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DAP5 associates with eIF2 beta and eIF4AI to promote Internal Ribosome Entry Site driven translation

机译：DAP5与eIF2 beta和eIF4AI相关联以促进内部核糖体进入位点驱动的翻译

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摘要

Initiation is a highly regulated rate-limiting step of mRNA translation. During cap-dependent translation, the cap-binding protein eIF4E recruits themRNA to the ribosome. Specific elements in the 5'UTR of some mRNAs referred to as Internal Ribosome Entry Sites (IRESes) allow direct association of the mRNA with the ribosome without the requirement for eIF4E. Cap-independent initiation permits translation of a subset of cellular and viral mRNAs under conditions wherein cap-dependent translation is inhibited, such as stress, mitosis and viral infection. DAP5 is an eIF4G homolog that has been proposed to regulate both cap-dependent and cap-independent translation. Herein, we demonstrate that DAP5 associates with eIF2 beta and eIF4AI to stimulate IRES-dependent translation of cellular mRNAs. In contrast, DAP5 is dispensable for cap-dependent translation. These findings provide the first mechanistic insights into the function of DAP5 as a selective regulator of cap-independent translation.

机译：起始是mRNA翻译的高度调节的限速步骤。在帽依赖性翻译过程中，帽结合蛋白eIF4E将它们RNA募集到核糖体。某些被称为内部核糖体进入位点（IRESes）的mRNA的5'UTR中的特定元件允许mRNA与核糖体直接缔合，而无需eIF4E。不依赖于帽的起始允许在其中不依赖帽的翻译被抑制的条件下，例如应激，有丝分裂和病毒感染，翻译细胞和病毒mRNA的子集。 DAP5是一种eIF4G同源物，已被提议用于调节依赖于帽的翻译和不依赖于帽的翻译。在这里，我们证明DAP5与eIF2 beta和eIF4AI相关联以刺激IRES依赖性的细胞mRNA翻译。相反，DAP5对于依赖于上限的翻译是必不可少的。这些发现为DAP5作为帽独立性翻译的选择性调节子的功能提供了初步的机械见解。

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《Nucleic Acids Research》 |2015年第7期|共12页
作者
Liberman Noa; Gandin Valentina; Svitkin Yuri V.; David Maya; Virgili Genevieve; Jaramillo Maritza; Holcik Martin; Nagar Bhushan; Kimchi Adi; Sonenberg Nahum;
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1. DAP5 associates with eIF2 beta and eIF4AI to promote Internal Ribosome Entry Site driven translation [J] . Liberman Noa, Gandin Valentina, Svitkin Yuri V., Nucleic Acids Research . 2015,第7期

机译：DAP5与eIF2 beta和eIF4AI相关联以促进内部核糖体进入位点驱动的翻译
2. Identification of elF2Bγ and eIF2γ as cofactors of hepatitis C virus internal ribosome entry site-mediated translation using a functional genomics approach [J] . Martin Kruger, Carmela Beger, Qiang-Xin Li Proceedings of the National Academy of Sciences of the United States of America . 2000,第15期

机译：使用功能基因组学方法鉴定eF2Bγ和eIF2γ作为丙型肝炎病毒内部核糖体进入位点介导的翻译的辅因子
3. Eukaryotic translation initiation factor 4GI and p97 promote cellular internal ribosome entry sequence-driven translation [J] . Hundsdoerfer P, Thoma C, Hentze MW Proceedings of the National Academy of Sciences of the United States of America . 2005,第38期

机译：真核翻译起始因子4GI和p97促进细胞内部核糖体进入序列驱动的翻译
4. Generation of △ TAp73 Proteins by Translation from a Putative Internal Ribosome Entry Site [C] . A. EMRE SAYAN, JEAN-PIERRE ROPERCH, BERNA S. SAYAN, Meeting on Cell Signaling World: Signal Transduction Pathways as Therapeutic Targets . 2007

机译：从假定的内部核糖体进入位点翻译产生△TAp73蛋白。
5. Regulation of p53 translation in response to DNA damage by the p53 internal ribosome entry site and its trans-activating factors, TCP80 and RHA. [D] . Halaby, Marie-jo. 2008

机译：响应p53内部核糖体进入位点及其反式激活因子TCP80和RHA对DNA的损伤，调节p53翻译。
6. DAP5 associates with eIF2β and eIF4AI to promote Internal Ribosome Entry Site driven translation [O] . Noa Liberman, Valentina Gandin, Yuri V. Svitkin, 2015

机译：DAP5与eIF2β和eIF4AI相关联以促进内部核糖体进入位点驱动的翻译
7. DAP5 associates with eIF2β and eIF4AI to promote Internal Ribosome Entry Site driven translation [O] . Noa Liberman, Valentina Gandin, Yuri V. Svitkin, 2015

机译：DAP5与EIF2β和EIF4AI联系，促进内部核糖体入口部位驱动翻译

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