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将双链 RNA 的作用扩展到细胞核:重定向选择性剪接。

Expanding the action of duplex RNAs into the nucleus: redirecting alternative splicing.

机构信息

Department of Pharmacology, UT Southwestern Medical Center at Dallas, Dallas, TX 75390-9041, USA.

出版信息

Nucleic Acids Res. 2012 Feb;40(3):1240-50. doi: 10.1093/nar/gkr780. Epub 2011 Sep 23.

Abstract

Double-stranded RNAs are powerful agents for silencing gene expression in the cytoplasm of mammalian cells. The potential for duplex RNAs to control expression in the nucleus has received less attention. Here, we investigate the ability of small RNAs to redirect splicing. We identify RNAs targeting an aberrant splice site that restore splicing and production of functional protein. RNAs can target sequences within exons or introns and affect the inclusion of exons within SMN2 and dystrophin, genes responsible for spinal muscular atrophy and Duchenne muscular dystrophy, respectively. Duplex RNAs recruit argonaute 2 (AGO2) to pre-mRNA transcripts and altered splicing requires AGO2 expression. AGO2 promotes transcript cleavage in the cytoplasm, but recruitment of AGO2 to pre-mRNAs does not reduce transcript levels, exposing a difference between cytoplasmic and nuclear pathways. Involvement of AGO2 in splicing, a classical nuclear process, reinforces the conclusion from studies of RNA-mediated transcriptional silencing that RNAi pathways can be adapted to function in the mammalian nucleus. These data provide a new strategy for controlling splicing and expand the reach of small RNAs within the nucleus of mammalian cells.

摘要

双链 RNA 是在哺乳动物细胞质中沉默基因表达的有效工具。双链 RNA 控制核内表达的潜力受到的关注较少。在这里,我们研究了小 RNA 重新引导剪接的能力。我们确定了靶向异常剪接位点的 RNA,这些 RNA 可以恢复剪接并产生功能性蛋白质。RNA 可以靶向外显子或内含子中的序列,并影响 SMN2 和 dystrophin 基因的外显子包含,这两个基因分别负责脊髓性肌萎缩症和杜氏肌营养不良症。双链 RNA 招募 Argonaute 2(AGO2)到 pre-mRNA 转录本中,并且改变的剪接需要 AGO2 的表达。AGO2 在细胞质中促进转录本切割,但 AGO2 对 pre-mRNAs 的募集不会降低转录本水平,这揭示了细胞质和核途径之间的差异。AGO2 参与剪接这一经典核过程,这一事实强化了 RNA 介导的转录沉默研究的结论,即 RNAi 途径可以适应在哺乳动物核内发挥作用。这些数据提供了一种控制剪接的新策略,并扩展了小 RNA 在哺乳动物细胞核内的作用范围。

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