 induced protective immune responses to RABV and CPV. Therefore, rHEP-VP2 and rHEP-dG-VP2 might be potential combined vaccines for RABV and CPV. (C) 2016 Elsevier Ltd. All rights reserved.
机译:狂犬病病毒(RABV)和犬细小病毒(CPV)均引起犬的致死性疾病。在这项研究中,RABV的高卵传代Flury(HEP-Flury)菌株和带有双RABV糖蛋白(G)基因的重组RABV均用于表达CPV病毒体蛋白2(VP2)基因,并命名为rHEP-VP2,并且rHEP-dG-VP2分别。与亲本菌株HEP-Flury相比,这两种重组RABV根据其病毒生长动力学测定可保持最佳病毒滴定度。 Western印迹表明G蛋白和VP2在体外表达。通过针对VP2的抗体的间接免疫荧光分析证实了rHEP-VP2和rHEP-dG-VP2感染后Crandell猫肾细胞中VP2的表达。在昆明小鼠中测试了重组狂犬病毒的免疫原性。与HEP-Flury相比,rHEP-VP2和rHEP-dG-VP2都诱导高水平的狂犬病抗体。用rHEP-VP2和rHEP-dG-VP2免疫的小鼠均具有高水平的抗VP2抗体,可以预防CPV感染。攻击实验表明,感染重组标准病毒24(CVS-24)后,超过80%的用重组RABV免疫的小鼠存活下来。总之,这项研究表明表达VP2的重组RABV诱导了对RABV和CPV的保护性免疫应答。因此,rHEP-VP2和rHEP-dG-VP2可能是RABV和CPV的潜在联合疫苗。 (C)2016 Elsevier Ltd.保留所有权利。

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