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Conserved Cis-Regulatory Modules Control Robustness in Msx1 Expression at Single-Cell Resolution

机译:保守的顺式调节模块以单细胞分辨率控制Msx1表达的鲁棒性

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摘要

The process of transcription is highly stochastic leading to cell-to-cell variations and noise in gene expression levels. However, key essential genes have to be precisely expressed at the correct amount and time to ensure proper cellular development and function. Studies in yeast and bacterial systems have shown that gene expression noise decreases as mean expression levels increase, a relationship that is controlled by promoter DNA sequence. However, the function of distal cis-regulatory modules (CRMs), an evolutionary novelty of metazoans, in controlling transcriptional robustness and variability is poorly understood. In this study, we used live cell imaging of transfected reporters combined with a mathematical modelling and statistical inference scheme to quantify the function of conserved Msx1 CRMs and promoters in modulating single-cell real-time transcription rates in C2C12 mouse myoblasts. The results show that the mean expression–noise relationship is solely promoter controlled for this key pluripotency regulator. In addition, we demonstrate that CRMs modulate single-cell basal promoter rate distributions in a graded manner across a population of cells. This extends the rheostatic model of CRM action to provide a more detailed understanding of CRM function at single-cell resolution. We also identify a novel CRM transcriptional filter function that acts to reduce intracellular variability in transcription rates and show that this can be phylogenetically separable from rate modulating CRM activities. These results are important for understanding how the expression of key vertebrate developmental transcription factors is precisely controlled both within and between individual cells.
机译:转录过程是高度随机的,导致细胞间差异和基因表达水平的噪音。但是,关键的必需基因必须以正确的数量和时间精确表达,以确保适当的细胞发育和功能。酵母和细菌系统的研究表明,基因表达噪音随平均表达水平的提高而降低,这种关系由启动子DNA序列控制。但是,人们对远端顺式调控模块(CRM)(后生动物的进化新奇)在控制转录鲁棒性和可变性方面的功能了解甚少。在这项研究中,我们使用转染报告基因的活细胞成像,结合数学建模和统计推断方案,量化保守的Msx1 CRM和启动子在调节C2C12小鼠成肌细胞单细胞实时转录率中的功能。结果表明,对于这种关键的多能性调节剂,平均表达与噪声的关系仅受启动子控制。此外,我们证明了CRM可以在整个细胞群体中以渐变的方式调节单细胞基础启动子的速率分布。这扩展了CRM动作的变阻模型,以在单细胞分辨率下提供对CRM功能的更详细的了解。我们还确定了一种新型的CRM转录过滤功能,其功能是减少转录速率的细胞内变异性,并表明这可以从速率调控CRM活动的系统发育上分离。这些结果对于理解关键脊椎动物发育转录因子的表达如何在单个细胞内和细胞之间被精确控制非常重要。

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