Premature mitotic entry induced by ATR inhibition potentiates olaparib inhibition‐mediated genomic instability, inflammatory signaling, and cytotoxicity in BRCA2‐deficient cancer cells

Pepijn M. Schoonen; Yannick P. Kok; Elles Wierenga; Bjorn Bakker; Floris Foijer; Diana C. J. Spierings; Marcel A. T. M. vanVugt

doi:10.1002/1878-0261.12573

Molecular Oncology (Nov 2019)

Premature mitotic entry induced by ATR inhibition potentiates olaparib inhibition‐mediated genomic instability, inflammatory signaling, and cytotoxicity in BRCA2‐deficient cancer cells

Pepijn M. Schoonen,
Yannick P. Kok,
Elles Wierenga,
Bjorn Bakker,
Floris Foijer,
Diana C. J. Spierings,
Marcel A. T. M. vanVugt

Affiliations

Pepijn M. Schoonen: Department of Medical Oncology University Medical Center Groningen University of Groningen The Netherlands
Yannick P. Kok: Department of Medical Oncology University Medical Center Groningen University of Groningen The Netherlands
Elles Wierenga: Department of Medical Oncology University Medical Center Groningen University of Groningen The Netherlands
Bjorn Bakker: European Institute for the Biology of Ageing (ERIBA) University Medical Center Groningen University of Groningen The Netherlands
Floris Foijer: European Institute for the Biology of Ageing (ERIBA) University Medical Center Groningen University of Groningen The Netherlands
Diana C. J. Spierings: European Institute for the Biology of Ageing (ERIBA) University Medical Center Groningen University of Groningen The Netherlands
Marcel A. T. M. vanVugt: Department of Medical Oncology University Medical Center Groningen University of Groningen The Netherlands

DOI: https://doi.org/10.1002/1878-0261.12573
Journal volume & issue: Vol. 13, no. 11
pp. 2422 – 2440

Abstract

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Poly(ADP‐ribose) polymerase (PARP) inhibitors are selectively cytotoxic in cancer cells with defects in homologous recombination (HR) (e.g., due to BRCA1/2 mutations). However, not all HR‐deficient tumors efficiently respond to PARP inhibition and often acquire resistance. It is therefore important to uncover how PARP inhibitors induce cytotoxicity and develop combination strategies to potentiate PARP inhibitor efficacy in HR‐deficient tumors. In this study, we found that forced mitotic entry upon ATR inhibition potentiates cytotoxic effects of PARP inhibition using olaparib in BRCA2‐depleted and Brca2 knockout cancer cell line models. Single DNA fiber analysis showed that ATR inhibition does not exacerbate replication fork degradation. Instead, we find ATR inhibitors accelerate mitotic entry, resulting in the formation of chromatin bridges and lagging chromosomes. Furthermore, using genome‐wide single‐cell sequencing, we show that ATR inhibition enhances genomic instability of olaparib‐treated BRCA2‐depleted cells. Inhibition of CDK1 to delay mitotic entry mitigated mitotic aberrancies and genomic instability upon ATR inhibition, underscoring the role of ATR in coordinating proper cell cycle timing in situations of DNA damage. Additionally, we show that olaparib treatment leads to increased numbers of micronuclei, which is accompanied by a cGAS/STING‐associated inflammatory response in BRCA2‐deficient cells. ATR inhibition further increased the numbers of cGAS‐positive micronuclei and the extent of cytokine production in olaparib‐treated BRCA2‐deficient cancer cells. Altogether, we show that ATR inhibition induces premature mitotic entry and mediates synergistic cytotoxicity with PARP inhibition in HR‐deficient cancer cells, which involves enhanced genomic instability and inflammatory signaling.

Published in Molecular Oncology

ISSN: 1574-7891 (Print); 1878-0261 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://febs.onlinelibrary.wiley.com/journal/18780261

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