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Conserved domains of human U4 snRNA required for snRNP and spliceosome assembly

机译:snRNP和剪接体组装所需的人U4 snRNA保守域

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U4 snRNA is phylogenetically highly conserved and organized in several domains. To determine the function of each of the domains of human U4 snRNA in the multi-step process of snRNP and spliceosome assembly, we used reconstitution procedures in combination with snRNA mutagenesis. The highly conserved 5′ terminal domain of U4 snRNA consists of the stem I and stem II regions that have been proposed to base pair with U6 snRNA, and the 5′ stem-loop structure. We found that each of these structural elements is essential for spliceosome assembly. However, only the stem II region is required for U4-U6 interaction, and none of these elements for Sm protein binding. In contrast, the 3′ terminal domain of U4 snRNA containing the Sm binding site is dispensable for both U4-U6 interaction and spliceosome assembly. Our results support an organization of the U4 snRNP into multiple functional domains, each of which acts at distinct stages of snRNP and spliceosome assembly.
机译:U4 snRNA在系统发育上高度保守,并在多个域中组织。为了确定人U4 snRNA的每个结构域在snRNP和剪接体组装的多步过程中的功能,我们将重组程序与snRNA诱变结合使用。 U4 snRNA的高度保守的5'末端结构域由提议与U6 snRNA碱基配对的茎I和茎II区域以及5'茎环结构组成。我们发现这些结构元素中的每一个对于剪接体组装都是必不可少的。但是,U4-U6相互作用仅需要茎II区,而Sm蛋白结合则不需要这些元素。相反,包含Sm结合位点的U4 snRNA的3'末端结构域对于U4-U6相互作用和剪接体组装都是可有可无的。我们的结果支持将U4 snRNP组织到多个功能域中,每个功能域都在snRNP和剪接体组装的不同阶段起作用。

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