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RNA 聚合酶 II 延伸抑制对可变剪接调控的全球影响。

Global impact of RNA polymerase II elongation inhibition on alternative splicing regulation.

机构信息

Banting and Best Department of Medical Research, Donnelly Centre, University of Toronto, Toronto, Ontario M5S 3E1, Canada.

出版信息

Genome Res. 2011 Mar;21(3):390-401. doi: 10.1101/gr.111070.110. Epub 2010 Dec 16.

Abstract

The rate of RNA polymerase II (Pol II) elongation can influence splice site selection in nascent transcripts, yet the extent and physiological relevance of this kinetic coupling between transcription and alternative splicing (AS) is not well understood. We performed experiments to perturb Pol II elongation and then globally compared AS patterns with genome-wide Pol II occupancy. RNA binding and RNA processing functions were significantly enriched among the genes with Pol II elongation inhibition-dependent changes in AS. Under conditions that interfere with Pol II elongation, including cell stress, increased Pol II occupancy was detected in the intronic regions flanking the alternative exons in these genes, and these exons generally became more included. A disproportionately high fraction of these exons introduced premature termination codons that elicited nonsense-mediated mRNA decay (NMD), thereby further reducing transcript levels. Our results provide evidence that kinetic coupling between transcription, AS, and NMD affords a rapid mechanism by which cells can respond to changes in growth conditions, including cell stress, to coordinate the levels of RNA processing factors with mRNA levels.

摘要

RNA 聚合酶 II(Pol II)延伸的速度可以影响新生转录本中剪接位点的选择,然而,这种转录和可变剪接(AS)之间的动力学偶联的程度和生理相关性还不是很清楚。我们进行了实验来干扰 Pol II 延伸,然后全局比较了 AS 模式与全基因组 Pol II 占据。在 RNA 结合和 RNA 加工功能在基因中显著富集,这些基因的 AS 随着 Pol II 延伸抑制而发生变化。在干扰 Pol II 延伸的条件下,包括细胞应激,在这些基因的可变外显子侧翼的内含子区域中检测到了更多的 Pol II 占据,并且这些外显子通常变得更被包含。这些外显子中引入了大量的终止密码子,引发无意义介导的 mRNA 降解(NMD),从而进一步降低了转录本水平。我们的结果提供了证据表明,转录、AS 和 NMD 之间的动力学偶联为细胞提供了一种快速的机制,可以使其能够响应生长条件的变化,包括细胞应激,从而协调 RNA 加工因子的水平与 mRNA 水平。

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