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The BRCT domain of mammalian Pes1 is crucial for nucleolar localization and rRNA processing

机译:哺乳动物Pes1的BRCT结构域对核仁定位和rRNA加工至关重要

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The nucleolar protein Pes1 interacts with Bop1 and WDR12 in a stable complex (PeBoW-complex) and its expression is tightly associated with cell proliferation. The yeast homologue Nop7p (Yph1p) functions in both, rRNA processing and cell cycle progression. The presence of a BRCT-domain (BRCA1 C-terminal) within Pes1 is quite unique for an rRNA processing factor, as this domain is normally found in factors involved in DNA-damage or repair pathways. Thus, the function of the BRCT-domain in Pes1 remains elusive. We established a conditional siRNA-based knock-down-knock-in system and analysed a panel of Pes1 truncation mutants for their functionality in ribosome synthesis in the absence of endogenous Pes1. Deletion of the BRCT-domain or single point mutations of highly conserved residues caused diffuse nucleoplasmic distribution and failure to replace endogenous Pes1 in rRNA processing. Further, the BRCT-mutants of Pes1 were less stable and not incorporated into the PeBoW-complex. Hence, the integrity of the BRCT-domain of Pes1 is crucial for nucleolar localization and its function in rRNA processing.
机译:核仁蛋白Pes1在稳定的复合体(PeBoW-复合体)中与Bop1和WDR12相互作用,并且其表达与细胞增殖紧密相关。酵母同源物Nop7p(Yph1p)在rRNA加工和细胞周期进程中均起作用。 Pes1中存在BRCT结构域(BRCA1 C端)对于rRNA加工因子而言是非常独特的,因为该结构域通常存在于与DNA损伤或修复途径有关的因子中。因此,在Pes1中BRCT域的功能仍然难以捉摸。我们建立了一个有条件的基于siRNA的敲除敲入系统,并分析了一组Pes1截短突变体在不存在内源性Pes1的情况下在核糖体合成中的功能。高度保守残基的BRCT结构域或单点突变的删除导致核仁扩散,并不能替代rRNA加工中的内源Pes1。此外,Pes1的BRCT突变体不稳定,没有掺入PeBoW-复合物中。因此,Pes1的BRCT结构域的完整性对于核仁定位及其在rRNA加工中的功能至关重要。

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