Network motifs in the transcriptional regulation network of Escherichia coli

Shen-Orr, Shai S.; Milo, Ron; Mangan, Shmuel; Alon, Uri

doi:10.1038/ng881

Cited by 2,669 publications

(2,632 citation statements)

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“…A number of topological features are common to the gene regulatory networks in E. coli and yeast 2,3 . A key common feature is that the number of target genes per transcription factor roughly obeys a power law, which is typical of 'scale-free' networks 19 (Fig.…”

Section: All Interactions 1409 906mentioning

confidence: 99%

“…These are sets of interactions connected in specific patterns called 'network motifs' 1,2,20 . These motifs have been engineered artificially 21,22 , but here we addressed how they were formed during evolution.…”

Section: All Interactions 1409 906mentioning

confidence: 99%

“…2a), or it may recognize a new binding site upstream of some other target gene(s). Investigation of the known network in both organisms 2,3,7 showed that duplication of transcription factor genes followed by inheritance of interaction has contributed considerably to the growth of the regulatory network: more than two-thirds of E. coli (77%) and yeast (69%) transcription factors have at least one interaction in common with their duplicates (Table 1). This accounts for 128 interactions (10%) in E. coli and 188 interactions (22%) in yeast ( Fig.…”

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Gene regulatory network growth by duplication

2004

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We are beginning to elucidate transcriptional regulatory networks on a large scale 1 and to understand some of the structural principles of these networks 2,3 , but the evolutionary mechanisms that form these networks are still mostly unknown. Here we investigate the role of gene duplication in network evolution. Gene duplication is the driving force for creating new genes in genomes: at least 50% of prokaryotic genes 4,5 and over 90% of eukaryotic genes 6 are products of gene duplication. The transcriptional interactions in regulatory networks consist of multiple components, and duplication processes that generate new interactions would need to be more complex. We define possible duplication scenarios and show that they formed the regulatory networks of the prokaryote Escherichia coli and the eukaryote Saccharomyces cerevisiae. Gene duplication has had a key role in network evolution: more than one-third of known regulatory interactions were inherited from the ancestral transcription factor or target gene after duplication, and roughly one-half of the interactions were gained during divergence after duplication. In addition, we conclude that evolution has been incremental, rather than making entire regulatory circuits or motifs by duplication with inheritance of interactions.

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Section: All Interactions 1409 906mentioning

confidence: 99%

Section: All Interactions 1409 906mentioning

confidence: 99%

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confidence: 99%

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Gene regulatory network growth by duplication

2004

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“…The genes encoding these enzymes are governed by a transcriptional regulatory network 12,13 , which is an excellent model system for studying the design principles of metabolic regulation. To study the dynamics of transcription of AAB genes at high temporal resolution and accuracy, we constructed a library of 52 reporter strains that represent ∼50% of known AAB genes.…”

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Just-in-time transcription program in metabolic pathways

et al. 2004

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A primary goal of systems biology is to understand the design principles of the transcription networks that govern the timing of gene expression 1-5 . Here we measured promoter activity for ∼100 genes in parallel from living cells at a resolution of minutes and accuracy of 10%, based on GFP and Lux reporter libraries 3 . Focusing on the amino-acid biosynthesis systems of Escherichia coli 4 , we identified a previously unknown temporal expression program and expression hierarchy that matches the enzyme order in unbranched pathways. We identified two design principles: the closer the enzyme is to the beginning of the pathway, the shorter the response time of the activation of its promoter and the higher its maximal promoter activity. Mathematical analysis suggests that this 'just-in-time' (ref. 5) transcription program is optimal under constraints of rapidly reaching a production goal with minimal total enzyme production 6,7 . Our findings suggest that metabolic regulation networks are designed to generate precision promoter timing and activity programs that can be understood using the engineering principles of production pipelines.Amino-acid biosynthesis (AAB) in E. coli is carried out by well-characterized enzymatic pathways 4,6-11 . The genes encoding these enzymes are governed by a transcriptional regulatory network 12,13 , which is an excellent model system for studying the design principles of metabolic regulation. To study the dynamics of transcription of AAB genes at high temporal resolution and accuracy, we constructed a library of 52 reporter strains that represent ∼50% of known AAB genes. We designed each reporter strain by cloning one of the promoter regions of E. coli K-12 MG1655 upstream of a Lux or a fast-folding GFP reporter gene (Fig. 1a). We measured promoter activity with a high temporal resolution by measuring fluorescence, luminescence and absorbance from 96 cultures in parallel in a multiwell fluorimeter 3,14 .

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“…Various types of network motifs significantly enriched as compared to randomized networks were revealed by the study of transcription regulatory network of E.coli : feed-forward loops (FFL), single-input modules (SIM), dense overlapping regulons (DOR) [63]. The ERGM modelling of networks offers a natural way of assessing importance of the network motifs.…”

Section: Resultsmentioning

confidence: 99%

Bayesian statistical modelling of human protein interaction network incorporating protein disorder information

Bulashevska

Eils

2010

BMC Bioinformatics

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BackgroundWe present a statistical method of analysis of biological networks based on the exponential random graph model, namely p2-model, as opposed to previous descriptive approaches. The model is capable to capture generic and structural properties of a network as emergent from local interdependencies and uses a limited number of parameters. Here, we consider one global parameter capturing the density of edges in the network, and local parameters representing each node's contribution to the formation of edges in the network. The modelling suggests a novel definition of important nodes in the network, namely social, as revealed based on the local sociality parameters of the model. Moreover, the sociality parameters help to reveal organizational principles of the network. An inherent advantage of our approach is the possibility of hypotheses testing: a priori knowledge about biological properties of the nodes can be incorporated into the statistical model to investigate its influence on the structure of the network.ResultsWe applied the statistical modelling to the human protein interaction network obtained with Y2H experiments. Bayesian approach for the estimation of the parameters was employed. We deduced social proteins, essential for the formation of the network, while incorporating into the model information on protein disorder. Intrinsically disordered are proteins which lack a well-defined three-dimensional structure under physiological conditions. We predicted the fold group (ordered or disordered) of proteins in the network from their primary sequences. The network analysis indicated that protein disorder has a positive effect on the connectivity of proteins in the network, but do not fully explains the interactivity.ConclusionsThe approach opens a perspective to study effects of biological properties of individual entities on the structure of biological networks.

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Network motifs in the transcriptional regulation network of Escherichia coli

Cited by 2,669 publications

References 19 publications

Gene regulatory network growth by duplication

Gene regulatory network growth by duplication

Just-in-time transcription program in metabolic pathways

Bayesian statistical modelling of human protein interaction network incorporating protein disorder information

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