首页> 美国卫生研究院文献>Nucleic Acids Research >The human Imp3 and Imp4 proteins form a ternary complex with hMpp10 which only interacts with the U3 snoRNA in 60–80S ribonucleoprotein complexes
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The human Imp3 and Imp4 proteins form a ternary complex with hMpp10 which only interacts with the U3 snoRNA in 60–80S ribonucleoprotein complexes

机译:人类的Imp3和Imp4蛋白与hMpp10形成三元复合物该复合物仅与60-80S核糖核蛋白复合物中的U3 snoRNA相互作用。

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摘要

Ribosome biogenesis requires a vast number of trans-acting factors many of which are required for the chemical modification and processing of the pre-rRNA component. The U3 snoRNP complex is required for the early cleavage steps in pre-rRNA processing. We have cloned cDNAs encoding the human and mouse homologs of the yeast U3 snoRNP-associated proteins Imp3 and Imp4. Both human proteins localize to nucleoli and interact with the U3 snoRNA. The results of complementation experiments show that, in contrast to mouse Imp4, mouse Imp3 can partially alleviate the growth defect of the corresponding yeast null strain, indicating that the role of Imp3 in pre-rRNA processing is evolutionarily conserved. The results of density gradient centrifugation experiments show that, in contrast to hU3-55K, the human Imp3 and Imp4 proteins predominantly interact with the U3 snoRNA in 60–80S ribonucleoprotein complexes. In addition, we have found that hImp3, hImp4 and hMpp10 can form a stable hetero-trimeric complex in vitro, which is generated by direct interactions of both hImp3 and hImp4 with hMpp10. The analysis of hImp3 and hImp4 mutants indicated that their binding to hMpp10 correlates with their nucleolar accumulation, strongly suggesting that the formation of the ternary complex of hImp3, hImp4 and hMpp10 is required for their association with nucleolar components.
机译:核糖体生物发生需要大量的反式作用因子,其中许多是前rRNA成分的化学修饰和加工所必需的。 U3 snoRNP复合物是rRNA加工前的早期切割步骤所必需的。我们已经克隆了编码与酵母U3 snoRNP相关的蛋白Imp3和Imp4的人和小鼠同源物的cDNA。两种人类蛋白都位于核仁并与U3 snoRNA相互作用。互补实验的结果表明,与小鼠Imp4相比,小鼠Imp3可以部分缓解相应酵母无效菌株的生长缺陷,这表明Imp3在pre-rRNA加工中的作用在进化上是保守的。密度梯度离心实验的结果表明,与hU3-55K相比,人的Imp3和Imp4蛋白主要与60-80S核糖核蛋白复合物中的U3 snoRNA相互作用。此外,我们发现hImp3,hImp4和hMpp10可以在体外形成稳定的异三聚体复合物,这是由hImp3和hImp4与hMpp10的直接相互作用生成的。对hImp3和hImp4突变体的分析表明,它们与hMpp10的结合与其核仁积累相关,强烈暗示了hImp3,hImp4和hMpp10三元复合物的形成是它们与核仁成分结合所必需的。

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