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Interplay between network structures regulatory modes and sensing mechanisms of transcription factors in the transcriptional regulatory network of E. coli

机译:大肠杆菌转录调控网络中转录因子的网络结构调控模式和传感机制之间的相互作用

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摘要

Though the bacterial transcription regulation apparatus is distinct in terms of several structural and functional features from its eukaryotic counterpart, the gross structure of the transcription regulatory network (TRN) is believed to be similar in both superkingdoms. Here, we explore the fine structure of the bacterial TRN and the underlying “co-regulatory network (CRN)” to show that despite the superficial similarities to eukaryotic networks, the bacterial networks display entirely different organizational principles. In particular unlike in eukaryotes, the hubs of bacterial networks are both global regulators and integrators of diverse disparate transcriptional responses. These and other organizational differences might correlate with the fundamental differences in gene and promoter organization in the two superkingdoms, especially the presence of operons and regulons in bacteria. Further we explored to find the interplay, if any, between network structures, mode of regulatory interactions and signal sensing of TFs in shaping up the bacterial transcriptional regulatory responses. For this purpose, we first classified TFs according to their regulatory mode (activator, repressor or dual regulator) and sensory mechanism (one-component systems responding to internal or external signals, TFs from 2-component systems and chromosomal structure modifying TFs) in the bacterial model organism E. coli and then we studied the overall evolutionary optimization of network structures. The incorporation of TFs in different hierarchical elements of the TRN appears to involve on a multi-dimensional selection process depending on regulatory and sensory modes of TFs in motifs, co-regulatory associations between TFs of different functional classes and transcript half-lives. As result it appears to have generated circuits that allow intricately regulated physiological state changes. We identified the biological significance of most of these optimizations, which can be further used as the basis to explore similar controls in other bacteria. We also show that, though on the larger evolutionary scale, unrelated TFs have evolved to become hubs, within lineages like γ-proteobacteria there is strong tendency to retain hubs, as well as certain higher-order network modules that have emerged through lineage specific paralog duplications.
机译:尽管细菌转录调控装置在几个结构和功能特征方面不同于其真核对应物,但据信在两个超级王国中,转录调控网络(TRN)的总体结构都相似。在这里,我们研究了细菌TRN的精细结构和潜在的“共调节网络(CRN)”,以表明尽管与真核细胞表面上相似,但是细菌网络显示出完全不同的组织原理。特别是与真核生物不同,细菌网络的中心既是全局的调节子,也是各种不同的转录反应的整合者。这些和其他组织上的差异可能与两个超级王国中基因和启动子组织上的根本差异有关,尤其是细菌中操纵子和调节子的存在。进一步,我们探索发现网络结构,调节相互作用的模式和TFs的信号感应在形成细菌转录调节反应之间的相互作用,如果有的话。为此,我们首先根据TF的调节模式(激活剂,阻遏物或双重调节剂)和感觉机制(响应内部或外部信号的单组分系统,来自2组分系统的TF和修饰TF的染色体结构)对TF进行分类。细菌模型生物大肠杆菌,然后我们研究了网络结构的整体进化优化。 TFs在TRN的不同层次元素中的结合似乎涉及多维选择过程,这取决于TFs在基序中的调节和感觉方式,不同功能类别的TFs之间的共调节关联和转录物半衰期。结果,似乎产生了允许复杂调节的生理状态变化的电路。我们确定了大多数这些优化方法的生物学意义,可以进一步用作探索其他细菌中类似对照的基础。我们还显示,尽管在更大的进化规模上,不相关的TF已进化成为集线器,在诸如γ-变形杆菌之类的谱系中,强烈保留集线器的趋势以及通过谱系特定的旁系同源物出现的某些更高阶的网络模块重复。

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  • 年(卷),期 -1(372),4
  • 年度 -1
  • 页码 1108–1122
  • 总页数 23
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