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Emergence and evolution of highly pathogenic porcine epidemic diarrhea virus by natural recombination of a low pathogenic vaccine isolate and a highly pathogenic strain in the spike gene

机译:低致病疫苗分离物天然重组的高致病性猪流行性腹泻病毒的出现与演变及穗基因中的高致病菌菌株

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Outbreaks of a new variant of porcine epidemic diarrhea virus (PEDV) at the end of 2010 have raised interest in the mutation and recombination of PEDV. A PEDV strain (CN/Liaoning25/2018) isolated from a clinical outbreak of piglet diarrhea contained a 49-bp deletion in the ORF3 gene. This deletion is considered a genetic characteristic of low pathogenic attenuated vaccine strains. However, CN/Liaoning25/2018 was highly pathogenic. Complete genome sequencing, identity analysis, phylogenetic tree construction, and recombination analysis showed that this virus was a recombinant strain containing the Spike (S) gene from the highly pathogenic CN/GDZQ/2014 strain and the remaining genomic regions from the low pathogenic vaccine isolate SQ2014. Histopathology and immunohistochemistry results confirmed that this strain was highly pathogenic and indicated that intestinal epithelial cell vacuolation was positively correlated with the intensity and density of PEDV antigens. A new natural recombination model for PEDV was identified. Our results suggest that new highly pathogenic recombinant strains in the field may be generated by recombination between low pathogenic attenuated live PEDV vaccines and pathogenic circulating PEDV strains. Our findings also highlight that the 49-bp deletion of the ORF3 gene in low pathogenic attenuated vaccine strains will no longer be a reliable standard to differentiate the classical vaccine attenuated from the field strains.
机译:2010年底爆发了猪流行病毒性腹泻病毒(PEDV)的新变种​​,对PEDV的突变和重组引起了兴趣。从仔猪腹泻的临床爆发中分离的PEDV菌株(CN / Liaoning25 / 2018)含有49-BP在ORF3基因中的缺失。该缺失被认为是低致病减毒疫苗菌株的遗传特征。然而,CN / Liaoning25 / 2018是高致病性的。完全基因组测序,身份分析,系统发育树结构和重组分析表明,该病毒是含有来自高致病性CN / GDZQ / 2014菌株的峰值菌株的重组菌株和来自低致病性疫苗分离物的剩余基因组区域SQ2014。组织病理学和免疫组织化学结果证实,该菌株是高致病性的,并表明肠上皮细胞真空与PEDV抗原的强度和密度正相关。鉴定了一种新的自然复合模型。我们的研究结果表明,该领域的新的高度致病重组菌株可以通过在低致病性减毒的活性PEDV疫苗和致病性循环PEDV菌株之间的重组产生。我们的研究结果还强调了低致病疫苗菌株中的49-BP缺失ORF3基因将不再是可靠的标准,以区分从现场菌株衰减的经典疫苗。

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