Combining PARP with ATR inhibition overcomes PARP inhibitor and platinum resistance in ovarian cancer models

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作者
Hyoung Kim
Haineng Xu
Erin George
Dorothy Hallberg
Sushil Kumar
Veena Jagannathan
Sergey Medvedev
Yasuto Kinose
Kyle Devins
Priyanka Verma
Kevin Ly
Yifan Wang
Roger A. Greenberg
Lauren Schwartz
Neil Johnson
Robert B. Scharpf
Gordon B. Mills
Rugang Zhang
Victor E. Velculescu
Eric J. Brown
Fiona Simpkins
机构
[1] University of Pennsylvania,Penn Ovarian Cancer Research Center, Division of Gynecologic Oncology, Department of Obstetrics and Gynecology
[2] Johns Hopkins University School of Medicine,The Sidney Kimmel Comprehensive Cancer Center
[3] University of Pennsylvania,Department of Cancer Biology, Perelman School of Medicine
[4] University of Pennsylvania,Department of Pathology and Laboratory Medicine, Perelman School of Medicine
[5] Fox Chase Cancer Center,Molecular Therapeutics Program
[6] Oregon Health & Science University School of Medicine,Department of Cell, Developmental and Cancer Biology
[7] The Wistar Institute,Gene Expression and Regulation Program
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摘要
Ovarian cancer (OVCA) inevitably acquires resistance to platinum chemotherapy and PARP inhibitors (PARPi). We show that acquisition of PARPi-resistance is accompanied by increased ATR-CHK1 activity and sensitivity to ATR inhibition (ATRi). However, PARPi-resistant cells are remarkably more sensitive to ATRi when combined with PARPi (PARPi-ATRi). Sensitivity to PARPi-ATRi in diverse PARPi and platinum-resistant models, including BRCA1/2 reversion and CCNE1-amplified models, correlate with synergistic increases in replication fork stalling, double-strand breaks, and apoptosis. Surprisingly, BRCA reversion mutations and an ability to form RAD51 foci are frequently not observed in models of acquired PARPi-resistance, suggesting the existence of alternative resistance mechanisms. However, regardless of the mechanisms of resistance, complete and durable therapeutic responses to PARPi-ATRi that significantly increase survival are observed in clinically relevant platinum and acquired PARPi-resistant patient-derived xenografts (PDXs) models. These findings indicate that PARPi-ATRi is a highly promising strategy for OVCAs that acquire resistance to PARPi and platinum.
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