Anti-proliferative activity of the quassinoid NBT-272 in childhood medulloblastoma cells

Anti-proliferative activity of the quassinoid NBT-272 in childhood medulloblastoma cells

With current treatment strategies, nearly half of all medulloblastoma (MB) patients die from progressive tumors. Accordingly, the identification of novel therapeutic strategies remains a major goal. Deregulation of c-MYC is evident in numerous human cancers. In MB, over-expression of c-MYC has been...

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Veröffentlicht in:BMC cancer 2007-01, Vol.7 (1), p.19-19, Article 19
Hauptverfasser: von Bueren, André O, Shalaby, Tarek, Rajtarova, Julia, Stearns, Duncan, Eberhart, Charles G, Helson, Lawrence, Arcaro, Alexandre, Grotzer, Michael A
Format: Artikel
Sprache:eng
Schlagworte:
Cell Line, Tumor
Cell Proliferation - drug effects
Cerebellar Neoplasms - drug therapy
Cerebellar Neoplasms - metabolism
Cerebellar Neoplasms - pathology
Child
DNA-Binding Proteins - antagonists & inhibitors
DNA-Binding Proteins - biosynthesis
Dose-Response Relationship, Drug
Growth Inhibitors - pharmacology
Growth Inhibitors - therapeutic use
Humans
Medulloblastoma - drug therapy
Medulloblastoma - metabolism
Medulloblastoma - pathology
Quassins - pharmacology
Quassins - therapeutic use
Transcription Factors - antagonists & inhibitors
Transcription Factors - biosynthesis
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Zusammenfassung:With current treatment strategies, nearly half of all medulloblastoma (MB) patients die from progressive tumors. Accordingly, the identification of novel therapeutic strategies remains a major goal. Deregulation of c-MYC is evident in numerous human cancers. In MB, over-expression of c-MYC has been shown to correlate with anaplasia and unfavorable prognosis. In neuroblastoma--an embryonal tumor with biological similarities to MB--the quassinoid NBT-272 has been demonstrated to inhibit cellular proliferation and to down-regulate c-MYC protein expression. To study MB cell responses to NBT-272 and their dependence on the level of c-MYC expression, DAOY (wild-type, empty vector transfected or c-MYC transfected), D341 (c-MYC amplification) and D425 (c-MYC amplification) human MB cells were used. The cells were treated with different concentrations of NBT-272 and the impact on cell proliferation, apoptosis and c-MYC expression was analyzed. NBT-272 treatment resulted in a dose-dependent inhibition of cellular proliferation (IC50 in the range of 1.7-9.6 ng/ml) and in a dose-dependent increase in apoptotic cell death in all human MB cell lines tested. Treatment with NBT-272 resulted in up to 90% down-regulation of c-MYC protein, as demonstrated by Western blot analysis, and in a significant inhibition of c-MYC binding activity. Anti-proliferative effects were slightly more prominent in D341 and D425 human MB cells with c-MYC amplification and slightly more pronounced in c-MYC over-expressing DAOY cells compared to DAOY wild-type cells. Moreover, treatment of synchronized cells by NBT-272 induced a marked cell arrest at the G1/S boundary. In human MB cells, NBT-272 treatment inhibits cellular proliferation at nanomolar concentrations, blocks cell cycle progression, induces apoptosis, and down-regulates the expression of the oncogene c-MYC. Thus, NBT-272 may represent a novel drug candidate to inhibit proliferation of human MB cells in vivo.
ISSN:1471-2407
1471-2407
DOI:10.1186/1471-2407-7-19