首页> 外文OA文献 >Potential use of a recombinant replication-defective adenovirus vector carrying the C-terminal portion of the P97 adhesin protein as a vaccine against Mycoplasma hyopneumoniae in swine.
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Potential use of a recombinant replication-defective adenovirus vector carrying the C-terminal portion of the P97 adhesin protein as a vaccine against Mycoplasma hyopneumoniae in swine.

机译:带有P97粘附素蛋白C端部分的重组复制缺陷型腺病毒载体作为猪猪肺炎支原体疫苗的潜在用途。

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摘要

Mycoplasma hyopneumoniae causes severe economic losses to the swine industry worldwide and the prevention of its related disease, enzootic porcine pneumonia, remains a challenge. The P97 adhesin protein of M. hyopneumoniae should be a good candidate for the development of a subunit vaccine because antibodies produced against P97 could prevent the adhesion of the pathogen to the respiratory epithelial cells in vitro. In the present study, a P97 recombinant replication-defective adenovirus (rAdP97c) subunit vaccine efficiency was evaluated in pigs. The rAdP97c vaccine was found to induce both strong P97 specific humoral and cellular immune responses. The rAdP97c vaccinated pigs developed a lower amount of macroscopic lung lesions (18.5 ± 9.6%) compared to the unvaccinated and challenged animals (45.8 ± 11.5%). rAdP97c vaccine reduced significantly the severity of inflammatory response and the amount of M. hyopneumoniae in the respiratory tract. Furthermore, the average daily weight gain was slightly improved in the rAdP97c vaccinated pigs (0.672 ± 0.068 kg/day) compared to the unvaccinated and challenged animals (0.568 ± 0.104 kg/day). A bacterin-based commercial vaccine (Suvaxyn® MH-one) was more efficient to induce a protective immune response than rAdP97c even if it did not evoke a P97 specific immune response. These results suggest that immunodominant antigens other than P97 adhesin are also important in the induction of a protective immune response and should be taken into account in the future development of M. hyopneumoniae subunit vaccines.
机译:猪肺炎支原体对全世界的养猪业造成了严重的经济损失,如何预防其相关疾病,即猪源性肺炎,仍然是一项挑战。猪肺炎支原体的P97粘附素蛋白应该是开发亚单位疫苗的良好候选者,因为针对P97产生的抗体可以在体外阻止病原体粘附于呼吸道上皮细胞。在本研究中,评估了P97重组复制缺陷型腺病毒(rAdP97c)亚基疫苗的效率。发现rAdP97c疫苗可诱导强烈的P97特异性体液和细胞免疫反应。与未接种疫苗和感染的动物(45.8±11.5%)相比,接种rAdP97c的猪出现的宏观肺损伤数量较少(18.5±9.6%)。 rAdP97c疫苗可显着降低炎症反应的严重程度和呼吸道猪肺炎支原体的数量。此外,与未接种疫苗和感染的动物(0.568±0.104 kg /天)相比,接种rAdP97c的猪的平均日增重略有改善(0.672±0.068 kg /天)。基于细菌的商业疫苗(Suvaxyn®MH-one)比rAdP97c更有效地诱导保护性免疫反应,即使它不引起P97特异性免疫反应。这些结果表明,除P97粘附素以外的其他免疫优势抗原在诱导保护性免疫应答中也很重要,在今后的猪肺炎支原体亚单位疫苗开发中应予以考虑。

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