Cell Reports (Jun 2016)

In Vivo Functional Platform Targeting Patient-Derived Xenografts Identifies WDR5-Myc Association as a Critical Determinant of Pancreatic Cancer

  • Alessandro Carugo,
  • Giannicola Genovese,
  • Sahil Seth,
  • Luigi Nezi,
  • Johnathon Lynn Rose,
  • Daniela Bossi,
  • Angelo Cicalese,
  • Parantu Krushnakant Shah,
  • Andrea Viale,
  • Piergiorgio Francesco Pettazzoni,
  • Kadir Caner Akdemir,
  • Christopher Aaron Bristow,
  • Frederick Scott Robinson,
  • James Tepper,
  • Nora Sanchez,
  • Sonal Gupta,
  • Marcos Roberto Estecio,
  • Virginia Giuliani,
  • Gaetano Ivan Dellino,
  • Laura Riva,
  • Wantong Yao,
  • Maria Emilia Di Francesco,
  • Tessa Green,
  • Carolina D’Alesio,
  • Denise Corti,
  • Ya’an Kang,
  • Philip Jones,
  • Huamin Wang,
  • Jason Bates Fleming,
  • Anirban Maitra,
  • Pier Giuseppe Pelicci,
  • Lynda Chin,
  • Ronald Anthony DePinho,
  • Luisa Lanfrancone,
  • Timothy Paul Heffernan,
  • Giulio Francesco Draetta

DOI
https://doi.org/10.1016/j.celrep.2016.05.063
Journal volume & issue
Vol. 16, no. 1
pp. 133 – 147

Abstract

Read online

Current treatment regimens for pancreatic ductal adenocarcinoma (PDAC) yield poor 5-year survival, emphasizing the critical need to identify druggable targets essential for PDAC maintenance. We developed an unbiased and in vivo target discovery approach to identify molecular vulnerabilities in low-passage and patient-derived PDAC xenografts or genetically engineered mouse model-derived allografts. Focusing on epigenetic regulators, we identified WDR5, a core member of the COMPASS histone H3 Lys4 (H3K4) MLL (1–4) methyltransferase complex, as a top tumor maintenance hit required across multiple human and mouse tumors. Mechanistically, WDR5 functions to sustain proper execution of DNA replication in PDAC cells, as previously suggested by replication stress studies involving MLL1, and c-Myc, also found to interact with WDR5. We indeed demonstrate that interaction with c-Myc is critical for this function. By showing that ATR inhibition mimicked the effects of WDR5 suppression, these data provide rationale to test ATR and WDR5 inhibitors for activity in this disease.