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Phenotypic and genotypic analyses of an attenuated porcine reproductive and respiratory syndrome virus strain after serial passages in cultured porcine alveolar macrophages

机译:在培养的猪肺泡巨噬细胞中连续传代后的减毒猪繁殖与呼吸综合征病毒株的表型和基因型分析

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摘要

The porcine reproductive and respiratory syndrome virus (PRRSV) is a globally ubiquitous swine viral pathogen that causes major economic losses worldwide. We previously reported an over-attenuated phenotype of cell-adapted PRRSV strain CA-2-P100 in vivo. In the present study, CA-2-P100 was serially propagated in cultured porcine alveolar macrophage (PAM) cells for up to 20 passages to obtain the derivative strain CA-2-MP120. Animal inoculation studies revealed that both CA-2-P100 and CA-2-MP120 had decreased virulence, eliciting weight gains, body temperatures, and histopathologic lesions similar to those in the negative control group. However, compared to CA-2-P100 infection, CA-2-MP120 yielded consistently higher viremia kinetics and enhanced antibody responses in pigs. All pigs inoculated with CA-2-MP120 developed viremia and seroconverted to PRRSV. During 20 passages in PAM cells, CA-2-MP120 acquired 15 amino acid changes that were mostly distributed in nsp2 and minor structural protein-coding regions. Among these changes, 6 mutations represented reversions to the sequences of the reference CA-2 and parental CA-2-P20 strains. These genetic drifts may be hypothetical molecular markers associated with PRRSV macrophage tropism and virulence. Our results indicate that the PAM-passaged CA-2-MP120 strain is a potential candidate for developing a live, attenuated PRRSV vaccine.
机译:猪繁殖与呼吸综合症病毒(PRRSV)是全球范围内普遍存在的猪病毒病原体,在世界范围内造成重大经济损失。我们先前曾报道过体内适应细胞的PRRSV株CA-2-P100的过度减毒表型。在本研究中,CA-2-P100在培养的猪肺泡巨噬细胞(PAM)细胞中连续繁殖达20代,以获得衍生菌株CA-2-MP120。动物接种研究表明,CA-2-P100和CA-2-MP120的毒力均降低,引起体重增加,体温升高和组织病理学损害,与阴性对照组相似。但是,与CA-2-P100感染相比,CA-2-MP120在猪中始终产生更高的病毒血症动力学和增强的抗体反应。接种CA-2-MP120的所有猪均出现病毒血症,并血清转化为PRRSV。在PAM细胞中传代20次后,CA-2-MP120获得了15个氨基酸变化,这些变化主要分布在nsp2和次要结构蛋白编码区域。在这些变化中,有6个突变代表参考CA-2和亲本CA-2-P20菌株的序列回复。这些遗传漂移可能是与PRRSV巨噬细胞嗜性和毒力相关的假设分子标记。我们的结果表明,PAM传代的CA-2-MP120菌株是开发活的减毒PRRSV疫苗的潜在候选者。

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