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High-Resolution Sequencing and Modeling Identifies Distinct Dynamic RNA Regulatory Strategies

机译:高分辨率测序和建模识别不同的动态RNa调控策略

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摘要

Cells control dynamic transitions in transcript levels by regulating transcription, processing, and/or degradation through an integrated regulatory strategy. Here, we combine RNA metabolic labeling, rRNA-depleted RNA-seq, and DRiLL, a novel computational framework, to quantify the level; editing sites; and transcription, processing, and degradation rates of each transcript at a splice junction resolution during the LPS response of mouse dendritic cells. Four key regulatory strategies, dominated by RNA transcription changes, generate most temporal gene expression patterns. Noncanonical strategies that also employ dynamic posttranscriptional regulation control only a minority of genes, but provide unique signal processing features. We validate Tristetraprolin (TTP) as a major regulator of RNA degradation in one noncanonical strategy. Applying DRiLL to the regulation of noncoding RNAs and to zebrafish embryogenesis demonstrates its broad utility. Our study provides a new quantitative approach to discover transcriptional and posttranscriptional events that control dynamic changes in transcript levels using RNA sequencing data.
机译:细胞通过整合的调控策略来调控转录,加工和/或降解,从而控制转录水平的动态转变。在这里,我们结合了RNA代谢标记,耗尽rRNA的RNA-seq和新颖的计算框架DRiLL来量化水平。编辑网站;小鼠树突状细胞LPS应答过程中,每个转录本在剪接连接处的转录,加工和降解速率。以RNA转录变化为主导的四种主要调控策略产生了大多数瞬时基因表达模式。也采用动态转录后调控的非经典策略仅控制少数基因,但提供独特的信号处理功能。我们验证Tristetraprolin(TTP)作为一种非经典策略中RNA降解的主要调节剂。将DRiLL应用于非编码RNA的调控和斑马鱼的胚胎发生证明了其广泛的实用性。我们的研究提供了一种新的定量方法来发现转录和转录后事件,这些事件可使用RNA测序数据来控制转录水平的动态变化。

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