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劳氏肉瘤病毒翻译再探讨:基因组RNA 5' 前导序列中内部核糖体进入片段的特征分析

Rous sarcoma virus translation revisited: characterization of an internal ribosome entry segment in the 5' leader of the genomic RNA.

作者信息

Deffaud C, Darlix J L

机构信息

LaboRétro, Unité de Virologie Humaine, Institut National de la Santé et de la Recherche Médicale, Ecole Normale Supérieure de Lyon, 69364 Lyon Cedex 07, France.

出版信息

J Virol. 2000 Dec;74(24):11581-8. doi: 10.1128/jvi.74.24.11581-11588.2000.

Abstract

The 5' leader of Rous sarcoma virus (RSV) genomic RNA and of retroviruses in general is long and contains stable secondary structures that are critical in the early and late steps of virus replication such as RNA dimerization and packaging and in the process of reverse transcription. The initiation of RSV Gag translation has been reported to be 5' cap dependent and controlled by three short open reading frames located in the 380-nucleotide leader upstream of the Gag start codon. Translation of RSV Gag would thus differ from that prevailing in other retroviruses such as murine leukemia virus, reticuloendotheliosis virus type A, and simian immunodeficiency virus, in which an internal ribosome entry segment (IRES) in the 5' end of the genomic RNA directs efficient Gag expression despite stable 5' secondary structures. This prompted us to investigate whether RSV Gag translation might be controlled by an IRES-dependent mechanism. The results show that the 5' leaders of RSV and v-Src RNA exhibit IRES properties, since these viral elements can promote efficient translation of monocistronic RNAs in conditions inhibiting 5' cap-dependent translation. When inserted between two cistrons in a canonical bicistronic construct, both the RSV and v-Src leaders promote expression of the 3' cistron. A genetic analysis of the RSV leader allowed the identification of two nonoverlapping 5' and 3' leader domains with IRES activity. In addition, the v-Src leader was found to contain unique 3' sequences promoting an efficient reinitiation of translation. Taken together, these data lead us to propose a new model for RSV translation.

摘要

劳氏肉瘤病毒(RSV)基因组RNA以及一般逆转录病毒的5'端前导序列较长,且含有稳定的二级结构,这些结构在病毒复制的早期和晚期步骤中至关重要,如RNA二聚化和包装以及逆转录过程。据报道,RSV Gag的翻译起始依赖于5'帽结构,并受位于Gag起始密码子上游380个核苷酸前导序列中的三个短开放阅读框控制。因此,RSV Gag的翻译与其他逆转录病毒(如鼠白血病病毒、A型网状内皮组织增生症病毒和猿猴免疫缺陷病毒)不同,在这些病毒中,基因组RNA 5'端的内部核糖体进入区段(IRES)尽管存在稳定的5'二级结构,仍能指导高效的Gag表达。这促使我们研究RSV Gag的翻译是否可能受IRES依赖机制的控制。结果表明,RSV和v-Src RNA的5'端前导序列具有IRES特性,因为这些病毒元件在抑制5'帽依赖翻译的条件下能够促进单顺反子RNA的高效翻译。当插入到典型双顺反子构建体的两个顺反子之间时,RSV和v-Src前导序列都能促进3'顺反子的表达。对RSV前导序列的遗传分析确定了两个具有IRES活性的非重叠5'和3'前导结构域。此外,还发现v-Src前导序列包含独特的3'序列,可促进翻译的有效重新起始。综上所述,这些数据使我们提出了一种新的RSV翻译模型。

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