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首页> 外文期刊>Scientific reports. >U6atac snRNA stem-loop interacts with U12 p65 RNA binding protein and is functionally interchangeable with the U12 apical stem-loop III
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U6atac snRNA stem-loop interacts with U12 p65 RNA binding protein and is functionally interchangeable with the U12 apical stem-loop III

机译:U6atac snRNA茎环与U12 p65 RNA结合蛋白相互作用,并且在功能上可与U12顶端茎环III互换

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Formation of catalytic core of the U12-dependent spliceosome involves U6atac and U12 interaction with the 5' splice site and branch site regions of a U12-dependent intron, respectively. Beyond the formation of intermolecular helix I region between U6atac and U12 snRNAs, several other regions within these RNA molecules are predicted to form stem-loop structures. Our previous work demonstrated that the 3' stem-loop region of U6atac snRNA contains a U12-dependent spliceosome-specific targeting activity. Here, we show a detailed structure-function analysis and requirement of a substructure of U6atac 3' stem-loop in U12-dependent in vivo splicing. We show that the C-terminal RNA recognition motif of p65, a U12 snRNA binding protein, also binds to the distal 3' stem-loop of U6atac. By using a binary splice site mutation suppressor assay we demonstrate that p65 protein-binding apical stem-loop of U12 snRNA can be replaced by this U6atac distal 3' stem-loop. Furthermore, we tested the compatibility of the U6atac 3' end from phylogenetically distant species in a human U6atac background, to establish the evolutionary relatedness of these structures and in vivo function. In summary, we demonstrate that RNA-RNA and RNA-protein interactions in the minor spliceosome are highly plastic as compared to the major spliceosome.
机译:U12依赖性剪接体催化核心的形成涉及U6atac和U12分别与U12依赖性内含子的5'剪接位点和分支位点区域相互作用。除了在U6atac和U12 snRNA之间形成分子间螺旋I区以外,还预计这些RNA分子内的其他几个区域会形成茎环结构。我们以前的工作表明,U6atac snRNA的3'茎环区域包含U12依赖性剪接体特异性靶向活性。在这里,我们显示了详细的结构功能分析和U12依赖的体内剪接中U6atac 3'茎环的亚结构的要求。我们显示,p65,U12 snRNA结合蛋白的C端RNA识别基序也结合到U6atac的远端3'茎环。通过使用二进制剪接位点突变抑制试验,我们证明了U12 snRNA的p65蛋白结合顶端茎环可以被该U6atac远端3'茎环代替。此外,我们在人类U6atac背景中测试了系统发育远缘物种的U6atac 3'末端的相容性,以建立这些结构与体内功能的进化相关性。总之,我们证明,与主要剪接体相比,次要剪接体中的RNA-RNA和RNA-蛋白质相互作用具有很高的可塑性。

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