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Mutations that permit efficient replication of hepatitis C virus RNA in Huh-7 cells prevent productive replication in chimpanzees

机译:允许丙型肝炎病毒RNA在Huh-7细胞中有效复制的突变阻止了黑猩猩中的有效复制

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摘要

The development of a subgenomic replicon derived from the hepatitis C virus (HCV) strain Con1 enabled the study of viral RNA replication in Huh-7 cells. The level of replication of replicons, as well as full-length Con1 genomes, increased significantly by a combination of two adaptive mutations in NS3 (E1202G and T1280I) and a single mutation in NS5A (S2197P). However, these cell culture-adaptive mutations influenced in vivo infectivity. After intrahepatic transfection of chimpanzees, the wild-type Con1 genome was infectious and produced viral titers similar to those produced by other infectious HCV clones. Repeated independent transfections with RNA transcripts of a Con1 genome containing the three adaptive mutations failed to achieve active HCV infection. Furthermore, although a chimpanzee transfected with RNA transcripts of a Con1 genome with only the NS5A mutation became infected, this mutation was detected only in virus genomes recovered from serum at day 4; viruses recovered at day 7 had a reversion back to the original Con1 sequence. Our study demonstrates that mutations that are adaptive for replication of HCV in cell culture may be highly attenuating in vivo.
机译:衍生自丙型肝炎病毒(HCV)菌株Con1的亚基因组复制子的开发使得能够研究Huh-7细胞中病毒RNA的复制。通过结合NS3中的两个适应性突变(E1202G和T1280I)和NS5A中的单个突变(S2197P),复制子以及全长Con1基因组的复制水平显着提高。但是,这些细胞培养适应性突变影响体内感染性。在黑猩猩的肝内转染后,野生型Con1基因组具有传染性,并产生与其他传染性HCV克隆相似的病毒滴度。用含有三个适应性突变的Con1基因组的RNA转录本重复独立转染未能实现主动HCV感染。此外,尽管只用NS1A突变的Con1基因组的RNA转录物转染的黑猩猩被感染,但仅在第4天从血清中回收的病毒基因组中检测到该突变。在第7天恢复的病毒恢复了原始的Con1序列。我们的研究表明,适应HCV在细胞培养物中复制的突变可能在体内高度减毒。

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