Differences in the expression of the hepatitis C virus core+1 open reading frame between a nuclear and a cytoplasmic expression system

被引:10
|
作者
Vassilaki, Niki [1 ]
Kalliampakou, Katerina I. [1 ]
Mavromara, Penelope [1 ]
机构
[1] Hellenic Pasteur Inst, Mol Virol Lab, Athens 11521, Greece
来源
关键词
D O I
10.1099/vir.0.83260-0
中图分类号
Q81 [生物工程学(生物技术)]; Q93 [微生物学];
学科分类号
071005 ; 0836 ; 090102 ; 100705 ;
摘要
The hepatitis C virus (HCV) genome possesses an open reading frame (ORF) overlapping the core gene at + 1 nucleotide (core+ 1 ORF). Initial in vitro studies suggested that the core+ 1 ORF is translated by a ribosomal -2/+1 frameshift mechanism during elongation of the viral polyprotein. Recent studies, however, based on transfection of mammalian cells with reporter constructs have shown that translation of the core + 1 ORF is mediated from internal core + 1 codons. To resolve the apparent discrepancies associated with the mechanism of core+ 1 translation, we examined the expression of the HCV-1 and HCV-1 a (H) core+ 1 ORF in a cytoplasmic transcription system based on Huh-7/T7 cells that constitutively synthesize the T7 RNA polymerase in comparison to that in Huh-7 cells. We showed that the efficiency of both the -2/+ 1 and -1/+2 frameshift events operating at the HCV-1 core coclons 8-11 is significantly enhanced in the Huh-7/T7 cytoplasmic transcription system and is dependent on the presence of the consecutive adenine (A) residues within core codons 8-11. In contrast, internal translation initiation at core+ 1 codons 85/87 occurs in both the nuclear and cytoplasmic transcription systems and is not repressed by the ribosomal frameshifting event. Finally, although core + 1 codons 85/87 is the most efficient site for internal initiation of core + 1 translation, it may not be unique, as additional internal core+ 1 codon(s) appear to drive translation at low levels.
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页码:222 / 231
页数:10
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