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The complexity of cellular gene, protein, and metabolite networks can hinder attempts to elucidate their structure and function. To address this problem, we used systematic transcriptional perturbations to construct a first-order model of regulatory interactions in a nine-gene subnetwork of the SOS pathway in Escherichia coli. The model correctly identified the major regulatory genes and the transcriptional targets of mitomycin C activity in the subnetwork. This approach, which is experimentally and computationally scalable, provides a framework for elucidating the functional properties of genetic networks and identifying molecular targets of pharmacological compounds.
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Timothy S. Gardner
Boston University
Diego di Bernardo
Telethon Institute Of Genetics And Medicine
David R. Lorenz
Harvard University
Science
Telethon Institute Of Genetics And Medicine
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Gardner et al. (Thu,) studied this question.
synapsesocial.com/papers/6a08e3efafc616802fe4b348 — DOI: https://doi.org/10.1126/science.1081900