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血清型内SAT2嵌合口蹄疫疫苗可保护牛抵御口蹄疫病毒攻击。

Intra-serotype SAT2 chimeric foot-and-mouth disease vaccine protects cattle against FMDV challenge.

作者信息

Maree Francois F, Nsamba Peninah, Mutowembwa Paidamwoyo, Rotherham Lia S, Esterhuysen Jan, Scott Katherine

机构信息

Transboundary Animal Diseases Programme, Onderstepoort Veterinary Institute, Agricultural Research Council, Private Bag X05, Onderstepoort 0110, South Africa; Department of Microbiology and Plant Pathology, Faculty of Agricultural and Natural Sciences, University of Pretoria, Pretoria 0002, South Africa.

Department of Veterinary Tropical Diseases, Faculty of Veterinary Science University of Pretoria, Private Bag X04, Onderstepoort 0110, South Africa; Makerere University, College of Veterinary Medicine, Animal Resources and Biosecurity, PO Box 7062, Kampala, Uganda.

出版信息

Vaccine. 2015 Jun 9;33(25):2909-16. doi: 10.1016/j.vaccine.2015.04.058. Epub 2015 Apr 27.

Abstract

The genetic diversity of the three Southern African Territories (SAT) types of foot-and-mouth disease virus (FMDV) reflects high antigenic variation, and indications are that vaccines targeting each SAT-specific topotype may be needed. This has serious implications for control of FMD using vaccines as well as the choice of strains to include in regional antigen banks. Here, we investigated an intra-serotype chimeric virus, vSAT2(ZIM14)-SAT2, which was engineered by replacing the surface-exposed capsid-coding region (1B-1D/2A) of a SAT2 genome-length clone, pSAT2, with that of the field isolate, SAT2/ZIM/14/90. The chimeric FMDV produced by this technique was viable, grew to high titres and stably maintained the 1B-1D/2A sequence upon passage. Chemically inactivated, oil adjuvanted vaccines of both the chimeric and parental immunogens were used to vaccinate cattle. The serological response to vaccination showed the production of strong neutralizing antibody titres that correlated with protection against homologous FMDV challenge. We also predicted a good likelihood that cattle vaccinated with an intra-serotype chimeric vaccine would be protected against challenge with viruses that caused recent outbreaks in southern Africa. These results provide support that chimeric vaccines containing the external capsid of field isolates induce protective immune responses in FMD host species similar to the parental vaccine.

摘要

口蹄疫病毒(FMDV)的三种南部非洲领土(SAT)型的遗传多样性反映出高度的抗原变异,这表明可能需要针对每种SAT特异性拓扑型的疫苗。这对于使用疫苗控制口蹄疫以及选择纳入区域抗原库的毒株具有严重影响。在此,我们研究了一种血清型内嵌合病毒,vSAT2(ZIM14)-SAT2,它是通过用田间分离株SAT2/ZIM/14/90的表面暴露衣壳编码区(1B - 1D/2A)替换SAT2基因组长度克隆pSAT2的相应区域而构建的。通过该技术产生的嵌合FMDV具有活性,能生长到高滴度,并且在传代时稳定维持1B - 1D/2A序列。用化学灭活的、油佐剂的嵌合免疫原和亲本免疫原疫苗对牛进行接种。接种疫苗后的血清学反应显示产生了强烈的中和抗体滴度,这与针对同源FMDV攻击的保护作用相关。我们还预测,用血清型内嵌合疫苗接种的牛很可能受到保护,免受在南部非洲近期引发疫情的病毒的攻击。这些结果支持了含有田间分离株外部衣壳的嵌合疫苗在口蹄疫宿主物种中诱导与亲本疫苗相似的保护性免疫反应。

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