miR-27b synergizes with anticancer drugs via p53 activation and CYP1B1 suppression

被引:0
|
作者
Wenjing Mu
Chaobo Hu
Haibin Zhang
Zengqiang Qu
Jin Cen
Zhixin Qiu
Chao Li
Haozhen Ren
Yixue Li
Xianghuo He
Xiaolei Shi
Lijian Hui
机构
[1] State Key Laboratory of Cell Biology,Department of Hepatobiliary Surgery
[2] Shanghai Institute of Biochemistry and Cell Biology,undefined
[3] Shanghai Institutes for Biological Sciences,undefined
[4] Chinese Academic of Sciences,undefined
[5] Eastern Hepatobilliary Surgery Hospital,undefined
[6] Second Military Medical University,undefined
[7] Key Laboratory of Systems Biology,undefined
[8] Shanghai Institutes for Biological Sciences,undefined
[9] Chinese Academy of Sciences,undefined
[10] the Affiliated Drum Tower Hospital of Nanjing University Medical School,undefined
[11] Fudan University Shanghai Cancer Center and Institutes of Biomedical Sciences,undefined
[12] Shanghai Medical College,undefined
[13] Fudan University,undefined
来源
Cell Research | 2015年 / 25卷
关键词
liver cancer; kidney cancer; miR-27b; drug resistance; p53; CYP1B1;
D O I
暂无
中图分类号
学科分类号
摘要
Liver and kidney cancers are notorious for drug resistance. Due to the complexity, redundancy and interpatient heterogeneity of resistance mechanisms, most efforts targeting a single pathway were unsuccessful. Novel personalized therapies targeting multiple essential drug resistance pathways in parallel hold a promise for future cancer treatment. Exploiting the multitarget characteristic of microRNAs (miRNAs), we developed a new therapeutic strategy by the combinational use of miRNA and anticancer drugs to increase drug response. By a systems approach, we identified that miR-27b, a miRNA deleted in liver and kidney cancers, sensitizes cancer cells to a broad spectrum of anticancer drugs in vitro and in vivo. Functionally, miR-27b enhances drug response by activating p53-dependent apoptosis and reducing CYP1B1-mediated drug detoxification. Notably, miR-27b promotes drug response specifically in patients carrying p53-wild-type or CYP1B1-high signature. Together, we propose that miR-27b synergizes with anticancer drugs in a defined subgroup of liver and kidney cancer patients.
引用
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页码:477 / 495
页数:18
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