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Translation of the first upstream ORF in the hepatitis B virus pregenomic RNA modulates translation at the core and polymerase initiation codons

机译:乙型肝炎病毒前基因组RNA中第一个上游ORF的翻译调节核心和聚合酶起始密码子的翻译

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摘要

The human hepatitis B virus (HBV) has a compact genome encoding four major overlapping coding regions: the core, polymerase, surface and X. The polymerase initiation codon is preceded by the partially overlapping core and four or more upstream initiation codons. There is evidence that several mechanisms are used to enable the synthesis of the polymerase protein, including leaky scanning and ribosome reinitiation. We have examined the first AUG in the pregenomic RNA, it precedes that of the core. It initiates an uncharacterized short upstream open reading frame (uORF), highly conserved in all HBV subtypes, we designated the C0 ORF. This arrangement suggested that expression of the core and polymerase may be affected by this uORF. Initiation at the C0 ORF was confirmed in reporter constructs in transfected cells. The C0 ORF had an inhibitory role in downstream expression from the core initiation site in HepG2 cells and in vitro, but also stimulated reinitiation at the polymerase start when in an optimal context. Our results indicate that the C0 ORF is a determinant in balancing the synthesis of the core and polymerase proteins.
机译:人类乙型肝炎病毒(HBV)具有紧凑的基因组,编码四个主要重叠的编码区:核心,聚合酶,表面和X。聚合酶起始密码子之前是部分重叠的核心和四个或更多上游起始密码子。有证据表明,有几种机制可用于合成聚合酶蛋白,包括泄漏扫描和核糖体重新初始化。我们已经检查了前基因组RNA中的第一个AUG,它先于核心。它启动了一个无特征的短上游开放阅读框(uORF),在所有HBV亚型中高度保守,我们将其称为C0 ORF。这种安排表明核心和聚合酶的表达可能受此uORF的影响。在转染细胞的报告基因构建物中证实了在C0 ORF处的起始。 C0 ORF在HepG2细胞和体外的核心起始位点的下游表达中具有抑制作用,但在最佳情况下,也可在聚合酶开始时刺激重新起始。我们的结果表明,C0 ORF是平衡核心蛋白和聚合酶蛋白合成的决定因素。

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