Molecular Oncology (Jun 2024)

Transcriptome‐wide gene expression outlier analysis pinpoints therapeutic vulnerabilities in colorectal cancer

  • Elisa Mariella,
  • Gaia Grasso,
  • Martina Miotto,
  • Kristi Buzo,
  • Nicole Megan Reilly,
  • Pietro Andrei,
  • Pietro Paolo Vitiello,
  • Giovanni Crisafulli,
  • Sabrina Arena,
  • Giuseppe Rospo,
  • Giorgio Corti,
  • Annalisa Lorenzato,
  • Carlotta Cancelliere,
  • Ludovic Barault,
  • Giulia Gionfriddo,
  • Michael Linnebacher,
  • Mariangela Russo,
  • Federica Di Nicolantonio,
  • Alberto Bardelli

DOI
https://doi.org/10.1002/1878-0261.13622
Journal volume & issue
Vol. 18, no. 6
pp. 1460 – 1485

Abstract

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Multiple strategies are continuously being explored to expand the drug target repertoire in solid tumors. We devised a novel computational workflow for transcriptome‐wide gene expression outlier analysis that allows the systematic identification of both overexpression and underexpression events in cancer cells. Here, it was applied to expression values obtained through RNA sequencing in 226 colorectal cancer (CRC) cell lines that were also characterized by whole‐exome sequencing and microarray‐based DNA methylation profiling. We found cell models displaying an abnormally high or low expression level for 3533 and 965 genes, respectively. Gene expression abnormalities that have been previously associated with clinically relevant features of CRC cell lines were confirmed. Moreover, by integrating multi‐omics data, we identified both genetic and epigenetic alternations underlying outlier expression values. Importantly, our atlas of CRC gene expression outliers can guide the discovery of novel drug targets and biomarkers. As a proof of concept, we found that CRC cell lines lacking expression of the MTAP gene are sensitive to treatment with a PRMT5‐MTA inhibitor (MRTX1719). Finally, other tumor types may also benefit from this approach.

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