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首页> 外文期刊>Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses >The multifunctional protein p54nrb/PSF recruits the exonuclease XRN2 to facilitate pre-mRNA 3' processing and transcription termination.
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The multifunctional protein p54nrb/PSF recruits the exonuclease XRN2 to facilitate pre-mRNA 3' processing and transcription termination.

机译:多功能蛋白p54nrb / PSF募集核酸外切酶XRN2,以促进mRNA前3'的加工和转录终止。

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摘要

Termination of RNA polymerase II transcription frequently requires a poly(A) signal and cleavage/polyadenylation factors. Recent work has shown that degradation of the downstream cleaved RNA by the exonuclease XRN2 promotes termination, but how XRN2 functions with 3'-processing factors to elicit termination remains unclear. Here we show that XRN2 physically associates with 3'-processing factors and accumulates at the 3' end of a transcribed gene. In vitro 3'-processing assays show that XRN2 is necessary to degrade the downstream RNA, but is not required for 3' cleavage. Significantly, degradation of the 3'-cleaved RNA was stimulated when coupled to cleavage. Unexpectedly, while investigating how XRN2 is recruited to the 3'-processing machinery, we found that XRN2 associates with p54nrb/NonO(p54)-protein-associated splicing factor (PSF), multifunctional proteins involved in several nuclear processes. Strikingly, p54 is also required for degradation of the 3'-cleaved RNA in vitro. p54 is present along the length of genes, and small interfering RNA (siRNA)-mediated knockdown leads to defects in XRN2 recruitment and termination. Together, our data indicate that p54nrb/PSF functions in recruitment of XRN2 to facilitate pre-mRNA 3' processing and transcription termination.
机译:RNA聚合酶II转录的终止通常需要poly(A)信号和裂解/聚腺苷酸化因子。最近的工作表明,核酸外切酶XRN2对下游切割的RNA的降解会促进终止,但是XRN2如何与3'-加工因子一起发挥作用来引发终止尚不清楚。在这里,我们显示XRN2在物理上与3'加工因子相关联并积累在转录基因的3'末端。体外3'加工测定表明XRN2是降解下游RNA所必需的,但3'裂解不是必需的。显着地,当与切割偶联时,刺激了3'切割的RNA的降解。出乎意料的是,在调查如何将XRN2募集到3'加工机器时,我们发现XRN2与p54nrb / NonO(p54)-蛋白质相关的剪接因子(PSF),涉及多个核过程的多功能蛋白质相关。令人惊讶的是,在体外降解3'-裂解的RNA时也需要p54。 p54沿着基因的长度存在,而小的干扰RNA(siRNA)介导的敲低导致XRN2募集和终止中的缺陷。总之,我们的数据表明p54nrb / PSF在XRN2募集中起作用,以促进mRNA前3'的加工和转录终止。

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