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首页> 外文期刊>Research in Veterinary Science >Intranasal inoculations of naked or PLGA-PEI nanovectored DNA vaccine induce systemic and mucosal antibodies in pigs: A feasibility study
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Intranasal inoculations of naked or PLGA-PEI nanovectored DNA vaccine induce systemic and mucosal antibodies in pigs: A feasibility study

机译:Naked或PLGA-PEI纳米疫苗疫苗的鼻内接种诱导猪中的全身和粘膜抗体:可行性研究

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Mucosa are the routes of entry of most pathogens into animals' organisms. Reducing the important global burden of mucosal infectious diseases in livestock animals is required in the field of veterinary public health. For veterinary respiratory pathogens, one possible strategy is the development of intranasal (IN) DNA vaccination. The aim of this study was to assess the feasibility of IN DNA vaccination in pigs, an important species in livestock production industry, and a source of zoonotic diseases. To achieve this goal, we used a DNA vaccine against pseudorabies virus (PrV) encoding the immunogenic glycoprotein B (pcDNA3-gB plasmid). When pigs were inoculated with the naked DNA vaccine through the IN route, PrV-specific IgG and IgA type antibodies were detected in porcine sera. Interestingly, mucosal salivary IgA antibodies against PrV were also detected, at similar levels to those measured following intramuscular injection (positive controls). Furthermore, the IN delivery of pcDNA3-gB combined with PLGA-PEI nanoparticles resulted in similar levels of antibodies but was associated with an increase in the duration of detection of mucosal IgA for 2 out of 3 pigs. Our results suggest that there is room to improve the efficacy of IN DNA vaccination in pigs through optimization of IN inoculations, for example by using nanoparticles such as PLGA-PEI. Further studies will be dedicated to optimizing and testing the protective potential of IN DNA vaccination procedures against PrV.
机译:粘膜是大多数病原体进入动物的生物的途径。在兽医公共卫生领域需要减少畜牧动物中的粘膜传染病的重要性。对于兽医呼吸道病原体,一种可能的策略是鼻内(IN)DNA疫苗接种的发展。本研究的目的是评估猪中DNA疫苗接种的可行性,畜牧业生产行业的重要物种,以及动物园疾病。为了实现这一目标,我们使用了对编码免疫原性糖蛋白B(PCDNA3-GB质粒)的伪疫苗的DNA疫苗。当通过在途径中用裸DNA疫苗接种猪时,在猪血清中检测到PRV特异性IgG和IgA型抗体。有趣的是,在肌内注射后(阳性对照)下测量的那些,也检测到对PRV的粘膜唾液IgA抗体。此外,CPDNA3-GB的递送与PLGA-PEI纳米粒子相结合,导致相似的抗体水平,但与3只猪中有2个粘膜IgA的检测持续时间增加相关。我们的研究结果表明,通过在接种中的优化,例如通过使用纳米颗粒如PLGA-PEI,可以提高猪中DNA疫苗接种的疗效。进一步的研究将致力于优化和测试DNA疫苗接种程序对PRV的保护潜力。

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