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The FCP1 phosphatase interacts with RNA polymerase II and with MEP50 a component of the methylosome complex involved in the assembly of snRNP

机译:FCP1磷酸酶与RNA聚合酶II和MEP50相互作用MEP50是与snRNP组装有关的甲基体复合物的组分

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摘要

RNA polymerase II transcription is associated with cyclic phosphorylation of the C-terminal domain (CTD) of the large subunit of RNA polymerase II. To date, FCP1 is the only specific CTD phosphatase, which is required for general transcription and cell viability. To identify FCP1-associated proteins, we constructed a human cell line expressing epitope-tagged FCP1. In addition to RAP74, a previously identified FCP1 interacting factor, we determined that FCP1-affinity purified extracts contain RNAPII that has either a hyper- or a hypo-phosphorylated CTD. In addition, by mass spectrometry of affinity purified FCP1-associated factors, we identified a novel FCP1-interacting protein, named MEP50, a recently described component of the methylosome complex that binds to the snRNP’s Sm proteins. We found that FCP1 specifically interacts with components of the spliceosomal U small nuclear ribonucleoproteins. These results suggest a putative role of FCP1 CTD-phosphatase in linking the transcription elongation with the splicing process.
机译:RNA聚合酶II转录与RNA聚合酶II大亚基的C末端结构域(CTD)的环状磷酸化有关。迄今为止,FCP1是唯一的特异性CTD磷酸酶,是一般转录和细胞活力所必需的。为了鉴定与FCP1相关的蛋白质,我们构建了一个表达表位标记的FCP1的人细胞系。除了RAP74(先前确定的FCP1相互作用因子)外,我们还确定FCP1亲和纯化的提取物含有具有高磷酸化CTD或低磷酸化CTD的RNAPII。此外,通过亲和纯化的FCP1相关因子的质谱分析,我们鉴定了一种新型的FCP1相互作用蛋白,称为MEP50,这是一种最近描述的与snRNP的Sm蛋白结合的甲基化复合物成分。我们发现FCP1专门与剪接U小核核糖核蛋白的成分相互作用。这些结果表明,FCP1 CTD-磷酸酶在将转录延伸与剪接过程联系起来方面具有假定作用。

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