Inferring cancer dependencies on metabolic genes from large-scale genetic screens

Shoval Lagziel; Won Dong Lee; Tomer Shlomi

doi:10.1186/s12915-019-0654-4

BMC Biology (Apr 2019)

Inferring cancer dependencies on metabolic genes from large-scale genetic screens

Shoval Lagziel,
Won Dong Lee,
Tomer Shlomi

Affiliations

Shoval Lagziel: Faculty of Computer Science, Technion
Won Dong Lee: Faculty of Biology, Technion
Tomer Shlomi: Faculty of Computer Science, Technion

DOI: https://doi.org/10.1186/s12915-019-0654-4
Journal volume & issue: Vol. 17, no. 1
pp. 1 – 11

Abstract

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Abstract Background Cancer cells reprogram their metabolism to survive and propagate. Thus, targeting metabolic rewiring in tumors is a promising therapeutic strategy. Genome-wide RNAi and CRISPR screens are powerful tools for identifying genes essential for cancer cell proliferation and survival. Integrating loss-of-function genetic screens with genomics and transcriptomics datasets reveals molecular mechanisms that underlie cancer cell dependence on specific genes; though explaining cell line-specific essentiality of metabolic genes was recently shown to be especially challenging. Results We find that variability in tissue culture medium between cell lines in a genetic screen is a major confounding factor affecting cell line-specific essentiality of metabolic genes—while, quite surprisingly, not being previously accounted for. Additionally, we find that altered expression level of a metabolic gene in a certain cell line is less indicative of its essentiality than for other genes. However, cell line-specific essentiality of metabolic genes is significantly correlated with changes in the expression of neighboring enzymes in the metabolic network. Utilizing a machine learning method that accounts for tissue culture media and functional association between neighboring enzymes, we generated predictive models for cancer cell line-specific dependence on 162 metabolic genes (representing a ~ 2.2-fold increase compared to previous studies). The generated predictive models reveal numerous novel associations between molecular features and cell line-specific dependency on metabolic genes. Specifically, we demonstrate how cancer cell dependence on one-carbon metabolic enzymes is explained based on cancer lineage, oncogenic mutations, and RNA expression of neighboring enzymes. Conclusions Considering culture media as well as accounting for molecular features of functionally related metabolic enzymes in a metabolic network significantly improves our understanding of cancer cell line-specific dependence on metabolic genes. We expect our approach and predictive models of metabolic gene essentiality to be a useful tool for investigating metabolic abnormalities in cancer.

Published in BMC Biology

ISSN: 1741-7007 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Science: Biology (General)
Website: http://www.biomedcentral.com/bmcbiol/

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