Talazoparib Is a Potent Radiosensitizer in Small Cell Lung Cancer Cell Lines and Xenografts

Small cell lung cancer (SCLC) is an aggressive malignancy with a critical need for novel therapies. Our goal was to determine whether PARP inhibition could sensitize SCLC cells to ionizing radiation (IR) and if so, to determine the contribution of PARP trapping to radiosensitization. Short-term viab...

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Published inClinical cancer research Vol. 24; no. 20; pp. 5143 - 5152
Main Authors Laird, James H, Lok, Benjamin H, Ma, Jennifer, Bell, Andrew, de Stanchina, Elisa, Poirier, John T, Rudin, Charles M
Format Journal Article
LanguageEnglish
Published United States 15.10.2018
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Summary:Small cell lung cancer (SCLC) is an aggressive malignancy with a critical need for novel therapies. Our goal was to determine whether PARP inhibition could sensitize SCLC cells to ionizing radiation (IR) and if so, to determine the contribution of PARP trapping to radiosensitization. Short-term viability assays and clonogenic survival assays (CSA) were used to assess radiosensitization in 6 SCLC cell lines. Doses of veliparib and talazoparib with equivalent enzymatic inhibitory activity but differing PARP trapping activity were identified and compared in CSAs. Talazoparib, IR, and their combination were tested in three patient-derived xenograft (PDX) models. Talazoparib radiosensitized 5 of 6 SCLC cell lines in short-term viability assays and confirmed in 3 of 3 cell lines by CSAs. Concentrations of 200 nmol/L talazoparib and 1,600 nmol/L veliparib similarly inhibited PAR polymerization; however, talazoparib exhibited greater PARP trapping activity that was associated with superior radiosensitization. This observation further correlated with an increased number of double-stranded DNA breaks induced by talazoparib as compared with veliparib. Finally, a dose of 0.2 mg/kg talazoparib caused tumor growth inhibition in combination with IR but not as a single agent in 3 SCLC PDX models. PARP inhibition effectively sensitizes SCLC cell lines and PDXs to IR, and PARP trapping activity enhances this effect. PARP inhibitors, especially those with high PARP trapping activity, may provide a powerful tool to improve the efficacy of radiotherapy in SCLC. .
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Development of Methodology: J.H. Laird, B.H. Lok, J.T. Poirier, C.M. Rudin
Acquisition of Data: J.H. Laird, B.H. Lok, J. Ma, A. Bell, E. de Stanchina, J.T. Poirier
Study Supervision: J.T. Poirier, C.M. Rudin
These authors jointly supervised this work
Equal contributions
Writing, Review, or Revision of the Manuscript: J.H. Laird, B.H. Lok, J. Ma, A. Bell, E. de Stanchina, J.T. Poirier, C.M. Rudin
Administrative, Technical, or Material Support: J.T. Poirier
Current address: Radiation Medicine Program, Princess Margaret Cancer Centre/University Health Network, Toronto, Canada.
Author Contributions
Conception and Design: J.H. Laird, B.H. Lok, J.T. Poirier, C.M. Rudin
ISSN:1078-0432
1557-3265
DOI:10.1158/1078-0432.CCR-18-0401