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Transcriptional Regulation by Competing Transcription Factor Modules

机译:通过竞争转录因子模块进行转录调控。

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Gene regulatory networks lie at the heart of cellular computation. In these networks, intracellular and extracellular signals are integrated by transcription factors, which control the expression of transcription units by binding to cis-regulatory regions on the DNA. The designs of both eukaryotic and prokaryotic cis-regulatory regions are usually highly complex. They frequently consist of both repetitive and overlapping transcription factor binding sites. To unravel the design principles of these promoter architectures, we have designed in silico prokaryotic transcriptional logic gates with predefined input–output relations using an evolutionary algorithm. The resulting cis-regulatory designs are often composed of modules that consist of tandem arrays of binding sites to which the transcription factors bind cooperatively. Moreover, these modules often overlap with each other, leading to competition between them. Our analysis thus identifies a new signal integration motif that is based upon the interplay between intramodular cooperativity and intermodular competition. We show that this signal integration mechanism drastically enhances the capacity of cis-regulatory domains to integrate signals. Our results provide a possible explanation for the complexity of promoter architectures and could be used for the rational design of synthetic gene circuits.
机译:基因调控网络是细胞计算的核心。在这些网络中,细胞内和细胞外信号通过转录因子整合,转录因子通过与DNA上的顺式调节区结合来控制转录单位的表达。真核和原核顺式调节区的设计通常高度复杂。它们通常由重复和重叠的转录因子结合位点组成。为了阐明这些启动子体系结构的设计原理,我们使用进化算法设计了具有预定义输入-输出关系的计算机原核转录逻辑门。所得的顺式调控设计通常由模块组成,该模块由转录位点协同结合的结合位点的串联阵列组成。而且,这些模块经常彼此重叠,导致它们之间的竞争。因此,我们的分析确定了一种新的信号积分模体,该模体是基于模块内协作性和模块间竞争之间的相互作用的。我们表明,这种信号整合机制极大地增强了顺式调节域整合信号的能力。我们的结果为启动子结构的复杂性提供了可能的解释,并可以用于合成基因电路的合理设计。

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