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首页> 外文期刊>Biochimica et Biophysica Acta. Gene Regulatory Mechanisms >The mechanism of splicing as told by group II introns: Ancestors of the spliceosome
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The mechanism of splicing as told by group II introns: Ancestors of the spliceosome

机译:由II族内含子的剪接机制:脾脏的祖先

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Spliceosomal introns and self-splicing group II introns share a common mechanism of intron splicing where two sequential transesterification reactions remove intron lariats and ligate exons. The recent revolution in cryo-electron microscopy (cryo-EM) has allowed visualization of the spliceosome's ribozyme core. Comparison of these cryo-EM structures to recent group 11 intron crystal structures presents an opportunity to draw parallels between the RNA active site, substrate positioning, and product formation in these two model systems of intron splicing. In addition to shared RNA architectural features, structural similarity between group 11 intron encoded proteins (IEPs) and the integral spliceosomal protein Prp8 further support a shared catalytic core. These mechanistic and structural similarities support the long-held assertion that group II introns and the eukaryotic spliceosome have a common evolutionary origin. In this review, we discuss how recent structural insights into group II introns and the spliceosome facilitate the chemistry of splicing, highlight similarities between the two systems, and discuss their likely evolutionary connections. This article is part of a Special Issue entitled: RNA structure and splicing regulation edited by Francisco Baralle, Ravindra Singh and Stefan Stamm.
机译:抗乳糖体内含子和自剪族II内外内含子共享内含子剪接的常见机制,其中两个连续的酯交换反应除去内含子松弛和拉伸外显子。最近在Cryo-Electronic显微镜(Cryo-EM)中的旋转允许可视化抗肌腱核酶核心。这些冷冻组结构对近期组11的综合晶体结构的比较呈现了在该两种内含子剪接的两种模型系统中在RNA活性位点,衬底定位和产品形成之间绘制平扰的机会。除了共享的RNA建筑特征外,第11组内含子编码蛋白(IEP)和整体抗乳糖体蛋白PRP8还支持共用催化核的结构相似性。这些机械和结构相似之处支持二族内含子和真核剪接组的长期断言具有常见的进化来源。在这篇综述中,我们讨论了最近的结构洞察II族内含子和脾脏促进拼接化学,突出了两个系统之间的相似性,并讨论了他们可能的进化连接。本文是题为特殊问题的一部分:RNA结构和Francisco Baralle,Ravindra Singh和Stefan STAM编辑的剪接规范。

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