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Vaccinia virus as a vaccine delivery system for marsupial wildlife

机译:牛痘病毒作为有袋野生动物的疫苗输送系统

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Vaccines based on recombinant poxviruses have proved successful in controlling diseases such as rabies and plague in wild eutherian mammals. They have also been trialled experimentally as delivery agents for fertility-control vaccines in rodents and foxes. In some countries, marsupial mammals represent a wildlife disease reservoir or a threat to conservation values but, as yet there has been no bespoke study of efficacy or immunogenicity of a poxvirus-based vaccine delivery system in a marsupial. Here, we report a study of the potential for vaccination using vaccinia virus in the Australian brushtail possum Trichosurus vulpecula, an introduced pest species in New Zealand. Parent-strain vaccinia virus (Lister) infected 8/8 possums following delivery of virus to the oral cavity and outer nares surfaces (oronasal immunisation), and persisted in the mucosal epithelium around the palatine tonsils for up to 2 weeks post-exposure. A recombinant vaccinia virus construct (VV399, which expresses the Eg95 antigen of the hydatid disease parasite Echinococcus granulosus) was shown to infect 10/15 possums after a single-dose oronasal delivery and to also persist. Both parent vaccinia virus and the VV399 construct virus induced peripheral blood lymphocyte reactivity against viral antigens in possums, first apparent at 4 weeks post-exposure and still detectable at 4 months post-exposure. Serum antibody reactivity to Eg95 was recorded in 7/8 possums which received a single dose of the VV399 construct and 7/7 animals which received triple-dose delivery, with titre end-points in the latter case exceeding 1/4000 dilution. This study demonstrates that vaccinia virus will readily infect possums via a delivery means used to deploy wildlife vaccines, and in doing is capable of generating immune reactivity against viral and heterologous antigens. This highlights the future potential of recombinant vaccinia virus as a vaccine delivery system in marsupial wildlife
机译:事实证明,基于重组痘病毒的疫苗已成功控制了狂犬病哺乳动物中的狂犬病和鼠疫等疾病。它们也已经作为啮齿动物和狐狸的生育控制疫苗的传递剂进行了试验性试验。在一些国家,有袋类哺乳动物是野生动物疾病库或对保护价值的威胁,但迄今为止,尚未对基于痘病毒的疫苗输送系统在有袋动物中的功效或免疫原性进行专门研究。在这里,我们报告了一项关于使用牛痘病毒在新西兰引入的有害生物澳大利亚假尾负鼠Trichosurus vulpecula中进行疫苗接种潜力的研究。亲本株痘苗病毒(李斯特菌)在病毒递送至口腔和外鼻孔表面(口鼻免疫)后感染了8/8个负鼠,并在暴露后2周内在in扁桃体周围的粘膜上皮中持续存在。重组牛痘病毒构建体(VV399,表达包虫病寄生虫棘球E虫的Eg95抗原)已显示在单剂量口鼻递送后感染了10/15负鼠,并持续存在。亲本痘苗病毒和VV399构建病毒均诱导负鼠负鼠抗病毒抗原的外周血淋巴细胞反应,首次在暴露后4周出现,但在暴露后4个月仍可检测到。在接受单剂​​量VV399构建体的7/8只负鼠和接受三剂量递送的7/7只动物中记录了对Eg95的血清抗体反应性,在后者的情况下滴定终点超过了1/4000稀释度。这项研究表明,牛痘病毒将很容易通过用于部署野生动植物疫苗的递送方式感染负鼠,并且能够产生针对病毒和异源抗原的免疫反应性。这突出了重组痘苗病毒作为有袋野生动物疫苗递送系统的未来潜力

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