Combined PARP and ATR inhibition potentiates genome instability and cell death in ATM-deficient cancer cells

Lloyd, Rebecca L.; Wijnhoven, Paul W.G.; Ramos-Montoya, Antonio; Wilson, Zena; Illuzzi, Giuditta; Falenta, Katarzyna; Jones, Gemma N.; James, Neil H.; Chabbert, Christophe D.; Stott, Jonathan; Dean, Emma; Lau, Alan; Young, Lucy A.

doi:10.1038/s41388-020-1328-y

Cited by 127 publications

(144 citation statements)

References 64 publications

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“…Recent in vitro study on PARPi-resistant OvC cell lines from Burgess et al [207] confirms these results with ATR inhibitor VE-821, making treatment with ATRi a new promising approach to overcome PARPi-resistance in HR-deficient OvC. ATR inhibitor AZD6738 in combination with PARPi has revealed higher efficiency than PARPi alone [208,209]. Olaparib-approved by FDA and EMA for use in OvC therapy [144] Rucaparib-approved by FDA and EMA for use in OvC therapy [144] Niraparib-approved by FDA and EMA for use in OvC therapy [144] Veliparib-advanced clinical trials in combination with carboplatin and paclitaxel.…”

Section: Therapeutic Perspectives-targeting Of Dna Repair System In Omentioning

confidence: 86%

“…The CHEK1i V158411, PF-477736 and AZD7762 inhibited the proliferation of OvC cells [202] AZD7762 in combination with cisplatin suggested synergistic effects in ovarian clear cell carcinoma cell lines in vitro and suppressed growth of tumors in vivo [203] Prexasertib-effective in monotherapy in PARPi-resistant HGSOC cell lines and mouse xenografts [204] Combination of prexasertib mesylate monohydrate (LY2606368), a CHEK1 and CHEK2 inhibitor, and a PARPi, olaparib synergistically decreased cell viability in HGSOC cell lines (OVCAR3, OV90, PEO1 and PEO4) cell lines and induced greater DNA damage and apoptosis than the control and/or monotherapies [204,211] Prexasertib-effective in clinical phase II study in recurrent HGSOC [201] ATRi ATRi (VE-821, VE-822, AZ20) resensitized PARPi-resistant BRCA1-mutated human OvC cell line to PARPi [206] AZD6738 efficient in in ATM-deficient cells and in vivo in PDX mouse models with complete ATM loss [208] Combination PARPi with ATRi (AZD6738) and CHEK1i (MK8776) is more effective than PARPi alone in reducing tumor burden in BRCA1/2 mutated HGSOC cells and PDX models [209] Ongoing clinical PhaseII CAPRI Study of ATRi AZD6738 (ceralasertib) in combination with PARPi olaparib in HGSOC patients [212] ATMi ATMi KU55933 enhanced the response to ionizing radiation in A2780 and OVCAR3 OvC cells [213] WEE1i…”

Section: Chek1imentioning

confidence: 99%

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DNA Repair and Ovarian Carcinogenesis: Impact on Risk, Prognosis and Therapy Outcome

Tomášová

Čumová

Šeborová

et al. 2020

Cancers

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There is ample evidence for the essential involvement of DNA repair and DNA damage response in the onset of solid malignancies, including ovarian cancer. Indeed, high-penetrance germline mutations in DNA repair genes are important players in familial cancers: BRCA1, BRCA2 mutations or mismatch repair, and polymerase deficiency in colorectal, breast, and ovarian cancers. Recently, some molecular hallmarks (e.g., TP53, KRAS, BRAF, RAD51C/D or PTEN mutations) of ovarian carcinomas were identified. The manuscript overviews the role of DNA repair machinery in ovarian cancer, its risk, prognosis, and therapy outcome. We have attempted to expose molecular hallmarks of ovarian cancer with a focus on DNA repair system and scrutinized genetic, epigenetic, functional, and protein alterations in individual DNA repair pathways (homologous recombination, non-homologous end-joining, DNA mismatch repair, base- and nucleotide-excision repair, and direct repair). We suggest that lack of knowledge particularly in non-homologous end joining repair pathway and the interplay between DNA repair pathways needs to be confronted. The most important genes of the DNA repair system are emphasized and their targeting in ovarian cancer will deserve further attention. The function of those genes, as well as the functional status of the entire DNA repair pathways, should be investigated in detail in the near future.

