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DEAD盒RNA解旋酶DDX3与输出信使核糖核蛋白以及顶端相关蛋白相关联,并参与翻译控制。

The DEAD-box RNA helicase DDX3 associates with export messenger ribonucleoproteins as well as tip-associated protein and participates in translational control.

作者信息

Lai Ming-Chih, Lee Yan-Hwa Wu, Tarn Woan-Yuh

机构信息

Institute of Biomedical Sciences, Academia Sinica, Taipei 115, Taiwan.

出版信息

Mol Biol Cell. 2008 Sep;19(9):3847-58. doi: 10.1091/mbc.e07-12-1264. Epub 2008 Jul 2.

Abstract

Nuclear export of mRNA is tightly linked to transcription, nuclear mRNA processing, and subsequent maturation in the cytoplasm. Tip-associated protein (TAP) is the major nuclear mRNA export receptor, and it acts coordinately with various factors involved in mRNA expression. We screened for protein factors that associate with TAP and identified several candidates, including RNA helicase DDX3. We demonstrate that DDX3 directly interacts with TAP and that its association with TAP as well as mRNA ribonucleoprotein complexes may occur in the nucleus. Depletion of TAP resulted in nuclear accumulation of DDX3, suggesting that DDX3 is, at least in part, exported along with messenger ribonucleoproteins to the cytoplasm via the TAP-mediated pathway. Moreover, the observation that DDX3 localizes transiently in cytoplasmic stress granules under cell stress conditions suggests a role for DDX3 in translational control. Indeed, DDX3 associates with translation initiation complexes. However, DDX3 is probably not critical for general mRNA translation but may instead promote efficient translation of mRNAs containing a long or structured 5' untranslated region. Given that the DDX3 RNA helicase activity is essential for its involvement in translation, we suggest that DDX3 facilitates translation by resolving secondary structures of the 5'-untranslated region in mRNAs during ribosome scanning.

摘要

mRNA的核输出与转录、核内mRNA加工以及随后在细胞质中的成熟过程紧密相连。Tip相关蛋白(TAP)是主要的核mRNA输出受体,它与参与mRNA表达的各种因子协同作用。我们筛选了与TAP相互作用的蛋白质因子,并鉴定出了几个候选因子,包括RNA解旋酶DDX3。我们证明DDX3直接与TAP相互作用,并且它与TAP以及mRNA核糖核蛋白复合物的结合可能发生在细胞核中。TAP的缺失导致DDX3在细胞核中积累,这表明DDX3至少部分地通过TAP介导的途径与信使核糖核蛋白一起输出到细胞质中。此外,在细胞应激条件下DDX3短暂定位于细胞质应激颗粒中的观察结果表明DDX3在翻译控制中发挥作用。事实上,DDX3与翻译起始复合物相关联。然而,DDX3可能对一般的mRNA翻译并不关键,而是可能促进含有长的或结构化的5'非翻译区的mRNA的有效翻译。鉴于DDX3的RNA解旋酶活性对其参与翻译至关重要,我们认为DDX3在核糖体扫描过程中通过解开mRNA中5'-非翻译区的二级结构来促进翻译。

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