The PARP Inhibitor AZD2461 Provides Insights into the Role of PARP3 Inhibition for Both Synthetic Lethality and Tolerability with Chemotherapy in Preclinical Models

O’Connor, Lenka Oplustil; Rulten, Stuart L.; Cranston, Aaron; Odedra, Rajesh; Brown, H. Shelton; Jaspers, Janneke E.; Jones, Louise; Knights, Charlotte; Evers, Bastiaan; Ting, Attilla; Bradbury, Robert H.; Pajic, Marina; Rottenberg, Sven; Jonkers, Jos; Rudge, David A.; Martin, Niall M.B.; Caldecott, Keith W.; Lau, Alan

doi:10.1158/0008-5472.can-15-3240

Cited by 70 publications

(73 citation statements)

References 49 publications

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“…Tumors from KB2P mouse donors were transplanted orthotopically into wild-type syngeneic mice, and when the tumor reached a volume >200 mm 3 , mice were treated with the PARPi AZD2461 for 28 consecutive days. Of note, PARPi AZD2461 is not a P-glycoprotein (Pgp) substrate, and therefore, acquired resistance to AZD2461 cannot be mediated by Pgp upregulation (Oplustil O’Connor et al, 2016). After an initial phase of response, the tumors eventually relapsed and were allowed to regrow to 100% volume, following which another treatment cycle was started.…”

Section: Resultsmentioning

confidence: 99%

Multifaceted Impact of MicroRNA 493-5p on Genome-Stabilizing Pathways Induces Platinum and PARP Inhibitor Resistance in BRCA2-Mutated Carcinomas

et al. 2018

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SUMMARY BRCA1/2-mutated ovarian cancers (OCs) are defective in homologous recombination repair (HRR) of double-strand breaks (DSBs) and thereby sensitive to platinum and PARP inhibitors (PARPis). Multiple PARPis have recently received US Food and Drug Administration (FDA) approval for treatment of OCs, and resistance to PARPis is a major clinical problem. Utilizing primary and recurrent BRCA1/2-mutated carcinomas from OC patients, patient-derived lines, and an in vivo BRCA2-mutated mouse model, we identified a microRNA, miR-493-5p, that induced platinum/PARPi resistance exclusively in BRCA2-mutated carcinomas. However, in contrast to the most prevalent resistance mechanisms in BRCA mutant carcinomas, miR-493-5p did not restore HRR. Expression of miR-493-5p in BRCA2-mutated/depleted cells reduced levels of nucleases and other factors involved in maintaining genomic stability. This resulted in relatively stable replication forks, diminished single-strand annealing of DSBs, and increased R-loop formation. We conclude that impact of miR-493-5p on multiple pathways pertinent to genome stability cumulatively causes PARPi/platinum resistance in BRCA2 mutant carcinomas.

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Section: Resultsmentioning

confidence: 99%

Multifaceted Impact of MicroRNA 493-5p on Genome-Stabilizing Pathways Induces Platinum and PARP Inhibitor Resistance in BRCA2-Mutated Carcinomas

et al. 2018

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“…2C,D). These events have also been known to mediate resistance in ovarian cancer patients (Swisher et al 2008;Patch et al 2015), showing the predictive potential of PDX models. The PDX models also revealed a novel resistance mechanism involving gene fusions that placed BRCA1 under transcriptional control of a heterologous promoter.…”

Section: Parpi Resistance Mechanisms In Brca-associated Breast Cancermentioning

confidence: 95%

“…Although the clinical relevance of P-gp up-regulation as cause of drug resistance remains controversial (AmiriKordestani et al 2012), expression of MDR1, the human counterpart of Abcb1, was recently found to be inversely correlated to olaparib response in human ovarian cancer cells (Vaidyanathan et al 2016). Such increased expression may result from complex genomic rearrangements that fuse a distant promoter to the MDR1 gene and thereby bypass the MDR1 promoter methylation (Patch et al 2015). The case of P-gp shows that a thorough mechanistic understanding is instrumental to combat resistant tumors-for example, by coadministration of tariquidar or by switching treatment to chemotherapeutics that are poor substrates for P-gp (Jaspers et al 2013).…”

Section: Parpi Resistance Mechanisms In Brca-associated Breast Cancermentioning

confidence: 99%

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Genetic Dissection of Cancer Development, Therapy Response, and Resistance in Mouse Models of Breast Cancer

Annunziato

Barazas

Rottenberg

et al. 2016

Cold Spring Harb Symp Quant Biol

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The cancer genomics revolution has rapidly expanded the inventory of somatic mutations characterizing human malignancies, highlighting a previously underappreciated extent of molecular variability between and within patients. Also in breast cancer, the most commonly diagnosed malignancy in women, this heterogeneity complicates the understanding of the stepwise sequence of pathogenic events and the design of effective and long-lasting target therapies. To disentangle this complexity and pinpoint which molecular perturbations are crucial to hijack the cellular machinery and lead to tumorigenesis and drug resistance, functional studies are needed in model systems that faithfully and comprehensively recapitulate all the salient aspects of their cognate human counterparts. Mouse models of breast cancer have been instrumental for the study of tumor initiation and drug response but also involve cost and time limitations that represent serious bottlenecks in translational research. To keep pace with the overwhelming amount of hypotheses that warrant in vivo testing, continuous refinement of current breast cancer models and implementation of new technologies is crucial. In this review, we summarize the current state of the art in modeling human breast cancer in mice, and we put forward our vision for future developments.

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“…These include BMN 673 (Biomarin) (24), niraparib (25), rucaparib (26), veliparib (27), and AZD2461 (28). In addition, the efficacy of some PARP inhibitors has been identified in non-BRCA-mutation-linked cancers, including sporadic castration-resistant prostate cancer and non-smallcell lung cancer.…”

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confidence: 99%

PARP Inhibitors and DNA Repair: A Novel Beneficial Approach for Targeting Synthetic Lethal Tumor Cells

et al. 2017

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The PARP Inhibitor AZD2461 Provides Insights into the Role of PARP3 Inhibition for Both Synthetic Lethality and Tolerability with Chemotherapy in Preclinical Models

Cited by 70 publications

References 49 publications

Multifaceted Impact of MicroRNA 493-5p on Genome-Stabilizing Pathways Induces Platinum and PARP Inhibitor Resistance in BRCA2-Mutated Carcinomas

Multifaceted Impact of MicroRNA 493-5p on Genome-Stabilizing Pathways Induces Platinum and PARP Inhibitor Resistance in BRCA2-Mutated Carcinomas

Genetic Dissection of Cancer Development, Therapy Response, and Resistance in Mouse Models of Breast Cancer

PARP Inhibitors and DNA Repair: A Novel Beneficial Approach for Targeting Synthetic Lethal Tumor Cells

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