首页> 外文期刊>Hepatology: Official Journal of the American Association for the Study of Liver Diseases >Hepatitis C virus JFH-1 strain infection in chimpanzees is associated with low pathogenicity and emergence of an adaptive mutation.
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Hepatitis C virus JFH-1 strain infection in chimpanzees is associated with low pathogenicity and emergence of an adaptive mutation.

机译:黑猩猩中的丙型肝炎病毒JFH-1株感染与低致病性和适应性突变的出现有关。

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The identification of the hepatitis C virus (HCV) strain JFH-1 enabled the successful development of infectious cell culture systems. Although this strain replicates efficiently and produces infectious virus in cell culture, the replication capacity and pathogenesis in vivo are still undefined. To assess the in vivo phenotype of the JFH-1 virus, cell culture-generated JFH-1 virus (JFH-1cc) and patient serum from which JFH-1 was isolated were inoculated into chimpanzees. Both animals became HCV RNA-positive 3 days after inoculation but showed low-level viremia and no evidence of hepatitis. HCV viremia persisted 8 and 34 weeks in JFH-1cc and patient serum-infected chimpanzees, respectively. Immunological analysis revealed that HCV-specific immune responses were similarly induced in both animals. Sequencing of HCV at various times of infection indicated more substitutions in the patient serum-inoculated chimpanzee, and the higher level of sequence variations seemed to be associated with a prolonged infection in this animal. A common mutation G838R in the NS2 region emerged early in both chimpanzees. This mutation enhances viral assembly, leading to an increase in viral production in transfected or infected cells. CONCLUSION: Our study shows that the HCV JFH-1 strain causes attenuated infection and low pathogenicity in chimpanzees and is capable of adapting in vivo with a unique mutation conferring an enhanced replicative phenotype.
机译:丙型肝炎病毒(HCV)菌株JFH-1的鉴定使感染性细胞培养系统得以成功开发。尽管该菌株有效地复制并在细胞培养物中产生感染性病毒,但体内的复制能力和发病机理仍然不确定。为了评估JFH-1病毒的体内表型,将细胞培养物产生的JFH-1病毒(JFH-1cc)和从中分离出JFH-1的患者血清接种到黑猩猩中。两只动物在接种3天后均呈HCV RNA阳性,但病毒血症水平较低,无肝炎迹象。在JFH-1cc和患者血清感染的黑猩猩中,HCV病毒血症分别持续8和34周。免疫学分析表明,在两只动物中HCV特异性免疫反应均被类似地诱导。在不同感染时间对HCV进行测序表明,在患者血清接种的黑猩猩中存在更多取代,并且较高水平的序列变异似乎与该动物的长期感染有关。在两个黑猩猩中,NS2区的一个常见突变G838R出现得较早。该突变增强了病毒装配,导致转染或感染的细胞中病毒产量增加。结论:我们的研究表明,HCV JFH-1菌株在黑猩猩中引起减弱的感染和低致病性,并且能够在体内适应具有赋予增强复制表型的独特突变。

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