Mapping the landscape of genetic dependencies in chordoma

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作者
Tanaz Sharifnia
Mathias J. Wawer
Amy Goodale
Yenarae Lee
Mariya Kazachkova
Joshua M. Dempster
Sandrine Muller
Joan Levy
Daniel M. Freed
Josh Sommer
Jérémie Kalfon
Francisca Vazquez
William C. Hahn
David E. Root
Paul A. Clemons
Stuart L. Schreiber
机构
[1] Broad Institute of Harvard and MIT,
[2] Chordoma Foundation,undefined
[3] Dana-Farber Cancer Institute,undefined
[4] Harvard University,undefined
[5] Kojin Therapeutics,undefined
[6] University of California San Diego,undefined
[7] Melanoma Research Alliance,undefined
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摘要
Identifying the spectrum of genes required for cancer cell survival can reveal essential cancer circuitry and therapeutic targets, but such a map remains incomplete for many cancer types. We apply genome-scale CRISPR-Cas9 loss-of-function screens to map the landscape of selectively essential genes in chordoma, a bone cancer with few validated targets. This approach confirms a known chordoma dependency, TBXT (T; brachyury), and identifies a range of additional dependencies, including PTPN11, ADAR, PRKRA, LUC7L2, SRRM2, SLC2A1, SLC7A5, FANCM, and THAP1. CDK6, SOX9, and EGFR, genes previously implicated in chordoma biology, are also recovered. We find genomic and transcriptomic features that predict specific dependencies, including interferon-stimulated gene expression, which correlates with ADAR dependence and is elevated in chordoma. Validating the therapeutic relevance of dependencies, small-molecule inhibitors of SHP2, encoded by PTPN11, have potent preclinical efficacy against chordoma. Our results generate an emerging map of chordoma dependencies to enable biological and therapeutic hypotheses.
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