MEK-ERK Signaling Dictates DNA-Repair Gene MGMT Expression and Temozolomide Resistance of Stem-Like Glioblastoma Cells via the MDM2-p53 Axis

被引:98
|
作者
Sato, Atsushi [1 ,2 ]
Sunayama, Jun [1 ,3 ,4 ]
Matsuda, Ken-ichiro [1 ,2 ]
Seino, Shizuka [1 ,3 ,4 ]
Suzuki, Kaori [1 ,3 ,4 ]
Watanabe, Eriko [1 ,3 ,4 ]
Tachibana, Ken [1 ]
Tomiyama, Arata [1 ]
Kayama, Takamasa [2 ]
Kitanaka, Chifumi [1 ,3 ,4 ]
机构
[1] Yamagata Univ, Dept Mol Canc Sci, Sch Med, Yamagata 9909585, Japan
[2] Yamagata Univ, Dept Neurosurg, Sch Med, Yamagata 9909585, Japan
[3] Yamagata Univ, Oncol Res Ctr, Res Inst Adv Mol Epidemiol, Yamagata 9909585, Japan
[4] Japan Soc Promot Sci, Global COE Program Med Sci, Tokyo, Japan
来源
STEM CELLS | 2011年 / 29卷 / 12期
基金
日本学术振兴会;
关键词
Glioma; Chemoresistance; Cancer stem cell; Mitogen-activated protein kinase; Combination therapy; O-6-METHYLGUANINE-DNA METHYLTRANSFERASE GENE; INITIATING CELLS; PROMOTER HYPERMETHYLATION; MALIGNANT GLIOMAS; TUMOR-CELLS; P53; TRANSCRIPTION; SENSITIVITY; THERAPY; LINES;
D O I
10.1002/stem.753
中图分类号
Q813 [细胞工程];
学科分类号
摘要
Overcoming the resistance of glioblastoma cells against temozolomide, the first-line chemotherapeutic agent of choice for newly diagnosed glioblastoma, is a major therapeutic challenge in the management of this deadly brain tumor. The gene encoding O(6)-methylguanine DNA methyltransferase (MGMT), which removes the methyl group attached by temozolomide, is often silenced by promoter methylation in glioblastoma but is nevertheless expressed in a significant fraction of cases and is therefore regarded as one of the most clinically relevant mechanisms of resistance against temozolomide. However, to date, signaling pathways regulating MGMT in MGMT-expressing glioblastoma cells have been poorly delineated. Here in this study, we provide lines of evidence that the mitogen-activated protein/extracellular signal-regulated kinase kinase (MEK)-extracellular signal-regulated kinase (ERK)-murine double minute 2 (MDM2)-p53 pathway plays a critical role in the regulation of MGMT expression, using stem-like glioblastoma cells directly derived from patient tumor samples and maintained in the absence of serum, which not only possess stem-like properties but are also known to phenocopy the characteristics of the original tumors from which they are derived. We show that, in stem-like glioblastoma cells, MEK inhibition reduced MDM2 expression and that inhibition of either MEK or MDM2 resulted in p53 activation accompanied by p53-dependent downregulation of MGMT expression. MEK inhibition rendered otherwise resistant stem-like glioblastoma cells sensitive to temozolomide, and combination of MEK inhibitor and temozolomide treatments effectively deprived stem-like glioblastoma cells of their tumorigenic potential. Our findings suggest that targeting of the MEK-ERK-MDM2-p53 pathway in combination with temozolomide could be a novel and promising therapeutic strategy in the treatment of glioblastoma. STEM CELLS 2011;29:1942-1951
引用
收藏
页码:1942 / 1951
页数:10
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