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外显子连接复合物控制着果蝇中 MAPK 和其他含有长内含子的转录本的剪接。

The exon junction complex controls the splicing of MAPK and other long intron-containing transcripts in Drosophila.

机构信息

Institute for Research in Immunology and Cancer, Laboratory of Intracellular Signaling, Université de Montréal, C.P. 6128, Succursale Centre-Ville, Montreal, Quebec, H3C 3J7, Canada.

出版信息

Cell. 2010 Oct 15;143(2):251-62. doi: 10.1016/j.cell.2010.09.014.

Abstract

Signaling pathways are controlled by a vast array of posttranslational mechanisms. By contrast, little is known regarding the mechanisms that regulate the expression of their core components. We conducted an RNAi screen in Drosophila for factors modulating RAS/MAPK signaling and identified the Exon Junction Complex (EJC) as a key element of this pathway. The EJC binds the exon-exon junctions of mRNAs and thus far, has been linked exclusively to postsplicing events. Here, we report that the EJC is required for proper splicing of mapk transcripts by a mechanism that apparently controls exon definition. Moreover, whole transcriptome and RT-PCR analyses of EJC-depleted cells revealed that the splicing of long intron-containing genes, which includes mapk, is sensitive to EJC activity. These results identify a role for the EJC in the splicing of a subset of transcripts and suggest that RAS/MAPK signaling depends on the regulation of MAPK levels by the EJC.

摘要

信号通路受到大量翻译后调控机制的控制。相比之下,对于调控其核心成分表达的机制知之甚少。我们在果蝇中进行了一项 RNAi 筛选,以寻找调节 RAS/MAPK 信号的因子,并发现外显子结合复合物(EJC)是该途径的关键组成部分。EJC 结合 mRNA 的外显子-外显子接头,迄今为止,它仅与转录后事件有关。在这里,我们报告 EJC 通过一种显然控制外显子定义的机制,是 mapk 转录物正确剪接所必需的。此外,EJC 耗尽细胞的全转录组和 RT-PCR 分析表明,包括 mapk 在内的长内含子基因的剪接对 EJC 活性敏感。这些结果确定了 EJC 在一组转录物剪接中的作用,并表明 RAS/MAPK 信号取决于 EJC 对 MAPK 水平的调节。

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