Abstract

Project 1 will follow up on initial observations that the diffuse character of these tumors is not simply due to the tumor cells migrating into the normal brain structures as had been previously thought but that the tumor actively recruits surrounding cells from the brain (brain stroma) and other sources into the tumor mass and induces their aberrant proliferation. These recruited stem/progenitor cells may function normally in the response to injury in a self-limiting manner. We will use lineage tracing combined with oncogenesis to genetically distinguish the progeny of the original tumor cells (marked by GFP expression) from the recruited cells. We will additionally use bioluminescence imaging to monitor the signaling activity of pathways known to drive stem/progenitor character in these recruited cells in slice preparations of tumors in situ. We have created reporter mice that express luciferase proportional to SHH, Wnt, and Notch signaling activity.
In Aim 1 we will determine the location from which the recruited cells arise, specifically the bone marrow and brain contribution. Our preliminary data indicates that a high percent of cells within gliomas are not derived from the original cell of origin and are recruited from other locations.
In Aim 2 we will determine whether loss of the known glioma tumor suppressors (INK4a, Arf, PTEN) will promote the incorporation and contribution of recruited cells to the tumor proper. In theory the recruited cells could acquire mutations independent from those found in the progeny of the cell of origin, and the cells making up the most malignant tumors could be derived from recruited cells.
In Aim 3 we will determine if the Gli-luc mouse line can be used for bioluminescence imaging to visualize recruitment and SHH signaling in gliomas overtime. The signaling pathways that attract recruited progenitor cells to the tumor and maintain them in proliferative and undifferentiated state are unknown.
Aim 4 we will determine if the SHH signaling and cell recruitment is a response to injury. Our preliminary data indicates that SHH signaling in gliomas is an in vivo phenomenon and that it may be a dysregulated response to injury that normally is tightly controlled temporally. We will systematically determine if SHH activation is part of a normal response to injury and if the alterations found in human gliomas that are known to induce gliomas in mice alter this effect.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center--Cooperative Agreements (U54)
Project #
5U54CA126518-04
Application #
7666262
Study Section
Special Emphasis Panel (ZCA1-SRRB-3 (O1))
Program Officer
Mohla, Suresh
Project Start
2006-09-20
Project End
2011-08-31
Budget Start
2009-09-01
Budget End
2010-08-31
Support Year
4
Fiscal Year
2009
Total Cost
$1,503,474
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

Pietras, Alexander; Katz, Amanda M; Ekström, Elin J et al. (2014) Osteopontin-CD44 signaling in the glioma perivascular niche enhances cancer stem cell phenotypes and promotes aggressive tumor growth. Cell Stem Cell 14:357-69
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
Sevenich, Lisa; Bowman, Robert L; Mason, Steven D et al. (2014) Analysis of tumour- and stroma-supplied proteolytic networks reveals a brain-metastasis-promoting role for cathepsin S. Nat Cell Biol 16:876-88
Pyonteck, Stephanie M; Akkari, Leila; Schuhmacher, Alberto J et al. (2013) CSF-1R inhibition alters macrophage polarization and blocks glioma progression. Nat Med 19:1264-72
Quail, Daniela F; Joyce, Johanna A (2013) Microenvironmental regulation of tumor progression and metastasis. Nat Med 19:1423-37
Charles, Nikki A; Holland, Eric C; Gilbertson, Richard et al. (2012) The brain tumor microenvironment. Glia 60:502-14
Pyonteck, S M; Gadea, B B; Wang, H-W et al. (2012) Deficiency of the macrophage growth factor CSF-1 disrupts pancreatic neuroendocrine tumor development. Oncogene 31:1459-67
Helmy, Karim; Halliday, John; Fomchenko, Elena et al. (2012) Identification of global alteration of translational regulation in glioma in vivo. PLoS One 7:e46965
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
Mason, Steven D; Joyce, Johanna A (2011) Proteolytic networks in cancer. Trends Cell Biol 21:228-37

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