OBJECTIVE: We investigated whether the hydroxyurea-induced loss of double-minute chromosomes containing amplified epidermal growth factor receptor (EGFR) genes would lead to a loss of tumorigenicity of a glioblastoma multiforme cell line. METHODS: Glioblastoma multiforme cells were treated in vitro with 0 (HU0) or 100 micromol/L (HU100) hydroxyurea and then injected into the flanks of nude mice. Survival and tumor volumes were evaluated. Pulsed-field gel electrophoresis, Southern blot hybridization, and slot-blot analysis were used to determine EGFR amplification levels. Flow cytometry and immunofluorescent staining were used for cell-cycle analysis and EGFR protein expression. RESULTS: Prior to injection, HU100 cells lost 95% of their amplified EGFR genes and developed into tumors 6 weeks after injection versus 3 weeks for HU0 cells. Mice with HU100 tumors had a median survival of 62 days versus 43 days for control mice with HU0 tumors. Pulse-field gel electrophoresis analysis showed that HU100 tumors had reamplified the EGFR gene as double-minute chromosomes of the same size as those originally present before hydroxyurea treatment. When HU100 cells were cultured in the absence of hydroxyurea, the EGFR gene also reamplified. HU100 cells grew at less than half the rate of untreated HU0 control cells in culture and showed a decreased number of cells entering the cell cycle. Immunofluorescent staining of HU150 (150 micromol/L) cells showed decreased EGFR protein expression. CONCLUSION: The EGFR gene is important for tumorigenicity in mice and growth in culture. Hydroxyurea induces the loss of double-minute chromosome-amplified EGFR genes against a selection gradient and significantly delays the onset of tumors. These results support the potential use of low-dose hydroxyurea for the treatment of human glioblastoma multiforme.
OBJECTIVE: We investigated whether the hydroxyurea-induced loss of double-minute chromosomes containing amplified epidermal growth factor receptor (EGFR) genes would lead to a loss of tumorigenicity of a glioblastoma multiforme cell line. METHODS:Glioblastoma multiforme cells were treated in vitro with 0 (HU0) or 100 micromol/L (HU100) hydroxyurea and then injected into the flanks of nude mice. Survival and tumor volumes were evaluated. Pulsed-field gel electrophoresis, Southern blot hybridization, and slot-blot analysis were used to determine EGFR amplification levels. Flow cytometry and immunofluorescent staining were used for cell-cycle analysis and EGFR protein expression. RESULTS: Prior to injection, HU100 cells lost 95% of their amplified EGFR genes and developed into tumors 6 weeks after injection versus 3 weeks for HU0 cells. Mice with HU100 tumors had a median survival of 62 days versus 43 days for control mice with HU0 tumors. Pulse-field gel electrophoresis analysis showed that HU100 tumors had reamplified the EGFR gene as double-minute chromosomes of the same size as those originally present before hydroxyurea treatment. When HU100 cells were cultured in the absence of hydroxyurea, the EGFR gene also reamplified. HU100 cells grew at less than half the rate of untreated HU0 control cells in culture and showed a decreased number of cells entering the cell cycle. Immunofluorescent staining of HU150 (150 micromol/L) cells showed decreased EGFR protein expression. CONCLUSION: The EGFR gene is important for tumorigenicity in mice and growth in culture. Hydroxyurea induces the loss of double-minute chromosome-amplified EGFR genes against a selection gradient and significantly delays the onset of tumors. These results support the potential use of low-dose hydroxyurea for the treatment of humanglioblastoma multiforme.
Authors: Gregor Dresemann; Michael Weller; Mark A Rosenthal; Ulrich Wedding; Wolfgang Wagner; Erik Engel; Bernhard Heinrich; Regine Mayer-Steinacker; Anders Karup-Hansen; Oystein Fluge; Anna Nowak; Maximilian Mehdorn; Eberhard Schleyer; Dietmar Krex; Ian N Olver; Joachim P Steinbach; Christian Hosius; Christian Sieder; Greg Sorenson; Richard Parker; Zariana Nikolova Journal: J Neurooncol Date: 2009-08-18 Impact factor: 4.130
Authors: Yuhui Wang; Nan Wu; Donglin Sun; Haiming Sun; Dandan Tong; Duo Liu; Bo Pang; Su Li; Jia Wei; Jialin Dai; Yang Liu; Jing Bai; Jingshu Geng; Songbin Fu; Yan Jin Journal: Cancer Sci Date: 2017-06-14 Impact factor: 6.716
Authors: E Zeynep Erson-Omay; Octavian Henegariu; S Bülent Omay; Akdes Serin Harmancı; Mark W Youngblood; Ketu Mishra-Gorur; Jie Li; Koray Özduman; Geneive Carrión-Grant; Victoria E Clark; Caner Çağlar; Mehmet Bakırcıoğlu; M Necmettin Pamir; Viviane Tabar; Alexander O Vortmeyer; Kaya Bilguvar; Katsuhito Yasuno; Lisa M DeAngelis; Joachim M Baehring; Jennifer Moliterno; Murat Günel Journal: Genome Med Date: 2017-02-02 Impact factor: 11.117