2 research outputs found
Feedbacks from the metabolic network to the genetic network reveal regulatory modules in E. coli and B. subtilis
The genetic regulatory network (GRN) plays a key role in controlling the
response of the cell to changes in the environment. Although the structure of
GRNs has been the subject of many studies, their large scale structure in the
light of feedbacks from the metabolic network (MN) has received relatively
little attention. Here we study the causal structure of the GRNs, namely the
chain of influence of one component on the other, taking into account feedback
from the MN. First we consider the GRNs of E. coli and B. subtilis without
feedback from MN and illustrate their causal structure. Next we augment the
GRNs with feedback from their respective MNs by including (a) links from genes
coding for enzymes to metabolites produced or consumed in reactions catalyzed
by those enzymes and (b) links from metabolites to genes coding for
transcription factors whose transcriptional activity the metabolites alter by
binding to them. We find that the inclusion of feedback from MN into GRN
significantly affects its causal structure, in particular the number of levels
and relative positions of nodes in the hierarchy, and the number and size of
the strongly connected components (SCCs). We then study the functional
significance of the SCCs. For this we identify condition specific feedbacks
from the MN into the GRN by retaining only those enzymes that are essential for
growth in specific environmental conditions simulated via the technique of flux
balance analysis (FBA). We find that the SCCs of the GRN augmented by these
feedbacks can be ascribed specific functional roles in the organism. Our
algorithmic approach thus reveals relatively autonomous subsystems with
specific functionality, or regulatory modules in the organism. This automated
approach could be useful in identifying biologically relevant modules in other
organisms for which network data is available, but whose biology is less well
studied.Comment: 15 figure
Analysis of the hierarchical structure of the B. subtilis transcriptional regulatory network.
The transcriptional regulation of gene expression is orchestrated by complex networks of interacting genes. Increasing evidence indicates that these 'transcriptional regulatory networks' (TRNs) in bacteria have an inherently hierarchical architecture, although the design principles and the specific advantages offered by this type of organization have not yet been fully elucidated. In this study, we focussed on the hierarchical structure of the TRN of the gram-positive bacterium Bacillus subtilis and performed a comparative analysis with the TRN of the gram-negative bacterium Escherichia coli. Using a graph-theoretic approach, we organized the transcription factors (TFs) and σ-factors in the TRNs of B. subtilis and E. coli into three hierarchical levels (Top, Middle and Bottom) and studied several structural and functional properties across them. In addition to many similarities, we found also specific differences, explaining the majority of them with variations in the distribution of σ-factors across the hierarchical levels in the two organisms. We then investigated the control of target metabolic genes by transcriptional regulators to characterize the differential regulation of three distinct metabolic subsystems (catabolism, anabolism and central energy metabolism). These results suggest that the hierarchical architecture that we observed in B. subtilis represents an effective organization of its TRN to achieve flexibility in response to a wide range of diverse stimuli.SK acknowledges The Institute of Mathematical Sciences for hospitality, University Grants Commission (UGC) India for Senior Research Fellowship, and University of Delhi grant DRCH/R&D/2013–2014/4155 for infrastructural support.This is the author accepted manuscript. The final version is available from the Royal Society of Chemistry via http://dx.doi.org/10.1039/C4MB00298