Targeting RNA Polymerase I transcription synergises with TOP1 inhibition in potentiating the DNA damage response in high-grade serous ovarian cancer

Yan, Shunfei; Madhamshettiwar, Piyush B.; Simpson, Kaylene J.; Ellis, Sarah; Kang, Jian; Cullinane, Carleen; Sheppard, Karen E.; Hannan, Katherine M.; Hannan, Ross D.; Sanij, Elaine; Pearson, Richard B.; Chan, Keefe T.

doi:10.1101/849307

Cited by 3 publications

(4 citation statements)

References 25 publications

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“…The strong association of higher proportions of active rDNA with sensitivity to growth inhibition by CX-5461 is consistent with CX-5461's mode of action in triggering defects associated with open chromatin and replication stress at the rDNA (Quin et al, 2016;Yan et al, 2019;Sanij et al, 2020), including potentially acting as a TOP 2 poison (Bruno et al, 2020) selectively at the rDNA and/or across the genome. We have demonstrated that CX-5461 activates nucleolar ATM and ATR leading to activation of cell cycle checkpoints and global replication-mediated DNA damage (Quin et al, 2016;Yan et al, 2019;Sanij et al, 2020). Our data therefore suggests that cells with a higher ratio of active rDNA are more sensitive to CX-5461-mediated nucleolar DDR and activation of cell cycle checkpoints, with faster proliferating cells being more responsive to cell cycle arrest.…”

Section: Discussionsupporting

confidence: 63%

“…We have previously shown that CX-5461 activates nucleolar DDR by inducing chromatin defects and replication stress at the rDNA ( Quin et al, 2016 ; Yan et al, 2019 ; Sanij et al, 2020 ). Therefore, we examined whether the number of active rDNA repeats and/or the proportion of active to inactive rDNA repeats are determining factors for CX-5461 sensitivity.…”

Section: Resultsmentioning

confidence: 99%

“…Pol I transcription is a therapeutic target for small anti-cancer drugs ( Bywater et al, 2012 ; Hein et al, 2013 ; Peltonen et al, 2014 ). The first-in-class Pol I transcription inhibitor, CX-5461 is a promising cancer therapy as a single agent and in combination therapy in pre-clinical models of lymphoma, acute myeloid leukemia, prostate and ovarian cancer ( Bywater et al, 2012 ; Devlin et al, 2016 ; Rebello et al, 2016 ; Hein et al, 2017 ; Yan et al, 2019 ; Sanij et al, 2020 ). Recently, the sensitivity profile of CX-5461 was shown to closely resemble a topoisomerase II (TOP2) poison ( Olivieri et al, 2019 ; Bruno et al, 2020 ).…”

Section: Introductionmentioning

confidence: 99%

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rDNA Chromatin Activity Status as a Biomarker of Sensitivity to the RNA Polymerase I Transcription Inhibitor CX-5461

Son

Hannan

Poortinga

et al. 2020

Front. Cell Dev. Biol.

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Section: Discussionsupporting

confidence: 63%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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rDNA Chromatin Activity Status as a Biomarker of Sensitivity to the RNA Polymerase I Transcription Inhibitor CX-5461

Son

Hannan

Poortinga

et al. 2020

Front. Cell Dev. Biol.

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“…6A-6B), all genes converging on DNA damage response. Based on our mechanistic work showing the DNA damaging effects of CX-5461 and previous observations of their efficacy in other cancers 43, 44 we chose to investigate drugs targeting these genes as potential combinations with CX-5461. Thus, we screened CHP-134, IMR-5, BE(2)-M17, and KELLY neuroblastoma cell lines with the combination of CX-5461 and AZD-1390 (ATM inhibitor), AZD-6738 (ATR inhibitor), and SN-38 (the active metabolite of irinotecan; TOP1 inhibitor).…”

Section: Resultsmentioning

confidence: 99%

The chemotherapeutic CX-5461 primarily targets TOP2B and exhibits selective activity in high-risk neuroblastoma

Pan

Wright

Chapple

et al. 2021

Preprint

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Survival in high-risk pediatric neuroblastoma has remained around 50% for the last 20 years, with immunotherapies and targeted therapies having had minimal impact. Here, we identify the small molecule CX-5461 as selectively cytotoxic to high-risk neuroblastoma and synergistic with low picomolar concentrations of topoisomerase I inhibitors improving survival in vivo in orthotopic patient-derived xenograft neuroblastoma mouse models. CX-5461 recently progressed through phase I clinical trial as a first-in-human inhibitor of RNA-POL I. However, we also use a comprehensive panel of in vitro and in vivo assays to demonstrate that CX-5461 has been mischaracterized and that its primary target at pharmacologically relevant concentrations, is in fact topoisomerase II beta (TOP2B), not RNA-POL I. These findings are important because existing clinically approved chemotherapeutics have well-documented off-target interactions with TOP2B, which have previously been shown to cause both therapy-induced leukemia and cardiotoxicity, often-fatal adverse events, which can emerge several years after treatment. Thus, while we show that combination therapies involving CX-5461 have promising anti-tumor activity in vivo in neuroblastoma, our identification of TOP2B as the primary target of CX-5461 indicates unexpected safety concerns that should be examined in ongoing phase II clinical trials in adult patients before pursuing clinical studies in children.

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The RNA polymerase I transcription inhibitor CX-5461 cooperates with topoisomerase 1 inhibition by enhancing the DNA damage response in homologous recombination-proficient high-grade serous ovarian cancer

et al. 2020

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Background Intrinsic and acquired drug resistance represent fundamental barriers to the cure of high-grade serous ovarian carcinoma (HGSC), the most common histological subtype accounting for the majority of ovarian cancer deaths. Defects in homologous recombination (HR) DNA repair are key determinants of sensitivity to chemotherapy and poly-ADP ribose polymerase inhibitors. Restoration of HR is a common mechanism of acquired resistance that results in patient mortality, highlighting the need to identify new therapies targeting HR-proficient disease. We have shown promise for CX-5461, a cancer therapeutic in early phase clinical trials, in treating HR-deficient HGSC. Methods Herein, we screen the whole protein-coding genome to identify potential targets whose depletion cooperates with CX-5461 in HR-proficient HGSC. Results We demonstrate robust proliferation inhibition in cells depleted of DNA topoisomerase 1 (TOP1). Combining the clinically used TOP1 inhibitor topotecan with CX-5461 potentiates a G2/M cell cycle checkpoint arrest in multiple HR-proficient HGSC cell lines. The combination enhances a nucleolar DNA damage response and global replication stress without increasing DNA strand breakage, significantly reducing clonogenic survival and tumour growth in vivo. Conclusions Our findings highlight the possibility of exploiting TOP1 inhibition to be combined with CX-5461 as a non-genotoxic approach in targeting HR-proficient HGSC.

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Targeting RNA Polymerase I transcription synergises with TOP1 inhibition in potentiating the DNA damage response in high-grade serous ovarian cancer

Cited by 3 publications

References 25 publications

rDNA Chromatin Activity Status as a Biomarker of Sensitivity to the RNA Polymerase I Transcription Inhibitor CX-5461

rDNA Chromatin Activity Status as a Biomarker of Sensitivity to the RNA Polymerase I Transcription Inhibitor CX-5461

The chemotherapeutic CX-5461 primarily targets TOP2B and exhibits selective activity in high-risk neuroblastoma

The RNA polymerase I transcription inhibitor CX-5461 cooperates with topoisomerase 1 inhibition by enhancing the DNA damage response in homologous recombination-proficient high-grade serous ovarian cancer

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