作者
Remko Prevo, Emmanouil Fokas, Philip M Reaper, Peter A Charlton, John R Pollard, W Gillies McKenna, Ruth J Muschel, Thomas B Brunner
发表日期
2012/9/1
期刊
Cancer biology & therapy
卷号
13
期号
11
页码范围
1072-1081
出版商
Taylor & Francis
简介
DNA damaging agents such as radiotherapy and gemcitabine are frequently used for the treatment of pancreatic cancer. However, these treatments typically provide only modest benefit. Improving the low survival rate for pancreatic cancer patients therefore remains a major challenge in oncology. Inhibition of the key DNA damage response kinase ATR has been suggested as an attractive approach for sensitization of tumor cells to DNA damaging agents, but specific ATR inhibitors have remained elusive. Here we investigated the sensitization potential of the first highly selective and potent ATR inhibitor, VE-821, in vitro. VE-821 inhibited radiation- and gemcitabine-induced phosphorylation of Chk1, confirming inhibition of ATR signaling. Consistently, VE-821 significantly enhanced the sensitivity of PSN-1, MiaPaCa-2 and primary PancM pancreatic cancer cells to radiation and gemcitabine under both normoxic and …
引用总数
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