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The NIP7 protein is required for accurate pre-rRNA processing in human cells

机译:NIP7蛋白是在人类细胞中进行准确的rRNA前加工所必需的

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摘要

Eukaryotic ribosome biogenesis requires the function of a large number of trans-acting factors which interact transiently with the nascent pre-rRNA and dissociate as the ribosomal subunits proceed to maturation and export to the cytoplasm. Loss-of-function mutations in human trans-acting factors or ribosome components may lead to genetic syndromes. In a previous study, we have shown association between the SBDS (Shwachman–Bodian–Diamond syndrome) and NIP7 proteins and that downregulation of SBDS in HEK293 affects gene expression at the transcriptional and translational levels. In this study, we show that downregulation of NIP7 affects pre-rRNA processing, causing an imbalance of the 40S/60S subunit ratio. We also identified defects at the pre-rRNA processing level with a decrease of the 34S pre-rRNA concentration and an increase of the 26S and 21S pre-rRNA concentrations, indicating that processing at site 2 is particularly slower in NIP7-depleted cells and showing that NIP7 is required for maturation of the 18S rRNA. The NIP7 protein is restricted to the nuclear compartment and co-sediments with complexes with molecular masses in the range of 40S–80S, suggesting an association to nucleolar pre-ribosomal particles. Downregulation of NIP7 affects cell proliferation, consistently with an important role for NIP7 in rRNA biosynthesis in human cells.
机译:真核生物核糖体的生物发生需要大量的反式作用因子的功能,这些因子与新生的pre-rRNA瞬时相互作用,并随着核糖体亚基的成熟和输出而解离。人类反式作用因子或核糖体成分的功能丧失突变可能导致遗传综合征。在先前的研究中,我们显示了SBDS(Shwachman–Bodian–Diamond综合征)和NIP7蛋白之间的关联,并且HEK293中SBDS的下调会影响转录和翻译水平的基因表达。在这项研究中,我们表明NIP7的下调会影响rRNA的前处理,从而导致40S / 60S亚基比例失衡。我们还确定了pre-rRNA加工水平的缺陷,即34S pre-rRNA浓度的降低以及26S和21S pre-rRNA浓度的增加,这表明在位点2的加工在NIP7耗尽的细胞中特别慢,并且显示NIP7是18S rRNA成熟所必需的。 NIP7蛋白仅限于核区室,并且与分子质量在40S-80S范围内的复合物共沉淀,表明与核仁核糖体前核糖体颗粒相关。 NIP7的下调影响细胞增殖,与NIP7在人类细胞中rRNA生物合成中的重要作用一致。

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