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首页> 外文期刊>BMC Veterinary Research >Trypsin-independent porcine epidemic diarrhea virus US strain with altered virus entry mechanism
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Trypsin-independent porcine epidemic diarrhea virus US strain with altered virus entry mechanism

机译:不依赖胰蛋白酶的猪流行性腹泻病毒US菌株,其病毒进入机制已改变

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Porcine Epidemic Diarrhea Virus (PEDV) is a coronavirus that infects the intestinal tract and causes diarrhea and vomiting in older pigs or extreme dehydration and death that could reach 100% mortality in neonatal piglets. In the US, the first PEDV outbreaks occurred in 2013 and since then US PEDV strains have quickly spread throughout the US and worldwide, causing significant economic and public health concerns. Currently two conditionally approved vaccines exist in the US, but there is no live attenuated vaccine, which is considered the best option in controlling PEDV by inducing transferrable mucosal immunity to susceptible neonatal piglets. In this study, we passaged an US PEDV isolate under various conditions to generate three strains and characterized their growth and antigenicity in cell culture using various assays including Western blot analysis, serum neutralization assay, sequencing analysis and confocal microscopy. Finally, these strains were evaluated for pathogenicity in nursing piglets (1–4?days old). One of the PEDV strains generated in this study (designated as PEDV 8aa) is able to replicate in cells without any protease and grows to a high titer of >8 log10 TCID50/ml in cell culture. Interestingly, replication of PEDV 8aa was severely reduced by trypsin and this correlated with the inhibition of virus attachment and entry into the cells. In neonatal nursing piglets, PEDV 8aa (passage number 70 or 105) was found to be fully attenuated with limited virus shedding. These results suggest that applying selective pressure during viral passages can facilitate attainment of viral attenuation and that PEDV 8aa warrants further investigation as an attenuated vaccine.
机译:猪流行性腹泻病毒(PEDV)是一种冠状病毒,可感染肠道并导致年纪较大的猪出现腹泻和呕吐,或极度脱水和死亡,新生仔猪的死亡率可达到100%。在美国,2013年首次爆发PEDV,此后,美国的PEDV毒株迅速在美国和全球传播,引起了重大的经济和公共卫生问题。目前,美国有两种有条件批准的疫苗,但尚无减毒活疫苗,它被认为是通过诱导易感新生仔猪可转移的粘膜免疫力来控制PEDV的最佳选择。在这项研究中,我们在各种条件下传代了美国PEDV分离株,以产生三种菌株,并使用多种测定方法(包括蛋白质印迹分析,血清中和测定,测序分析和共聚焦显微镜)表征了它们在细胞培养中的生长和抗原性。最后,评估了这些菌株在哺乳仔猪(1-4天大)中的致病性。这项研究中产生的一种PEDV菌株(命名为PEDV 8aa)能够在没有任何蛋白酶的细胞中复制,并在细胞培养中生长至> 8 log10 TCID50 / ml的高滴度。有趣的是,胰蛋白酶严重降低了PEDV 8aa的复制,这与抑制病毒附着和进入细胞有关。在新生的哺乳仔猪中,发现PEDV 8aa(第70或105代)通过有限的病毒脱落被完全减毒。这些结果表明,在病毒传代期间施加选择性压力可以促进病毒减毒的实现,并且PEDV 8aa作为减毒疫苗值得进一步研究。

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