首页> 美国卫生研究院文献>Journal of Virology >In Vivo Study of the HC-TN Strain of Hepatitis C Virus Recovered from a Patient with Fulminant Hepatitis: RNA Transcripts of a Molecular Clone (pHC-TN) Are Infectious in Chimpanzees but Not in Huh7.5 Cells
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In Vivo Study of the HC-TN Strain of Hepatitis C Virus Recovered from a Patient with Fulminant Hepatitis: RNA Transcripts of a Molecular Clone (pHC-TN) Are Infectious in Chimpanzees but Not in Huh7.5 Cells

机译:从暴发性肝炎患者中回收的丙型肝炎病毒HC-TN株的体内研究:分子克隆(pHC-TN)的RNA转录本在黑猩猩中具有感染性但在Huh7.5细胞中却没有。

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摘要

Both viral and host factors are thought to influence the pathogenesis of hepatitis C virus (HCV) infection. We studied strain HC-TN (genotype 1a), which caused fulminant hepatic failure in a patient and, subsequently, severe hepatitis in a chimpanzee (CH1422), to analyze the relationship between disease severity, host immune response, viral evolution, and outcome. A second chimpanzee (CH1581) was infected from CH1422 plasma, and a third chimpanzee (CH1579) was infected from RNA transcripts of a consensus cDNA of HC-TN (pHC-TN). RNA transcripts of pHC-TN did not replicate in Huh7.5 cells, which were recently found to be susceptible to infection with another fulminant HCV strain (JFH1). The courses of viremia were similar in the three animals. However, CH1581 and CH1579 developed a less severe acute hepatitis than CH1422. CH1579 and CH1422 resolved the infection, whereas CH1581 became persistently infected. CH1579 and CH1581, despite their differing outcomes, both developed significant intrahepatic cellular immune responses, but not antibodies to the envelope glycoproteins or neutralizing antibodies, during the acute infection. We analyzed the polyprotein sequences of virus recovered at five and nine time points from CH1579 and CH1581, respectively, during the first year of follow-up. High mutation rates and high proportions of nonsynonymous mutations suggested immune pressure and positive selection in both animals. Changes were not selected until after the initial decrease in virus titers and after the development of immune responses and hepatitis. Subsequently, however, mutations emerged repeatedly in both animals. Overall, our results indicate that disease severity and outcome of acute HCV infection depend primarily on the host response.
机译:病毒和宿主因素都被认为会影响丙型肝炎病毒(HCV)感染的发病机理。我们研究了HC-TN菌株(基因型1a),该菌株导致患者暴发性肝衰竭,随后导致黑猩猩(CH1422)患严重肝炎,以分析疾病严重程度,宿主免疫反应,病毒进化和结果之间的关系。从CH1422血浆感染了第二只黑猩猩(CH1581),从HC-TN(pHC-TN)共有cDNA的RNA转录本感染了第三只黑猩猩(CH1579)。 pHC-TN的RNA转录本无法在Huh7.5细胞中复制,该细胞最近被发现容易感染另一株暴发性HCV株(JFH1)。三只动物的病毒血症过程相似。但是,CH1581和CH1579患上的急性肝炎不如CH1422。 CH1579和CH1422解决了感染,而CH1581却被持续感染。尽管结果不同,CH1579和CH1581在急性感染过程中均产生了明显的肝内细胞免疫应答,但未产生针对包膜糖蛋白的抗体或中和抗体。我们分析了在随访的第一年中分别从CH1579和CH1581在五个和九个时间点回收的病毒的多蛋白序列。高突变率和高比例的非同义突变表明两只动物的免疫压力和阳性选择。直到病毒滴度最初降低,免疫应答和肝炎发生之后才选择变化。然而,随后,在两只动物中反复出现突变。总的来说,我们的结果表明疾病的严重程度和急性HCV感染的结果主要取决于宿主的反应。

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