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A comprehensive clinically informed map of dependencies in cancer cells and framework for target prioritization

Autori:

  • C. Pacini, E. Duncan, E. Gonçalves, J. Gilbert, S. Bhosle, S. Horswell, E. Karakoc, H. Lightfoot, E. Curry, F. Muyas, M. Bouaboula, C. S. Pedamallu, I. Cortes-Ciriano, F. M. Behan, L. Zalmas, A. Barthorpe, H. Francies, S. Rowley, J. Pollard, P. Beltrao, L. Parts,
  • Iorio F.,
  • M. J. Garnett

Sommario:

Genetic screens in cancer cell lines inform gene function and drug discovery. More comprehensive screen datasets with multi-omics data are needed to enhance opportunities to functionally map genetic vulnerabilities. Here, we construct a second-generation map of cancer dependencies by annotating 930 cancer cell lines with multi-omic data and analyze relationships between molecular markers and cancer dependencies derived from CRISPR-Cas9 screens. We identify dependency-associated gene expression markers beyond driver genes, and observe many gene addiction relationships driven by gain of function rather than synthetic lethal effects. By combining clinically informed dependency-marker associations with protein-protein interaction networks, we identify 370 anti-cancer priority targets for 27 cancer types, many of which have network-based evidence of a functional link with a marker in a cancer type. Mapping these targets to sequenced tumor cohorts identifies tractable targets in different cancer types. This target prioritization map enhances understanding of gene dependencies and identifies candidate anti-cancer targets for drug development.

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