BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Lung cancer, Retina, Amniocentesis, Rapamycin, rs4950928, FXYD4, Apoptosis)
Bookmark Forward

Enumerating metabolic pathways for the production of heterologous target chemicals in chassis organisms.

Pablo Carbonell, Davide Fichera, Shashi B Pandit, Jean-Loup Faulon

iSSB, Institute of Systems and Synthetic Biology, University of Evry, Genopole Campus 1, Genavenir 6, 5 rue Henri Desbruères, 91030 EVRY Cedex, France.

BMC systems biology 2012


filter terms:
  • algorithms (1)
  • biosynthetic pathway (1)
  • engineering (3)
  • growth (1)
  • metabolic networks (2)
  • metabolic networks and pathways (5)
  • models biological (1)
    • Sizes of these terms reflect their relevance to your search.

    We consider the possibility of engineering metabolic pathways in a chassis organism in order to synthesize novel target compounds that are heterologous to the chassis. For this purpose, we model metabolic networks through hypergraphs where reactions are represented by hyperarcs. Each hyperarc represents an enzyme-catalyzed reaction that transforms set of substrates compounds into product compounds. We follow a retrosynthetic approach in order to search in the metabolic space (hypergraphs) for pathways (hyperpaths) linking the target compounds to a source set of compounds. To select the best pathways to engineer, we have developed an objective function that computes the cost of inserting a heterologous pathway in a given chassis organism. In order to find minimum-cost pathways, we propose in this paper two methods based on steady state analysis and network topology that are to the best of our knowledge, the first to enumerate all possible heterologous pathways linking a target compounds to a source set of compounds. In the context of metabolic engineering, the source set is composed of all naturally produced chassis compounds (endogenuous chassis metabolites) and the target set can be any compound of the chemical space. We also provide an algorithm for identifying precursors which can be supplied to the growth media in order to increase the number of ways to synthesize specific target compounds. We find the topological approach to be faster by several orders of magnitude than the steady state approach. Yet both methods are generally scalable in time with the number of pathways in the metabolic network. Therefore this work provides a powerful tool for pathway enumeration with direct application to biosynthetic pathway design.

    Citation

    Pablo Carbonell, Davide Fichera, Shashi B Pandit, Jean-Loup Faulon. Enumerating metabolic pathways for the production of heterologous target chemicals in chassis organisms. BMC systems biology. 2012;6:10

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 22309974

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.