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Frequency Domain Analysis of Fluctuations of mRNA and Protein Copy Numbers within a Cell Lineage: Theory and Experimental Validation

机译:细胞谱系MRNA和蛋白质拷贝数波动的频域分析:理论与实验验证

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The stochasticity of gene expression is manifested in the fluctuations of messenger ribonucleic acid and protein copy numbers within a cell lineage over time. While data of this type can be obtained for many generations, most mathematical models are unsuitable to interpret such data since they assume nongrowing cells. Here we develop a theoretical approach that quantitatively links the frequency content of lineage data to subcellular dynamics. We elucidate how the position, height, and width of the peaks in the power spectrum provide a distinctive fingerprint that encodes a wealth of information about mechanisms controlling transcription, translation, replication, degradation, bursting, promoter switching, cell cycle duration, cell division, gene dosage compensation, and cell-size homeostasis. Predictions are confirmed by analysis of single-cell Escherichia coli data obtained using fluorescence microscopy. Furthermore, by matching the experimental and theoretical power spectra, we infer the temperature-dependent gene expression parameters, without the need of measurements relating fluorescence intensities to molecule numbers.
机译:基因表达的随机性表现在细胞谱系随时间内的信使核糖核酸和蛋白质拷贝数的波动中。虽然可以获得这种类型的数据,但是对于许多代来说,大多数数学模型都不适合解释这些数据,因为它们假设非创业单元。在这里,我们开发一种理论方法,可以定量地将谱系数据的频率内容链接到亚细胞动态。我们阐明功率谱中峰值的位置,高度和宽度提供了一种独特的指纹,可以编码有关控制转录,翻译,复制,劣化,爆破,启动子切换,细胞周期持续时间,细胞划分的机制的丰富信息的特殊指纹。基因剂量补偿和细胞大小的稳态。通过分析使用荧光显微镜获得的单细胞大肠杆菌数据来确认预测。此外,通过匹配实验和理论功率谱,我们推断温度依赖性基因表达参数,而不需要测量与分子数相关的荧光强度。

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