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反式激活 miRNA 反应揭示 poly(A) 在翻译抑制中的新作用。

Activation of a microRNA response in trans reveals a new role for poly(A) in translational repression.

机构信息

Ecole Normale Supérieure de Lyon, Unité de Virologie Humaine, IFR 128, Lyon, F-69364 France.

出版信息

Nucleic Acids Res. 2011 Jul;39(12):5215-31. doi: 10.1093/nar/gkr086. Epub 2011 Mar 8.

Abstract

Here, we report that the untreated rabbit reticulocyte lysate contains over 300 different endogenous microRNAs together with the major components of the RNA-induced silencing complex and thus can be used as a model in vitro system to study the effects of microRNAs on gene expression. By using this system, we were able to show that microRNA hybridization to its target resulted in a very rapid and strong inhibition of expression that was exerted exclusively at the level of translation initiation with no involvement of transcript degradation or deadenylation. Moreover, we demonstrate that the magnitude of microRNA-induced repression can only be recapitulated in the context of a competitive translating environment. By using a wide spectrum of competitor cellular and viral RNAs, we could further show that competition was not exerted at the level of general components of the translational machinery, but relied exclusively on the presence of the poly(A) tail with virtually no involvement of the cap structure.

摘要

在这里,我们报告说,未经处理的兔网织红细胞裂解物中含有 300 多种不同的内源性 microRNAs,以及 RNA 诱导沉默复合物的主要成分,因此可以作为体外模型系统来研究 microRNAs 对基因表达的影响。通过使用该系统,我们能够证明 microRNA 与其靶标杂交会导致表达的快速且强烈抑制,这种抑制仅发生在翻译起始水平,而不涉及转录降解或去腺苷酸化。此外,我们证明,microRNA 诱导的抑制程度只能在竞争性翻译环境中重现。通过使用广泛的竞争性细胞和病毒 RNA,我们还可以进一步表明,竞争不是在翻译机制的一般成分水平上发挥作用,而是完全依赖于 poly(A)尾巴的存在,几乎不涉及帽结构。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2b44/3130266/e612221e7345/gkr086f1.jpg

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