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Section: Therapeutic Perspectives-targeting Of Dna Repair System In Omentioning

confidence: 86%

Section: Chek1imentioning

confidence: 99%

DNA Repair and Ovarian Carcinogenesis: Impact on Risk, Prognosis and Therapy Outcome

Tomášová

Čumová

Šeborová

et al. 2020

Cancers

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show abstract

“…Moreover, it ablated already present metastases in the liver after FOLFIRINOX induction in line with the abrogation of escaper clones being more invasive. Therefore one might speculate that the triple inhibition of PARP, ATR, and DNA-PKcs in an HR deficient context could prevent the observed selection process upon prolonged FOLFIRINOX, probably by increasing DNA damage beyond a tolerable threshold due to the sensitizing effects of FOLFIRINOX [19]. This ablation of any escaper clones is likely responsible for reduced metastatic burden [36].…”

Section: Discussionmentioning

confidence: 99%

Maintenance Therapy for ATM-Deficient Pancreatic Cancer by Multiple DNA Damage Response Interferences after Platinum-Based Chemotherapy

Roger¹,

Gout²,

Arnold³

et al. 2020

Cells

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Personalized medicine in treating pancreatic ductal adenocarcinoma (PDAC) is still in its infancy, albeit PDAC-related deaths are projected to rise over the next decade. Only recently, maintenance therapy with the PARP inhibitor olaparib showed improved progression-free survival in germline BRCA1/2-mutated PDAC patients after platinum-based induction for the first time. Transferability of such a concept to other DNA damage response (DDR) genes remains unclear. Here, we conducted a placebo-controlled, three-armed preclinical trial to evaluate the efficacy of multi-DDR interference (mDDRi) as maintenance therapy vs. continuous FOLFIRINOX treatment, implemented with orthotopically transplanted ATM-deficient PDAC cell lines. Kaplan–Meier analysis, cross-sectional imaging, histology, and in vitro analysis served as analytical readouts. Median overall survival was significantly longer in the mDDRi maintenance arm compared to the maintained FOLFIRINOX treatment. This survival benefit was mirrored in the highest DNA-damage load, accompanied by superior disease control and reduced metastatic burden. In vitro analysis suggests FOLFIRINOX-driven selection of invasive subclones, erased by subsequent mDDRi treatment. Collectively, this preclinical trial substantiates mDDRi in a maintenance setting as a novel therapeutic option and extends the concept to non-germline BRCA1/2-mutant PDAC.

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“…As discussed above for ATMi, also ATRi are able to increase toxicity more powerfully in cancer cells lacking ATM or that display a mutated form of p53 [ 54 , 55 , 56 ]. Coherently, ATM deficiency is one of the most advantageous biomarkers used for patient’s selection in clinical trials employing ATRi [ 40 , 49 , 57 ].…”

Section: Inhibition Of Ddr Kinases To Overcome Therapy Resistance mentioning

confidence: 99%

Targeting the DNA Damage Response to Overcome Cancer Drug Resistance in Glioblastoma

Ferri

Stagni

Barilá

2020

IJMS

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Glioblastoma multiforme (GBM) is a severe brain tumor whose ability to mutate and adapt to therapies is at the base for the extremely poor survival rate of patients. Despite multiple efforts to develop alternative forms of treatment, advances have been disappointing and GBM remains an arduous tumor to treat. One of the leading causes for its strong resistance is the innate upregulation of DNA repair mechanisms. Since standard therapy consists of a combinatory use of ionizing radiation and alkylating drugs, which both damage DNA, targeting the DNA damage response (DDR) is proving to be a beneficial strategy to sensitize tumor cells to treatment. In this review, we will discuss how recent progress in the availability of the DDR kinase inhibitors will be key for future therapy development. Further, we will examine the principal existing DDR inhibitors, with special focus on those currently in use for GBM clinical trials.

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Combined PARP and ATR inhibition potentiates genome instability and cell death in ATM-deficient cancer cells

Cited by 127 publications

References 64 publications

DNA Repair and Ovarian Carcinogenesis: Impact on Risk, Prognosis and Therapy Outcome

DNA Repair and Ovarian Carcinogenesis: Impact on Risk, Prognosis and Therapy Outcome

Maintenance Therapy for ATM-Deficient Pancreatic Cancer by Multiple DNA Damage Response Interferences after Platinum-Based Chemotherapy

Targeting the DNA Damage Response to Overcome Cancer Drug Resistance in Glioblastoma

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