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Elucidating the connection between cell population heterogeneity and genetic regulatory architecture in specific artificial networks.

机译:阐明特定人工网络中细胞种群异质性与遗传调控体系结构之间的联系。

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Understanding the expression patterns of simple, synthetic gene regulatory networks will not only shed light into the complexity of naturally occurring networks, but it will also provide a platform for expression control that can be valuable in biotechnological applications. The expression of regulatory networks is influenced by the fact that the intracellular environment varies among the cells of a population. In turn, this variability is tightly related to the architecture of such networks. The relationship between the architecture of synthetic regulatory networks and cell population heterogeneity was studied using two model regulatory networks: a gene-switching system and an oscillatory system. A green fluorescent protein (GFP) served as the reporter for both systems, which were expressed from plasmids in the Gram-negative bacterium Escherichia coli. Inducer concentrations were varied in shake flask cultures, and GFP distributions were monitored over time with flow cytometry.;In studying the effect of GFP half-life on the gene-switching network behavior, we observed how it influences the view of the network behavior: using a lower half-life GFP reduced the inducer concentration range at which we could distinguish between network states due to lower GFP expression, but its use also showed better evidence of the fast-switching transient behavior predicted by the network architecture through wider separation of states. The oscillatory network was shown to exhibit three steady states, bi-threshold behavior, and multiplicity, contrary to behavior predicted by an existing model. We experimentally discovered four significant nonspecific interactions between promoters and repressors within the network that, through modeling, can be shown to qualitatively create the behavior experimentally observed.;Beyond the understanding of network behavior gained through the combination of average and population-level data, the distributions demonstrated a connection between the network architecture and heterogeneity. We found heterogeneity expanded at intermediate inducer levels in both networks, when the distribution was bimodal (gene-switching network) or individual cells were displaying oscillatory behavior (oscillatory network). Both the oscillatory behavior and bimodal distributions are a result of the network architectures. We had the ability to restrict heterogeneity with multiple inducers in the oscillatory network. However, there were observable limits in doing so.
机译:了解简单的合成基因调控网络的表达模式,不仅可以揭示自然发生的网络的复杂性,而且还可以为表达控制提供一个平台,该平台在生物技术应用中非常有价值。调节网络的表达受群体细胞间细胞内环境变化这一事实的影响。反过来,这种可变性与此类网络的体系结构紧密相关。使用两个模型调控网络研究了合成调控网络的体系结构与细胞群体异质性之间的关系:基因转换系统和振荡系统。绿色荧光蛋白(GFP)作为这两个系统的报告基因,由革兰氏阴性细菌大肠杆菌中的质粒表达。摇瓶培养物中的诱导物浓度各不相同,并通过流式细胞仪监测GFP的分布。在研究GFP半衰期对基因转换网络行为的影响时,我们观察到了它如何影响网络行为的观点:使用较低半衰期的GFP会降低诱导剂浓度范围,由于GFP较低的表达,我们可以在其中区分网络状态,但是使用它还显示出网络架构通过更广泛的状态分离预测的快速切换瞬态行为的更好证据。与现有模型所预测的行为相反,该振荡网络显示出三个稳态,双阈值行为和多重性。我们通过实验发现了网络中启动子和阻遏物之间的四个重要的非特异性相互作用,通过建模可以证明它们定性地创建了实验观察到的行为。除了对通过平均和总体水平数据相结合而获得的网络行为的了解之外,发行版证明了网络体系结构和异构之间的联系。我们发现,当分布为双峰分布(基因转换网络)或单个细胞表现出振荡行为(振荡网络)时,两个网络中的诱导物水平均会扩大异质性。振荡行为和双峰分布都是网络体系结构的结果。我们有能力限制振荡网络中多个诱导物的异质性。但是,这样做有明显的限制。

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