The identification of the ATR inhibitor VE-822 as a therapeutic strategy for enhancing cisplatin chemosensitivity in esophageal squamous cell carcinoma

The identification of the ATR inhibitor VE-822 as a therapeutic strategy for enhancing cisplatin chemosensitivity in esophageal squamous cell carcinoma

Inducing DNA damage is known to be one of the mechanisms of cytotoxic chemotherapy agents for cancer such as cisplatin. The endogenous DNA damage response confers chemoresistance to these agents by repairing DNA damage. The initiation and transduction of the DNA damage response (DDR) signaling pathw...

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Veröffentlicht in:Cancer letters 2018-09, Vol.432, p.56-68
Hauptverfasser: Shi, Qi, Shen, Lu-Yan, Dong, Bin, Fu, Hao, Kang, Xiao-Zheng, Yang, Yong-Bo, Dai, Liang, Yan, Wan-Pu, Xiong, Hong-Chao, Liang, Zhen, Chen, Ke-Neng
Format: Artikel
Sprache:eng
Schlagworte:
Activation
Antigens
Apoptosis
Ataxia
Ataxia telangiectasia
Ataxia telangiectasia mutated protein
ATM deficiency
ATR inhibitor
Cancer therapies
Cell cycle
Cell proliferation
Cell survival
Chemoresistance
Chemotherapy
CHK1 protein
Cisplatin
Cytotoxicity
Deoxyribonucleic acid
DNA
DNA damage
DNA damage response
DNA repair
Drug dosages
Esophageal cancer
Esophagus
G1 phase
Glycoproteins
Inhibition
Kinases
Maintenance
Medical prognosis
Signal transduction
Squamous cell carcinoma
Strategy
Surgery
Synergistic effect
Thoracic surgery
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Zusammenfassung:Inducing DNA damage is known to be one of the mechanisms of cytotoxic chemotherapy agents for cancer such as cisplatin. The endogenous DNA damage response confers chemoresistance to these agents by repairing DNA damage. The initiation and transduction of the DNA damage response (DDR) signaling pathway, which is dependent on the activation of ATM (ataxia-telangiectasia mutated) and ATR (ataxia telangiectasia and Rad3-related), is essential for DNA damage repair, the maintenance of genomic stability and cell survival. Therefore, ATM or ATR inhibition is considered as a promising strategy for sensitizing cancer cells to chemotherapy. This study is aimed to explore the effect of ATR inhibitor on sensitizing ESCC (esophageal squamous cell carcinoma) cells to cisplatin, and whether ATM deficiency could impact the sensitization. We found that 21.5% of ESCC cases had ATM deficiency and that patients with ATR activation after neoadjuvant chemotherapy had worse chemotherapy response and poorer overall survival than that without ATR activation (32 mons vs. >140mons). Then, it was shown that VE-822 inhibited ATR-CHK1 pathway activation, leading to the accumulation of cisplatin-modified DNA. And it inhibited cell proliferation, induced cell cycle arrest in G1 phase and enhanced cell apoptosis. Moreover, VE-822 significantly sensitized ESCC cells to cisplatin, and these two drugs had synergistic effects, especially in ATM-deficient cells, in vitro and in vivo. Our results suggest that ATR inhibition combining with cisplatin is a new strategy for managing patients with ESCC, especially those with ATM-deficiency. However, this is an idea that requires further validation. •ATR activation was associated with efficiency of neoadjuvant chemotherapy.•VE-822 promoted cell apoptosis and induced cell cycle arrest in ESCC cells.•VE-822 sensitized ESCC cells to cisplatin, in vitro and in vivo.•VE-822 along with cisplatin induces DNA-cisplatin adduct accumulation.
ISSN:0304-3835
1872-7980
DOI:10.1016/j.canlet.2018.06.010