Abstract

Glioblastomas have markedly elevated activity of signal transduction pathways relative to low-grade gliomas. Analysis of human glioma samples using Western blot analysis with antibodies specific for the activated forms of these signaling components demonstrates that all of the GBMs show elevated levels of Erk. These data strongly indicate that the downstream readout of Ras in these tumors in vivo is through Raf, MEK, and Erk. Akt activity is elevated in about 60% of GBMs and is associated with phosphorylation of S6 kinase and 4EBP, both of which are downstream of mTOR. The elevation of activity of these proteins relative to normal brain or lower-grade gliomas is striking and alone suggests that these signaling pathways may be causally related to the formation of gliomas. The proof that the activity of these pathways can actually cause GBM is derived from mouse modeling studies with the RCAS/tv-a system where the combination of activated Ras and Akt results in the formation of GBMs in mice. Therefore, not only are these pathways elevated in human GBMs but also experimental elevation of these pathways in mice results in the formation of a very similar tumor. From these data we hypothesize that the signaling pathways are the etiology of at least some GBMs in humans. We propose to investigate three major specific questions that will be addressed in eight limited specific aims in this project. The first major question is whether the oncogenic effect of Ras in the formation of glioblastoma proceeds through Raf, Mek, and Erk. Specifically whether this pathway is necessary and sufficient for Ras activity in this context. The second major question is whether EGFR activity and PTEN loss functions through Akt and mTOR and whether mTOR activity is necessary and sufficient for the oncogenic effects of elevated Akt activity in glioblastomas. The critical importance of these first two questions relates to the available small molecule inhibitors that are currently in clinical trials. These drugs are specific for certain components within these signaling pathways but we do not know if these pathways are actually the oncogenic effectors for the formation of gliomas. In this grant we will address these questions using the RCAS/tv-a mouse modeling system for Ras + Akt-induced gliomas. ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA100688-03
Application #
6883935
Study Section
Special Emphasis Panel (ZRG1-CAMP (01))
Program Officer
Mietz, Judy
Project Start
2003-04-10
Project End
2008-03-31
Budget Start
2005-04-01
Budget End
2006-03-31
Support Year
3
Fiscal Year
2005
Total Cost
$352,663
Indirect Cost

  Institution

Name
Sloan-Kettering Institute for Cancer Research
Department
Type
DUNS #
064931884
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Ozawa, Tatsuya; Arora, Sonali; Szulzewsky, Frank et al. (2018) A De Novo Mouse Model of C11orf95-RELA Fusion-Driven Ependymoma Identifies Driver Functions in Addition to NF-?B. Cell Rep 23:3787-3797
Pattwell, Siobhan S; Holland, Eric C (2017) Putting Glioblastoma in Its Place: IRF3 Inhibits Invasion. Trends Mol Med 23:773-776
Pitter, Kenneth L; Tamagno, Ilaria; Alikhanyan, Kristina et al. (2016) Corticosteroids compromise survival in glioblastoma. Brain 139:1458-71
Halliday, John; Helmy, Karim; Pattwell, Siobhan S et al. (2014) In vivo radiation response of proneural glioma characterized by protective p53 transcriptional program and proneural-mesenchymal shift. Proc Natl Acad Sci U S A 111:5248-53
Leder, Kevin; Pitter, Ken; LaPlant, Quincey et al. (2014) Mathematical modeling of PDGF-driven glioblastoma reveals optimized radiation dosing schedules. Cell 156:603-616
Ozawa, Tatsuya; Riester, Markus; Cheng, Yu-Kang et al. (2014) Most human non-GCIMP glioblastoma subtypes evolve from a common proneural-like precursor glioma. Cancer Cell 26:288-300
Helmy, Karim; Halliday, John; Fomchenko, Elena et al. (2012) Identification of global alteration of translational regulation in glioma in vivo. PLoS One 7:e46965
Katz, Amanda M; Amankulor, Nduka M; Pitter, Ken et al. (2012) Astrocyte-specific expression patterns associated with the PDGF-induced glioma microenvironment. PLoS One 7:e32453
Jones, T S; Holland, E C (2012) Standard of care therapy for malignant glioma and its effect on tumor and stromal cells. Oncogene 31:1995-2006
Bazzoli, Elena; Pulvirenti, Teodoro; Oberstadt, Moritz C et al. (2012) MEF promotes stemness in the pathogenesis of gliomas. Cell Stem Cell 11:836-44

Showing the most recent 10 out of 36 publications