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DOI: 10.1371/journal.pone.0011397
¤ OpenAccess: Gold
This work has “Gold” OA status. This means it is published in an Open Access journal that is indexed by the DOAJ.

Targeting DNA-PKcs and ATM with miR-101 Sensitizes Tumors to Radiation

Dan Yan,Wooi Loon Ng,Xiangming Zhang,Ping Wang,Zhaobin Zhang,Yin‐Yuan Mo,Hui Mao,Chunhai Hao,Jeffrey J. Olson,Walter J. Curran,Ya Wang

DNA repair
DNA-PKcs
Homologous recombination
2010
Background Radiotherapy kills tumor-cells by inducing DNA double strand breaks (DSBs). However, the efficient repair of tumors frequently prevents successful treatment. Therefore, identifying new practical sensitizers is an essential step towards successful radiotherapy. In this study, we tested the new hypothesis: identifying the miRNAs to target DNA DSB repair genes could be a new way for sensitizing tumors to ionizing radiation. Principal Findings Here, we chose two genes: DNA-PKcs (an essential factor for non-homologous end-joining repair) and ATM (an important checkpoint regulator for promoting homologous recombination repair) as the targets to search their regulating miRNAs. By combining the database search and the bench work, we picked out miR-101. We identified that miR-101 could efficiently target DNA-PKcs and ATM via binding to the 3′- UTR of DNA-PKcs or ATM mRNA. Up-regulating miR-101 efficiently reduced the protein levels of DNA-PKcs and ATM in these tumor cells and most importantly, sensitized the tumor cells to radiation in vitro and in vivo. Conclusions These data demonstrate for the first time that miRNAs could be used to target DNA repair genes and thus sensitize tumors to radiation. These results provide a new way for improving tumor radiotherapy.
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    Targeting DNA-PKcs and ATM with miR-101 Sensitizes Tumors to Radiation” is a paper by Dan Yan Wooi Loon Ng Xiangming Zhang Ping Wang Zhaobin Zhang Yin‐Yuan Mo Hui Mao Chunhai Hao Jeffrey J. Olson Walter J. Curran Ya Wang published in 2010. It has an Open Access status of “gold”. You can read and download a PDF Full Text of this paper here.