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RNA Enhancement by lncRNA Promotes Translation Through Recruitment of ILF3 and EIF4A1 to the Target Mammalian mRNAs

机译:通过LNCRNA的RNA提高通过募集ILF3和EIF4A1至靶哺乳动物MRNA来促进翻译

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摘要

The previously developed technology RNA enhancement (RNAe) is reported to increase specific gene expression at post-transcriptional level via a long noncoding RNA (lncRNA). The mechanism for SINEB2-dependent enhancement of translation remains not well understood. Here we present the result of experiments with the folded states of lncRNA in doubly deionized water obtained by slowcool method. These lncRNA were used in RNA pull-down assay that yielded six lncRNA-binding proteins potentially involved in RNAe. The direct interactions of lncRNA with interleukin enhancer-binding factor 3 (ILF3) and eukaryotic initiation factor 4A-I (eIF4A1) in vivo and in vitro were confirmed in RNA-binding protein affinity experiment and electrophoretic mobility shift assay (EMSA), respectively. These observations could explain RNAe phenomenon through lncRNA-dependent guiding of ILF3 protein, which, in turn, recruits polysomes or the factors for translation initiation, and attracting eIF4A1 proteins accelerating the unwinding of the secondary structure at the 5'-end of mRNA during translation initiation. Therefore, the hypothetical mechanism through which lncRNAs may regulate the translation of a specific mRNA is proposed.
机译:据报道,先前开发的技术RNA增强(RNAE)通过长的非加入RNA(LNCRNA)增加转录后水平的特定基因表达。依赖于翻译的SineB2依赖性增强的机制仍然不太了解。在这里,我们介绍了通过慢池方法获得的双去离子水中的LNCRNA的折叠状态的实验结果。将这些LNCRNA用于RNA下拉测定中,其产生六个LNCRNA结合蛋白,可能涉及RNAE。在RNA结合蛋白亲和力实验和电泳迁移率转变测定(EMSA)中,确认了在体内和体内运动局和体外真核素增强因子3(ILF3)和真核引发因子4a-i(EIF4A1)的直接相互作用。这些观察结果可以通过ILF3蛋白的LNCRNA依赖性引导来解释RNAE现象,其反过来招募多肌质或翻译引发的因素,并吸引EIF4A1蛋白在翻译期间MRNA的5'-末端的次要结构加速次要结构的展开引发。因此,提出了LNCRNA可以调节特异性mRNA的翻译的假设机制。

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