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Macromolecular Crowding Induces Spatial Correlations That Control Gene Expression Bursting Patterns

机译:大分子挤在一起控制基因表达爆裂模式的空间相关性

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Recent superresolution microscopy studies in i>E.?coli demonstrate that the cytoplasm has highly variable local concentrations where macromolecular crowding plays a central role in establishing membrane-less compartmentalization. This spatial inhomogeneity significantly influences molecular transport and association processes central to gene expression. Yet, little is known about how macromolecular crowding influences gene expression bursting—the episodic process where mRNA and proteins are produced in bursts. Here, we simultaneously measured mRNA and protein reporters in cell-free systems, showing that macromolecular crowding decoupled the well-known relationship between fluctuations in the protein population (noise) and mRNA population statistics. Crowded environments led to a 10-fold increase in protein noise even though there were only modest changes in the mRNA population and fluctuations. Instead, cell-like macromolecular crowding created an inhomogeneous spatial distribution of mRNA (“spatial noise”) that led to large variability in the protein production burst size. As a result, the mRNA spatial noise created large temporal fluctuations in the protein population. These results highlight the interplay between macromolecular crowding, spatial inhomogeneities, and the resulting dynamics of gene expression, and provide insights into using these organizational principles in both cell-based and cell-free synthetic biology.
机译:最近的超级化学显微镜研究在&ltisi中研究表明细胞质具有高度可变的局部浓度,其中大分子挤在建立膜的舱室化方面的核心作用。这种空间不均匀性显着影响分子运输和关联过程对基因表达的核心。然而,关于大分子挤出如何影响基因表达的突发 - 在爆发中产生mRNA和蛋白质的显着过程很少。在这里,我们同时测量无细胞系统中的mRNA和蛋白质记者,显示大分子挤在蛋白质群体(噪声)和mRNA人口统计中波动之间的众所周知的关系。拥挤的环境导致蛋白质噪音增加10倍,即使mRNA人口和波动的变化只有适度变化。相反,细胞样大分子挤在蛋白质生产突发尺寸中产生的mRNA(“空间噪声”)的不均匀空间分布产生了巨大的变化。结果,mRNA空间噪声在蛋白质群体中产生了大的时间波动。这些结果突出了大分子拥挤,空间不均匀性和基因表达所得到的动态之间的相互作用,并在基于细胞和无细胞合成生物学中使用这些组织原理的见解。

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