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在持续性感染期间,冠状病毒mRNA上会选择一个翻译减弱的前导区内开放阅读框。

A translation-attenuating intraleader open reading frame is selected on coronavirus mRNAs during persistent infection.

作者信息

Hofmann M A, Senanayake S D, Brian D A

机构信息

Department of Microbiology, University of Tennessee, Knoxville 37996-0845.

出版信息

Proc Natl Acad Sci U S A. 1993 Dec 15;90(24):11733-7. doi: 10.1073/pnas.90.24.11733.

Abstract

Short open reading frames within the 5' leader of some eukaryotic mRNAs are known to regulate the rate of translation initiation on the downstream open reading frame. By employing the polymerase chain reaction, we learned that the 5'-terminal 5 nt on the common leader sequence of bovine coronavirus subgenomic mRNAs were heterogeneous and hypervariable throughout early infection in cell culture and that as a persistent infection became established, termini giving rise to a common 33-nt intraleader open reading frame were selected. Since the common leader is derived from the genomic 5' end during transcription, a common focus of origin for the heterogeneity is expected. The intraleader open reading frame was shown by in vitro translation studies to attenuate translation of downstream open reading frames in a cloned bovine coronavirus mRNA molecule. Selection of an intraleader open reading frame resulting in a general attenuation of mRNA translation and a consequent attenuation of virus replication may, therefore, be a mechanism by which coronaviruses and possibly other RNA viruses with a similar transcriptional strategy maintain a persistent infection.

摘要

已知一些真核生物mRNA 5'前导序列中的短开放阅读框可调节下游开放阅读框的翻译起始速率。通过聚合酶链反应,我们了解到牛冠状病毒亚基因组mRNA共同前导序列上的5'末端5个核苷酸在细胞培养的早期感染过程中是异质且高度可变的,并且随着持续性感染的建立,产生共同的33个核苷酸的前导区内开放阅读框的末端被选择。由于共同前导序列是在转录过程中从基因组5'末端衍生而来的,因此预期异质性有一个共同的起源焦点。体外翻译研究表明,前导区内开放阅读框可减弱克隆的牛冠状病毒mRNA分子中下游开放阅读框的翻译。因此,选择一个导致mRNA翻译普遍减弱并进而导致病毒复制减弱的前导区内开放阅读框,可能是冠状病毒以及可能具有类似转录策略的其他RNA病毒维持持续性感染的一种机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b998/48058/ac34ce84a0a4/pnas01531-0306-a.jpg

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