| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2107042 | Cancer Cell | 2015 | 15 Pages |
•Driver genes are comprehensively identified across a large pan-cancer cohort•In silico prescription links approved or experimental targeted therapies to patients•Up to 73.3% of patients could benefit from agents in clinical stages•80 therapeutically unexploited targetable cancer driver genes are identified
SummaryLarge efforts dedicated to detect somatic alterations across tumor genomes/exomes are expected to produce significant improvements in precision cancer medicine. However, high inter-tumor heterogeneity is a major obstacle to developing and applying therapeutic targeted agents to treat most cancer patients. Here, we offer a comprehensive assessment of the scope of targeted therapeutic agents in a large pan-cancer cohort. We developed an in silico prescription strategy based on identification of the driver alterations in each tumor and their druggability options. Although relatively few tumors are tractable by approved agents following clinical guidelines (5.9%), up to 40.2% could benefit from different repurposing options, and up to 73.3% considering treatments currently under clinical investigation. We also identified 80 therapeutically targetable cancer genes.
Graphical AbstractFigure optionsDownload full-size imageDownload high-quality image (158 K)Download as PowerPoint slide
