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性致死蛋白的氨基末端介导RNA结合中的协同相互作用,对剪接调控至关重要。

The Sex-lethal amino terminus mediates cooperative interactions in RNA binding and is essential for splicing regulation.

作者信息

Wang J, Bell L R

机构信息

Department of Biological Sciences, University of Southern California, Los Angeles 90089-1340.

出版信息

Genes Dev. 1994 Sep 1;8(17):2072-85. doi: 10.1101/gad.8.17.2072.

Abstract

Sex-lethal (Sxl) acts as a binary switch that regulates Drosophila sexual differentiation and dosage compensation and also maintains a stable female state through autoregulation. As part of a cascade of genes that are regulated by sex-specific splicing, Sxl controls the sex-specific splicing of transformer (tra) RNA and also its own RNA. Sxl contains two RNP-CS (RNA-binding) domains and is known to bind tra pre-mRNA near the alternative 3' splice site, thus blocking use of that site to give the female-specific splicing pattern. Here, we test how Sxl protein interacts with Sxl RNA during autoregulation. We show that Sxl not only binds Sxl pre-mRNA near the alternative 3' splice site but also at distant, multiple sites surrounding the Sxl alternative exon. Moreover, Sxl binds cooperatively at these multiple sites. The Sxl amino terminus is essential for the cooperative interaction and is also required for regulatory activity in vivo. It appears that this region of Sxl protein, which resembles regions in some other RNA-binding proteins, is a domain that mediates protein-protein interactions during RNA binding and plays an important role in splicing regulation.

摘要

性致死基因(Sex-lethal,Sxl)作为一个二元开关,调控果蝇的性别分化和剂量补偿,还通过自我调节维持稳定的雌性状态。作为由性别特异性剪接调控的一系列基因的一部分,Sxl控制transformer(tra)RNA以及其自身RNA的性别特异性剪接。Sxl包含两个RNP-CS(RNA结合)结构域,已知它在可变3'剪接位点附近结合tra前体mRNA,从而阻止该位点的使用,产生雌性特异性剪接模式。在这里,我们测试Sxl蛋白在自我调节过程中如何与Sxl RNA相互作用。我们发现Sxl不仅在可变3'剪接位点附近结合Sxl前体mRNA,还在Sxl可变外显子周围的多个远距离位点结合。此外,Sxl在这些多个位点协同结合。Sxl氨基末端对于协同相互作用至关重要,在体内调节活性中也是必需的。看来Sxl蛋白的这个区域类似于其他一些RNA结合蛋白中的区域,是一个在RNA结合过程中介导蛋白质-蛋白质相互作用并在剪接调控中起重要作用的结构域。

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