首页> 美国卫生研究院文献>Journal of Virology >Capped RNA Transcripts of Full-Length cDNA Clones of Swine Hepatitis E Virus Are Replication Competent When Transfected into Huh7 Cells and Infectious When Intrahepatically Inoculated into Pigs
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Capped RNA Transcripts of Full-Length cDNA Clones of Swine Hepatitis E Virus Are Replication Competent When Transfected into Huh7 Cells and Infectious When Intrahepatically Inoculated into Pigs

机译:猪戊型肝炎病毒全长cDNA克隆的带帽RNA转录物在转染到Huh7细胞中时具有复制能力而在肝内接种时则具有感染性

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摘要

Swine hepatitis E virus (swine HEV), the first animal strain of HEV to be isolated, is a zoonotic agent. We report here the construction and in vitro and in vivo characterizations of infectious cDNA clones of swine HEV. Eight overlapping fragments spanning the entire genome were amplified by reverse transcription-PCR and assembled into a full-length cDNA clone, clone C, which contained 14 mutations compared to the consensus sequence of swine HEV. RNA transcripts from clone C were not infectious, as determined by intrahepatic inoculation into pigs and by in vitro transfection of Huh7 cells. Multiple site-based site-directed mutagenesis was performed to generate three new cDNA clones (pSHEV-1, pSHEV-2, and pSHEV-3) which differed from each other. The transfection of capped RNA transcripts into human liver Huh7 cells resulted in the synthesis of both ORF2 capsid and ORF3 proteins, indicating that the cDNA clones were replication competent. Each of the three clones resulted in active swine HEV infections after the intrahepatic inoculation of pigs with capped RNA transcripts. The patterns of seroconversion, viremia, and fecal virus shedding for pigs inoculated with RNA transcripts from clones pSHEV-2 and pSHEV-3 were similar to each other and to those for pigs inoculated with wild-type swine HEV, suggesting that the nucleotide differences between these two cDNA clones were not critical for replication. Pigs inoculated with RNA transcripts from clone pSHEV-1, which contained three nonsilent mutations in the ORF2 capsid gene, had a delayed appearance of seroconversion and fecal virus shedding and had undetectable viremia. The availability of these infectious cDNA clones affords us an opportunity to understand the mechanisms of cross-species infection by constructing chimeric human and swine HEVs.
机译:猪戊型肝炎病毒(猪HEV)是第一个被分离出的HEV动物株,是一种人畜共患病原体。我们在此报告猪HEV感染性cDNA克隆的构建以及体外和体内特征。通过逆转录PCR扩增跨越整个基因组的八个重叠片段,并组装成全长cDNA克隆,克隆C,其与猪HEV的共有序列相比包含14个突变。克隆C的RNA转录本无感染性,这是通过肝内接种猪和体外转染Huh7细胞确定的。进行了基于多位点的定点诱变,以生成三个彼此不同的新cDNA克隆(pSHEV-1,pSHEV-2和pSHEV-3)。将带帽RNA转录本转染到人肝Huh7细胞中,导致ORF2衣壳和ORF3蛋白都合成,表明cDNA克隆具有复制能力。在猪肝内接种带帽RNA转录本后,三个克隆中的每一个均导致活跃的猪HEV感染。接种了来自克隆pSHEV-2和pSHEV-3的RNA转录本的猪的血清转换,病毒血症和粪便病毒脱落的模式彼此相似,并且与接种野生型猪HEV的猪相似。这两个cDNA克隆对于复制不是关键的。接种了来自克隆pSHEV-1的RNA转录本的猪,该克隆在ORF2衣壳基因中包含三个非沉默突变,其血清转化和粪便病毒脱落的出现延迟,并且病毒血症不可检测。这些感染性cDNA克隆的可用性为我们提供了通过构建嵌合的人和猪HEV来了解跨物种感染机制的机会。

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