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首页> 外文期刊>Nucleic Acids Research >CWC22-dependent pre-mRNA splicing and eIF4A3 binding enables global deposition of exon junction complexes
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CWC22-dependent pre-mRNA splicing and eIF4A3 binding enables global deposition of exon junction complexes

机译:依赖CWC22的pre-mRNA剪接和eIF4A3结合可实现外显子连接复合物的整体沉积

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摘要

In metazoan cells, spliced mRNAs are marked by the exon junction complex (EJC), a multi-protein complex that serves as a key regulator of post-transcriptional mRNA metabolism. Deposition of EJCs on mRNA is intimately linked to the splicing process. The spliceosomal protein CWC22 directly binds the core EJC-protein eIF4A3, guides it to the spliceosome and initiates EJC assembly. In addition, CWC22 is involved in the splicing process itself, but the molecular details of its dual function remain elusive. Here we analyze the mechanisms, by which CWC22 co-regulates pre-mRNA splicing and EJC assembly. We show that the core of CWC22 is sufficient to mediate both pre-mRNA splicing and EJC assembly. Nonetheless, both processes can be functionally uncoupled with an eIF4A3-binding deficient mutant of CWC22, which impedes EJC assembly. A C-terminal domain of CWC22 strongly enhances its spliceosomal interaction and likely regulates its function. High-throughput RNA-sequencing identifies global defects of pre-mRNA splicing and downregulation of diverse gene expression pathways in CWC22-depleted cells. We propose a model, in which CWC22 represents an integral component of the spliceosome and orchestrates pre-mRNA splicing and eIF4A3 binding to achieve global assembly of exon junction complexes.
机译:在后生动物细胞中,剪接的mRNA由外显子连接复合物(EJC)标记,EJC是一种多蛋白复合物,可作为转录后mRNA代谢的关键调节剂。 EJC在mRNA上的沉积与剪接过程密切相关。剪接体蛋白CWC22直接结合核心EJC蛋白eIF4A3,将其引导至剪接体并启动EJC组装。此外,CWC22本身参与剪接过程,但其双重功能的分子细节仍然难以捉摸。在这里,我们分析了CWC22共同调节mRNA前的剪接和EJC组装的机制。我们显示,CWC22的核心足以介导前mRNA剪接和EJC组装。尽管如此,这两个过程都可以在功能上与CWC22的eIF4A3结合缺陷型突变体解偶联,这阻碍了EJC的组装。 CWC22的C末端域强烈增强其剪接体相互作用,并可能调节其功能。高通量RNA测序可识别出pre-mRNA剪接的整体缺陷以及在CWC22缺失的细胞中多种基因表达途径的下调。我们提出一个模型,其中CWC22代表剪接体的组成部分,并编排pre-mRNA剪接和eIF4A3结合以实现外显子连接复合体的整体组装。

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