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Combined action of the dinuclear platinum compound BBR3610 with the PI3-K inhibitor PX-866 in glioblastoma.

Authors :
Gwak, Ho-Shin
Shingu, Takashi
Chumbalkar, Vaibhav
Hwang, Yeo-Hyeon
DeJournett, Robert
Latha, Khatri
Koul, Dimpy
Alfred Yung, W. K.
Powis, Garth
Farrell, Nicholas P.
Bögler, Oliver
Source :
International Journal of Cancer; Feb2011, Vol. 128 Issue 4, p787-796, 10p
Publication Year :
2011

Abstract

Polynuclear platinum compounds are more effective at killing glioblastoma cells than cisplatin, work by a different mechanism, and typically do not induce high levels of apoptosis at early time points after exposure. Here, we tested the hypothesis that combining BBR3610, the most potent polynuclear platinum, with a phosphoinositide-3-kinase (PI3K) inhibitor would promote apoptosis and enhance the impact on glioblastoma cells. The PI3K pathway is commonly activated in glioblastoma and promotes tumor cell survival, suggesting that its inhibition would make cells more sensitive to cytotoxic agents. We chose PX-866 as a PI3K inhibitor as it is a clinically promising agent being evaluated for brain tumor therapy. Combining BBR3610 and PX-866 resulted in synergistic killing of cultured glioma cells and an extension of survival in an orthotopic xenograft animal model. Both agents alone induced autophagy, and this appeared to be saturated, because when they were combined no additional autophagy was observed. However, the combination of PX-866 and BBR3610 did induce statistically significant increases in the level of apoptosis, associated with a reduction in pAkt and pBad, as well as inhibition of transwell migration. We conclude that combining polynuclear platinums with PI3K inhibitors has translational potential and alters the cellular response to include early apoptosis. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
00207136
Volume :
128
Issue :
4
Database :
Complementary Index
Journal :
International Journal of Cancer
Publication Type :
Academic Journal
Accession number :
62207060
Full Text :
https://doi.org/10.1002/ijc.25394