The DNA Damage Response: Making It Safe to Play with Knives

Ciccia, Alberto; Elledge, Stephen J.

doi:10.1016/j.molcel.2010.09.019

Cited by 3,618 publications

(3,985 citation statements)

References 247 publications

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“…cDNA pool prepared from the previous reaction was diluted by Activated checkpoints not only induce cell cycle arrest or cell death in response to some types of DNA damage (Nakano and Vousden, 2001;Yu et al, 2001) but also shown to protect tumour cells from apoptosis (Meuth, 2010;Rodriguez and Meuth, 2006;Sidi et al, 2008). In eukaryotic cells there are two highly conserved signalling cascades: two members of the phosphatidylinositol 3-kinase-like family of kinases, Ataxia telangiectasia mutated (ATM) and ATM and Rad3 related (ATR) (Ciccia and Elledge, 2010) participate in these systems. Under DNA damage or replication stress, these activated kinases phosphorylate a number of downstream proteins to protect DNA integrity, including two key protein kinases, checkpoint kinase 1 (CHK1) and checkpoint kinase 2 (CHK2) (Bartek and Lukas, 2003).…”

Section: Qpcrmentioning

confidence: 99%

Differential response of normal and malignant urothelial cells to CHK1 and ATM inhibitors

2014

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Section: Qpcrmentioning

confidence: 99%

Differential response of normal and malignant urothelial cells to CHK1 and ATM inhibitors

2014

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“…As is known, DNA repair after radiation is an important mechanism of radioresistance 33, 34. Considering that bioinformatic prediction has become a preferential method to explore the targets of miRNAs,35, 36 we chose potential targets from predicted ones involved in radioresistance and confirmed these targets by biochemical experiments.…”

Section: Discussionmentioning

confidence: 99%

Radiosensitizing effects of miR‐18a‐5p on lung cancer stem‐like cells via downregulating both ATM and HIF‐1α

Chen

et al. 2018

Cancer Medicine

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Lung cancer is one of the main causes of cancer mortality globally. Most patients received radiotherapy during the course of disease. However, radioresistance generally occurs in the majority of these patients, leading to poor curative effect, and the underlying mechanism remains unclear. In the present study, miR‐18a‐5p expression was downregulated in irradiated lung cancer cells. Overexpression of miR‐18a‐5p increased the radiosensitivity of lung cancer cells and inhibited the growth of A549 xenografts after radiation exposure. Dual luciferase report system and miR‐18a‐5p overexpression identified ataxia telangiectasia mutated (ATM) and hypoxia inducible factor 1 alpha (HIF‐1α) as the targets of miR‐18a‐5p. The mRNA and protein expressions of ATM and HIF‐1α were dramatically downregulated by miR‐18a‐5p in vitro and in vivo. Clinically, plasma miR‐18a‐5p expression was significantly higher in radiosensitive than in radioresistant group (P < .001). The cutoff value of miR‐18a‐5p >2.28 was obtained from receiver operating characteristic (ROC) curve. The objective response rate (ORR) was significantly higher in miR‐18a‐5p‐high group than in miR‐18a‐5p‐low group (P < .001). A tendency demonstrated that the median local progression‐free survival (PFS) from radiotherapy was longer in miR‐18a‐5p‐high than in miR‐18a‐5p‐low group (P = .082). The median overall survival (OS) from radiotherapy was numerically longer in miR‐18a‐5p‐high than in miR‐18a‐5p‐low group (P = .281). The sensitivity and specificity of plasma miR‐18a‐5p to predict radiosensitivity was 87% and 95%, respectively. Collectively, these results indicate that miR‐18a‐5p increases the radiosensitivity in lung cancer cells and CD133+ stem‐like cells via downregulating ATM and HIF‐1α expressions. Plasma miR‐18a‐5p would be an available indicator of radiosensitivity in lung cancer patients.

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“…Physical and biochemical repair of radiation induced DNA damage is executed by three main pathways: non-homologous end-joining (NHEJ) and homologous recombination (HR), which repair double stranded DNA breaks (DSB); and base excision repair (BER), which repairs single stranded DNA breaks (SSB) (reviewed in [3]). In the context of conventional external beam radiotherapy, DSB are generated in far fewer numbers than SSB but are highly mutagenic, and are cytotoxic if unrepaired.…”

Section: Introductionmentioning

confidence: 99%

Science in Focus: Combining Radiotherapy with Inhibitors of the DNA Damage Response

Chalmers

2016

Clinical Oncology

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The DNA Damage Response: Making It Safe to Play with Knives

Cited by 3,618 publications

References 247 publications

Differential response of normal and malignant urothelial cells to CHK1 and ATM inhibitors

Differential response of normal and malignant urothelial cells to CHK1 and ATM inhibitors

Radiosensitizing effects of miR‐18a‐5p on lung cancer stem‐like cells via downregulating both ATM and HIF‐1α

Science in Focus: Combining Radiotherapy with Inhibitors of the DNA Damage Response

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