4.8 Article

Genome-Scale Architecture of Small Molecule Regulatory Networks and the Fundamental Trade-Off between Regulation and Enzymatic Activity

Journal

CELL REPORTS
Volume 20, Issue 11, Pages 2666-2677

Publisher

CELL PRESS
DOI: 10.1016/j.celrep.2017.08.066

Keywords

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Funding

  1. Swiss Initiative in Systems Biology (SystemsX.ch) TPdF fellowship [2014-230]
  2. Swiss Initiative in Systems Biology (SystemsX.ch) IPhD fellowship
  3. Boston University Undergraduate Research Opportunities Program (UROP)
  4. DOE [DE-SC0012627]
  5. MURI [W911NF-12-1-0390]
  6. NIH [R01GM121950]
  7. NSFOCE-BSF grant [1635070]
  8. The Human Frontier Science Program [RGP0020/2016]
  9. Sidney Kimmel Center for Prostate and Urologic Cancers
  10. Marie-Josee and Henry R. Kravis Center for Molecular Oncology
  11. MSK Cancer Center [P30 CA008748]
  12. U.S. Department of Energy (DOE) [DE-SC0012627] Funding Source: U.S. Department of Energy (DOE)

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Metabolic flux is in part regulated by endogenous small molecules that modulate the catalytic activity of an enzyme, e.g., allosteric inhibition. In contrast to transcriptional regulation of enzymes, technical limitations have hindered the production of a genome-scale atlas of small molecule-enzyme regulatory interactions. Here, we develop a framework leveraging the vast, but fragmented, biochemical literature to reconstruct and analyze the small molecule regulatory network (SMRN) of the model organism Escherichia coli, including the primary metabolite regulators and enzyme targets. Using metabolic control analysis, we prove a fundamental trade-off between regulation and enzymatic activity, and we combine it with metabolomic measurements and the SMRN to make inferences on the sensitivity of enzymes to their regulators. Generalizing the analysis to other organisms, we identify highly conserved regulatory interactions across evolutionarily divergent species, further emphasizing a critical role for small molecule interactions in the maintenance of metabolic homeostasis.

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