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A Multi-Parameter Analysis of Cellular Coordination of Major Transcriptome Regulation Mechanisms

机译:主要转录组调控机制的细胞协调的多参数分析。

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摘要

To understand cellular coordination of multiple transcriptome regulation mechanisms, we simultaneously measured transcription rate (TR), mRNA abundance (RA) and translation activity (TA). This revealed multiple insights. First, the three parameters displayed systematic statistical differences. Sequentially more genes exhibited extreme (low or high) expression values from TR to RA, and then to TA; that is, cellular coordination of multiple transcriptome regulatory mechanisms leads to sequentially enhanced gene expression selectivity as the genetic information flow from the genome to the proteome. Second, contribution of the stabilization-by-translation regulatory mechanism to the cellular coordination process was assessed. The data enabled an estimation of mRNA stability, revealing a moderate but significant positive correlation between mRNA stability and translation activity. Third, the proportion of mRNA occupied by un-translated regions (UTR) exhibited a negative relationship with the level of this correlation, and was thus a major determinant of the mode of regulation of the mRNA. High-UTR-proportion mRNAs tend to defy the stabilization-by-translation regulatory mechanism, staying out of the polysome but remaining stable; mRNAs with little UTRs largely followed this regulation. In summary, we quantitatively delineated the relationship among multiple transcriptome regulation parameters, i.e., cellular coordination of corresponding regulatory mechanisms.
机译:为了解多种转录组调控机制的细胞协调作用,我们同时测量了转录速率(TR),mRNA丰度(RA)和翻译活性(TA)。这揭示了多种见解。首先,这三个参数显示出系统的统计差异。从TR到RA,再到TA,依次有更多的基因表现出极高的(低或高)表达值。也就是说,随着遗传信息从基因组流向蛋白质组,多种转录组调控机制的细胞协调会导致顺序增强的基因表达选择性。其次,评估了翻译稳定化调节机制对细胞协调过程的贡献。数据使得能够估计mRNA的稳定性,揭示了mRNA稳定性和翻译活性之间中等但显着的正相关。第三,非翻译区(UTR)所占据的mRNA比例与该相关水平呈负相关,因此是mRNA调控方式的主要决定因素。高UTR比例的mRNA倾向于违抗翻译稳定调节机制,不参与多核糖体,但保持稳定。具有很少UTR的mRNA在很大程度上遵循这一规定。总之,我们定量地描述了多个转录组调节参数之间的关系,即相应调节机制的细胞协调。

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