JCI Insight (Aug 2022)

Axon guidance receptor ROBO3 modulates subtype identity and prognosis via AXL-associated inflammatory network in pancreatic cancer

  • Niklas Krebs,
  • Lukas Klein,
  • Florian Wegwitz,
  • Elisa Espinet,
  • Hans Carlo Maurer,
  • Mengyu Tu,
  • Frederike Penz,
  • Stefan Küffer,
  • Xingbo Xu,
  • Hanibal Bohnenberger,
  • Silke Cameron,
  • Marius Brunner,
  • Albrecht Neesse,
  • Uday Kishore,
  • Elisabeth Hessmann,
  • Andreas Trumpp,
  • Philipp Ströbel,
  • Rolf A. Brekken,
  • Volker Ellenrieder,
  • Shiv K. Singh

Journal volume & issue
Vol. 7, no. 16

Abstract

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Metastatic pancreatic cancer (PDAC) has a poor clinical outcome with a 5-year survival rate below 3%. Recent transcriptome profiling of PDAC biopsies has identified 2 clinically distinct subtypes — the “basal-like” (BL) subtype with poor prognosis and therapy resistance compared with the less aggressive and drug-susceptible “classical” (CLA) subtype. However, the mechanistic events and environmental factors that promote the BL subtype identity are not very clear. Using preclinical models, patient-derived xenografts, and FACS-sorted PDAC patient biopsies, we report here that the axon guidance receptor, roundabout guidance receptor 3 (ROBO3), promotes the BL metastatic program via a potentially unique AXL/IL-6/phosphorylated STAT3 (p-STAT3) regulatory axis. RNA-Seq identified a ROBO3-mediated BL-specific gene program, while tyrosine kinase profiling revealed AXL as the key mediator of the p-STAT3 activation. CRISPR/dCas9-based ROBO3 silencing disrupted the AXL/p-STAT3 signaling axis, thereby halting metastasis and enhancing therapy sensitivity. Transcriptome analysis of resected patient tumors revealed that AXLhi neoplastic cells associated with the inflammatory stromal program. Combining AXL inhibitor and chemotherapy substantially restored a CLA phenotypic state and reduced disease aggressiveness. Thus, we conclude that a ROBO3-driven hierarchical network determines the inflammatory and prometastatic programs in a specific PDAC subtype.

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