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Wnt activation is implicated in glioblastoma radioresistance
Author(s) -
Yonghyun Kim,
Kang Ho Kim,
Jeena Lee,
Jeena Lee,
Young-Ae Lee,
Misuk Kim,
Se Jeong Lee,
Se Jeong Lee,
Kernyu Park,
Heekyoung Yang,
Juyoun Jin,
Kyeung Min Joo,
Jeongwu Lee,
Jeongwu Lee,
DoHyun Nam
Publication year - 2011
Publication title -
laboratory investigation
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.542
H-Index - 150
eISSN - 1530-0307
pISSN - 0023-6837
DOI - 10.1038/labinvest.2011.161
Subject(s) - radioresistance , sox2 , wnt signaling pathway , cancer research , clonogenic assay , in vivo , population , radiation therapy , stem cell , cd44 , biology , cell culture , ionizing radiation , medicine , cell , transcription factor , signal transduction , microbiology and biotechnology , irradiation , nuclear physics , physics , biochemistry , environmental health , gene , genetics
Glioblastoma (GBM) patients have dismal median survival even with the most rigorous treatments currently available. Radiotherapy is the most effective non-surgical therapy for GBM patients; however, patients succumb due to tumor recurrence within a year. To develop a curative therapeutic approach, we need to better understand the underlying molecular mechanism of radiation resistance in GBM. Towards this goal, we developed an in vivo orthotopic GBM model system that mimics the radiation response of human GBM, using both established-GBM cell line and patient-derived freshly dissociated GBM specimen. In-vivo ionizing radiation (IR) treatment prolonged the survival of mice with intracranical tumor derived from U373MG, but failed to prevent tumor recurrence. U373MG and GBM578 cells isolated after in-vivo IR (U373-IR and 578-IR) were more clonogenic and enriched with stem cell-like characteristics, compared with mock-treated control tumor cells. Transcriptomic analyses and quantitative real-time reverse-transcription PCR analyses using these matched GBM cells before and after radiation treatment revealed that Wnt pathways were preferentially activated in post-IR GBM cells. U373-IR cells and 578-IR were enriched with cells positive for both active β-catenin (ABC) and Sox2 population, and this subpopulation was further increased after additional in-vitro radiation treatment, suggesting that radiation resistance of GBM is mediated due, in part, to the activation of stem cell-associated pathways including Wnt. Finally, pharmacological and siRNA inhibition of Wnt pathway significantly decreased the survival and clonogenicity of GBM cells and reduced their ABC(+)/Sox2(+) population. Together, these data suggest that Wnt activation is a molecular mechanism to confer GBM radioresistance and an important therapeutic target.

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