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Eukaryotic Initiation Factor 4G-Poly(A) Binding Protein Interaction Is Required for Poly(A) Tail-Mediated Stimulation of Picornavirus Internal Ribosome Entry Segment-Driven Translation but Not for X-Mediated Stimulation of Hepatitis C Virus Translation

机译：真核生物起始因子4G-Poly（A）结合蛋白相互作用是小核糖核酸病毒内部核糖体进入片段驱动翻译的Poly（A）尾部介导刺激的必需条件但对于丙型肝炎病毒翻译的X介导刺激则不需要

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Efficient translation of most eukaryotic mRNAs results from synergistic cooperation between the 5′ m⁷GpppN cap and the 3′ poly(A) tail. In contrast to such mRNAs, the polyadenylated genomic RNAs of picornaviruses are not capped, and translation is initiated internally, driven by an extensive sequence termed IRES (for internal ribosome entry segment). Here we have used our recently described poly(A)-dependent rabbit reticulocyte lysate cell-free translation system to study the role of mRNA polyadenylation in IRES-driven translation. Polyadenylation significantly stimulated translation driven by representatives of each of the three types of picornaviral IRES (poliovirus, encephalomyocarditis virus, and hepatitis A virus, respectively). This did not result from a poly(A)-dependent alteration of mRNA stability in our in vitro translation system but was very sensitive to salt concentration. Disruption of the eukaryotic initiation factor 4G-poly(A) binding protein (eIF4G-PABP) interaction or cleavage of eIF4G abolished or severely reduced poly(A) tail-mediated stimulation of picornavirus IRES-driven translation. In contrast, translation driven by the flaviviral hepatitis C virus (HCV) IRES was not stimulated by polyadenylation but rather by the authentic viral RNA 3′ end: the highly structured X region. X region-mediated stimulation of HCV IRES activity was not affected by disruption of the eIF4G-PABP interaction. These data demonstrate that the protein-protein interactions required for synergistic cooperativity on capped and polyadenylated cellular mRNAs mediate 3′-end stimulation of picornaviral IRES activity but not HCV IRES activity. Their implications for the picornavirus infectious cycle and for the increasing number of identified cellular IRES-carrying mRNAs are discussed.

机译：5'm ^{7 GpppN cap和3'poly（A）尾部之间的协同协同作用可实现大多数真核mRNA的高效翻译。与此类mRNA相比，小核糖核酸病毒的多腺苷酸化基因组RNA没有加盖，并且在内部被称为IRES（用于内部核糖体进入片段）的广泛序列驱动下开始翻译。在这里，我们已使用我们最近描述的依赖poly（A）的兔网织红细胞溶解产物无细胞翻译系统来研究mRNA聚腺苷酸在IRES驱动的翻译中的作用。聚腺苷酸化显着地刺激了由三种形式的微核病毒IRES（分别为脊髓灰质炎病毒，脑心肌炎病毒和甲型肝炎病毒）的代表驱动的翻译。这不是由我们体外翻译系统中依赖于poly（A）的mRNA稳定性改变引起的，但对盐浓度非常敏感。真核生物起始因子4G-poly（A）结合蛋白（eIF4G-PABP）相互作用的破坏或eIF4G的裂解消除或严重降低了poly（A）尾部介导的微小RNA病毒IRES驱动翻译的刺激。相反，由黄病毒丙型肝炎病毒（HCV）IRES驱动的翻译不是由聚腺苷酸化刺激的，而是由真正的病毒RNA 3'末端刺激的：高度结构化的X区。 X区域介导的HCV IRES活性刺激不受eIF4G-PABP相互作用破坏的影响。这些数据表明，在加帽的和聚腺苷酸化的细胞mRNA上协同协同作用所需的蛋白质相互作用需要介导3'端刺激皮甲病毒IRES活性，而不是HCV IRES活性。讨论了它们对小核糖核酸病毒感染周期和确定的携带细胞IRES的mRNA数量增加的影响。}

