The Journal of Clinical Investigation (Jun 2023)

POLQ inhibition elicits an immune response in homologous recombination–deficient pancreatic adenocarcinoma via cGAS/STING signaling

  • Grace Oh,
  • Annie Wang,
  • Lidong Wang,
  • Jiufeng Li,
  • Gregor Werba,
  • Daniel Weissinger,
  • Ende Zhao,
  • Surajit Dhara,
  • Rosmel E. Hernandez,
  • Amanda Ackermann,
  • Sarina Porcella,
  • Despoina Kalfakakou,
  • Igor Dolgalev,
  • Emily Kawaler,
  • Talia Golan,
  • Theodore H. Welling,
  • Agnel Sfeir,
  • Diane M. Simeone

Journal volume & issue
Vol. 133, no. 11

Abstract

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Pancreatic ductal adenocarcinoma (PDAC) is a highly lethal malignancy that harbors mutations in homologous recombination–repair (HR-repair) proteins in 20%–25% of cases. Defects in HR impart a specific vulnerability to poly ADP ribose polymerase inhibitors and platinum-containing chemotherapy in tumor cells. However, not all patients who receive these therapies respond, and many who initially respond ultimately develop resistance. Inactivation of the HR pathway is associated with the overexpression of polymerase theta (Polθ, or POLQ). This key enzyme regulates the microhomology-mediated end-joining (MMEJ) pathway of double-strand break (DSB) repair. Using human and murine HR-deficient PDAC models, we found that POLQ knockdown is synthetically lethal in combination with mutations in HR genes such as BRCA1 and BRCA2 and the DNA damage repair gene ATM. Further, POLQ knockdown enhances cytosolic micronuclei formation and activates signaling of cyclic GMP-AMP synthase–stimulator of interferon genes (cGAS-STING), leading to enhanced infiltration of activated CD8+ T cells in BRCA2-deficient PDAC tumors in vivo. Overall, POLQ, a key mediator in the MMEJ pathway, is critical for DSB repair in BRCA2-deficient PDAC. Its inhibition represents a synthetic lethal approach to blocking tumor growth while concurrently activating the cGAS-STING signaling pathway to enhance tumor immune infiltration, highlighting what we believe to be a new role for POLQ in the tumor immune environment.

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