Phenotype-based cell-specific metabolic modeling reveals metabolic liabilities of cancer

Keren Yizhak; Edoardo Gaude; Sylvia Le Dévédec; Yedael Y Waldman; Gideon Y Stein; Bob van de Water; Christian Frezza; Eytan Ruppin

doi:10.7554/eLife.03641

eLife (Nov 2014)

Phenotype-based cell-specific metabolic modeling reveals metabolic liabilities of cancer

Keren Yizhak,
Edoardo Gaude,
Sylvia Le Dévédec,
Yedael Y Waldman,
Gideon Y Stein,
Bob van de Water,
Christian Frezza,
Eytan Ruppin

Affiliations

Keren Yizhak: Blavatnik School of Computer Science, Tel-Aviv University, Tel-Aviv, Israel
Edoardo Gaude: MRC Cancer Unit, University of Cambridge, Cambridge, United Kingdom
Sylvia Le Dévédec: Division of Toxicology, Leiden Academic Center for Drug Research, Leiden University, Leiden, Netherlands
Yedael Y Waldman: Blavatnik School of Computer Science, Tel-Aviv University, Tel-Aviv, Israel
Gideon Y Stein: Department of Internal Medicine ‘B’, Beilinson Hospital, Rabin Medical Center, Petah-Tikva, Israel; Sackler School of Medicine, Tel Aviv University, Tel-Aviv, Israel
Bob van de Water: Division of Toxicology, Leiden Academic Center for Drug Research, Leiden University, Leiden, Netherlands
Christian Frezza: MRC Cancer Unit, University of Cambridge, Cambridge, United Kingdom
Eytan Ruppin: Blavatnik School of Computer Science, Tel-Aviv University, Tel-Aviv, Israel; Sackler School of Medicine, Tel Aviv University, Tel-Aviv, Israel

DOI: https://doi.org/10.7554/eLife.03641
Journal volume & issue: Vol. 3

Abstract

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Utilizing molecular data to derive functional physiological models tailored for specific cancer cells can facilitate the use of individually tailored therapies. To this end we present an approach termed PRIME for generating cell-specific genome-scale metabolic models (GSMMs) based on molecular and phenotypic data. We build >280 models of normal and cancer cell-lines that successfully predict metabolic phenotypes in an individual manner. We utilize this set of cell-specific models to predict drug targets that selectively inhibit cancerous but not normal cell proliferation. The top predicted target, MLYCD, is experimentally validated and the metabolic effects of MLYCD depletion investigated. Furthermore, we tested cell-specific predicted responses to the inhibition of metabolic enzymes, and successfully inferred the prognosis of cancer patients based on their PRIME-derived individual GSMMs. These results lay a computational basis and a counterpart experimental proof of concept for future personalized metabolic modeling applications, enhancing the search for novel selective anticancer therapies.

Published in eLife

ISSN: 2050-084X (Online)
Publisher: eLife Sciences Publications Ltd
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Biology (General)
Website: https://elifesciences.org

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