ATR Inhibitors VE-821 and VX-970 Sensitize Cancer Cells to Topoisomerase I Inhibitors by Disabling DNA Replication Initiation and Fork Elongation Responses

Jossé, Rozenn; Martin, Scott E.; Guha, Rajarshi; Ormanoglu, Pinar; Pfister, Thomas D.; Reaper, Philip M.; Barnes, Christopher S.; Jones, Julie L.; Charlton, Peter; Pollard, John R.; Morris, Joel; Doroshow, James H.; Pommier, ﻿Yves

doi:10.1158/0008-5472.can-13-3369

Cited by 139 publications

(116 citation statements)

References 48 publications

(112 reference statements)

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“…In the same study VX-970 increased sensitivity to cisplatin in six out of seven NSCLC PDX models [94]. In addition, ATR inhibitors have been shown to increase sensitivity to topoisomerase I inhibitors in colorectal cancer cell lines in vitro and in vivo [95], rationalising the combination of ATR inhibitors and topotecan in early phase clinical trials in SCLC. Summary of DNA damage pathways and therapeutics (Fig.…”

Section: Vx-970mentioning

confidence: 85%

Targeting DNA damage in SCLC

et al. 2017

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A B S T R A C TSCLC accounts for 15% of lung cancer worldwide. Characterised by early dissemination and rapid development of chemo-resistant disease, less than 5% of patients survive 5 years. Despite 3 decades of clinical trials there has been no change to the standard platinum and etoposide regimen for first line treatment developed in the 1970's.The exceptionally high number of genomic aberrations observed in SCLC combined with the characteristic rapid cellular proliferation results in accumulation of DNA damage and genomic instability. To flourish in this precarious genomic context, SCLC cells are reliant on functional DNA damage repair pathways and cell cycle checkpoints.Current cytotoxic drugs and radiotherapy treatments for SCLC have long been known to act by induction of DNA damage and the response of cancer cells to such damage determines treatment efficacy. Recent years have witnessed improved understanding of strategies to exploit DNA damage and repair mechanisms in order to increase treatment efficacy.This review will summarise the rationale to target DNA damage response in SCLC, the progress made in evaluating novel DDR inhibitors and highlight various ongoing challenges for their clinical development in this disease.

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Section: Vx-970mentioning

confidence: 85%

Targeting DNA damage in SCLC

et al. 2017

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“…Nevertheless, how replication stress can be measured in normal and cancer cells remains elusive. Because multiple ATRi and Chk1i are being tested in clinical trials for cancer therapy (Foote et al, 2013; Josse et al, 2014; Karp et al, 2012; Ma et al, 2013; Sausville et al, 2014; Seto et al, 2013), understanding the mechanisms of action and unique properties of these inhibitors may help to guide their applications in clinical settings.…”

Section: Introductionmentioning

confidence: 99%

Distinct but Concerted Roles of ATR, DNA-PK, and Chk1 in Countering Replication Stress during S Phase

et al. 2015

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The ATR-Chk1 pathway is critical for DNA damage responses and cell cycle progression. Chk1 inhibition is more deleterious to cycling cells than ATR inhibition, raising questions about ATR and Chk1 functions in the absence of extrinsic replication stress. Here, we show that a key role of ATR in S phase is to coordinate RRM2 accumulation and origin firing. ATR inhibitor (ATRi) induces massive ssDNA accumulation and replication catastrophe in a fraction of early S-phase cells. In other S-phase cells, however, ATRi induces moderate ssDNA and triggers a DNA-PK and Chk1-mediated backup pathway to suppress origin firing. The backup pathway creates a threshold such that ATRi selectively kills cells under high replication stress, whereas Chk1 inhibitor induces cell death at a lower threshold. The levels of ATRi-induced ssDNA correlate with ATRi sensitivity in a panel of cell lines, suggesting that ATRi-induced ssDNA could be predictive of ATRi sensitivity in cancer cells.

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“…In vivo studies using both VE-821 and VX-970 showed robust results. Indeed, these two ATR inhibitors synergized with radiotherapy and gemcitabine in pancreatic cancer xenograft models [76, 77] and with irinotecan in a colorectal cancer model [79]. Nowadays, different clinical trials are ongoing against solid tumors to assess the safety, tolerability, and pharmacokinetics of VX-970 in combination with cytotoxic chemotherapy (NCT02157792, NCT02595931, NCT02567422, and NCT02595892).…”

Section: Introductionmentioning

confidence: 99%

The cell cycle checkpoint inhibitors in the treatment of leukemias

2017

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The inhibition of the DNA damage response (DDR) pathway in the treatment of cancers has recently reached an exciting stage with several cell cycle checkpoint inhibitors that are now being tested in several clinical trials in cancer patients. Although the great amount of pre-clinical and clinical data are from the solid tumor experience, only few studies have been done on leukemias using specific cell cycle checkpoint inhibitors. This review aims to summarize the most recent data found on the biological mechanisms of the response to DNA damages highlighting the role of the different elements of the DDR pathway in normal and cancer cells and focusing on the main genetic alteration or aberrant gene expression that has been found on acute and chronic leukemias. This review, for the first time, outlines the most important pre-clinical and clinical data available on the efficacy of cell cycle checkpoint inhibitors in single agent and in combination with different agents normally used for the treatment of acute and chronic leukemias.

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ATR Inhibitors VE-821 and VX-970 Sensitize Cancer Cells to Topoisomerase I Inhibitors by Disabling DNA Replication Initiation and Fork Elongation Responses

Cited by 139 publications

References 48 publications

Targeting DNA damage in SCLC

Targeting DNA damage in SCLC

Distinct but Concerted Roles of ATR, DNA-PK, and Chk1 in Countering Replication Stress during S Phase

The cell cycle checkpoint inhibitors in the treatment of leukemias

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