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期刊名称 Molecular and Cellular Biology
作者
Yanne M. Michel; Andrew M. Borman; Sylvie Paulous; Katherine M. Kean;
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年(卷),期 2001(21),13
年度 2001
页码 4097–4109
总页数 13
原文格式 PDF
正文语种
中图分类分子生物学;细胞生物学;
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入库时间 2022-08-17 12:23:10

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专利

1. Eukaryotic Initiation Factor 4G-Poly(A) Binding Protein Interaction Is Required for Poly(A) Tail-Mediated Stimulation of Picornavirus Internal Ribosome Entry Segment-Driven Translation but Not for X-Mediated Stimulation of Hepatitis C Virus Translation [J] . Yanne M. Michel, Andrew M. Borman, Sylvie Paulous, Molecular and Cellular Biology . 2001,第13期

机译：真核生物起始因子4G-Poly（A）结合蛋白相互作用是小核糖核酸病毒内部核糖体进入片段驱动翻译的Poly（A）尾部介导的刺激，而不是丙型肝炎病毒翻译的X介导的刺激。
2. Porcine polypyrimidine tract‐binding protein stimulates translation initiation at the internal ribosome entry site of foot‐and‐mouth‐disease virus [J] . Niepmann Michael FEBS Letters . 1996,第1期

机译：猪多嘧啶束结合蛋白刺激口蹄疫病毒内部核糖体进入位点的翻译起始
3. The interaction between human initiation factor eIF3 subunit c and heat-shock protein 90: A necessary factor for translation mediated by the hepatitis C virus internal ribosome entry site [J] . UjinoS., NishitsujiH., SugiyamaR., Virus Research: An International Journal of Molecular and Cellular Virology . 2012,第1期

机译：人类起始因子eIF3亚基c与热激蛋白90之间的相互作用：丙型肝炎病毒内部核糖体进入位点介导的翻译必需因子
4. Identification of a cellular protein required for hepatitis C virus internal ribosome entry site (IRES)-mediated translation [C] . T. PENG, H. TANG, F. WONG-STAAL Falk Symposium . 2004

机译：鉴定丙型肝炎病毒内部核糖体入口部位（IRES）介导的翻译所需的细胞蛋白质
5. Interactions of eukaryotic translation initiation factors and 3' untranslated region of barley yellow dwarf virus mRNA during protein synthesis: A study of equilibrium binding, kinetics and thermodynamics. [D] . Banerjee, Bidisha. 2014

机译：蛋白质合成过程中大麦黄矮病毒mRNA的真核翻译起始因子和3'非翻译区的相互作用：平衡结合，动力学和热力学的研究。
6. Epstein-Barr Virus Protein EB2 Stimulates Translation Initiation of mRNAs through Direct Interactions with both Poly(A)-Binding Protein and Eukaryotic Initiation Factor 4G [O] . Fabrice Mure, Baptiste Panthu, Isabelle Zanella-Cléon, 2018

机译：爱泼斯坦-巴尔病毒蛋白EB2通过与Poly（A）结合蛋白和真核起始因子4G的直接相互作用刺激mRNA的翻译起始
7. Eukaryotic Initiation Factor 4G-Poly(A) Binding Protein Interaction Is Required for Poly(A) Tail-Mediated Stimulation of Picornavirus Internal Ribosome Entry Segment-Driven Translation but Not for X-Mediated Stimulation of Hepatitis C Virus Translation [O] . Michel, Yanne M., Borman, Andrew M., Paulous, Sylvie, 2001

机译：真核生物起始因子4G-Poly（A）结合蛋白相互作用是小核糖核酸病毒内部核糖体进入片段驱动翻译的Poly（A）尾部介导刺激的必需条件，但对于丙型肝炎病毒翻译的X介导刺激则不需要

Eukaryotic Initiation Factor 4G-Poly(A) Binding Protein Interaction Is Required for Poly(A) Tail-Mediated Stimulation of Picornavirus Internal Ribosome Entry Segment-Driven Translation but Not for X-Mediated Stimulation of Hepatitis C Virus Translation

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