Abstract

We have assembled a complementary team of basic cancer geneticists, mouse biologists, neuropathologists, neuro-oncologists, developmental neurobiologists, neurologists, and genomics-bioinformatics specialists to delineate the critical events in the genesis, progression and maintenance of malignant glioma. Malignant gliomas are aggressive, highly invasive and neurologically destructive tumors considered to be among the deadliest of human cancers. In its most aggressive manifestation, glioblastoma, median survival ranges from 9 to 12 months -- a fact that has changed little over several decades. It is indeed notable that, despite detailed knowledge of glioma-associated gene mutations, we know precious little about how such mutations contribute to the unique biology of this tumor type, whether such lesions play roles in both tumor genesis and maintenance, which cellular compartments serve as target for or origin of the transformation process, and why malignant gliomas remain refractory to existing therapy. It is our belief that the proposed studies will lead to meaningful insights that promise to validate specific mutations as essential or non-essential therapeutic targets as well as to identify biomarkers that will aide in glioma classification and ultimately clinical management. This new P01 application rests upon the hypotheses that: (1) genetic mutations involved in tumor genesis remain relevant to tumor maintenance; (2) tumor-associated genetic lesions play specific and discernable roles which relate to the unique biological features of glioma; and (3) genes/pathways controlling normal glia cell proliferation, survival and differentiation also contribute the pathogenesis of glioma. Drs. DePinho and Maher will exploit the experimental merits of the mouse to dissect how cellular differentiation and specific RTK and tumor suppressor gene mutations contribute to glioma progression and maintenance. Drs. Cavenee and Furnari will evaluate the genetic interactions of EGFR and PTEN through the com-bined use of expression profiling, genetic screens and cross-species model comparisons. Using neural stem cell technology and functional genomics, Drs. Rowitch and Bachoo will evaluate the role of key glioma-relevant mutations in the growth, survival and differentiation processes of normal glia. These projects will be aided by cores for Transgenic Mice and Neural Stem Cells (DePinho), Neuropathology (Louis), Genomics-Bioinformatics (Chin/Wong), and Administration (DePinho). The goals of this P01 mirror precisely the priorities articulated by the recent NCI/NINDS Brain Tumor PRG.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
1P01CA095616-01A1
Application #
6559455
Study Section
Subcommittee G - Education (NCI)
Program Officer
Mohla, Suresh
Project Start
2003-03-10
Project End
2008-02-29
Budget Start
2003-03-10
Budget End
2004-02-29
Support Year
1
Fiscal Year
2003
Total Cost
$1,627,903
Indirect Cost

  Institution

Name
Dana-Farber Cancer Institute
Department
Type
DUNS #
076580745
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Reardon, Colin; Murray, Kaitlin; Lomax, Alan E (2018) Neuroimmune Communication in Health and Disease. Physiol Rev 98:2287-2316
Roncali, Emilie; Stockhoff, Mariele; Cherry, Simon R (2017) An integrated model of scintillator-reflector properties for advanced simulations of optical transport. Phys Med Biol 62:4811-4830
Nanavaty, Vishal; Sandhu, Ranjodh; Jehi, Sanaa E et al. (2017) Trypanosoma brucei RAP1 maintains telomere and subtelomere integrity by suppressing TERRA and telomeric RNA:DNA hybrids. Nucleic Acids Res 45:5785-5796
Leonard, Paul G; Satani, Nikunj; Maxwell, David et al. (2016) SF2312 is a natural phosphonate inhibitor of enolase. Nat Chem Biol 12:1053-1058
Hiu, Takeshi; Farzampour, Zoya; Paz, Jeanne T et al. (2016) Enhanced phasic GABA inhibition during the repair phase of stroke: a novel therapeutic target. Brain 139:468-80
Gilhooly, Neville S; Carrasco, Carolina; Gollnick, Benjamin et al. (2016) Chi hotspots trigger a conformational change in the helicase-like domain of AddAB to activate homologous recombination. Nucleic Acids Res 44:2727-41
Liu, Rui; Yang, Guang; Zhou, Meng-Hua et al. (2016) Flotillin-1 downregulates K(+) current by directly coupling with Kv2.1 subunit. Protein Cell 7:455-60
Schrager-Lavelle, Amanda; Herrera, Leslie A; Maloof, Julin N (2016) Tomato phyE Is Required for Shade Avoidance in the Absence of phyB1 and phyB2. Front Plant Sci 7:1275
Hu, Baoli; Wang, Qianghu; Wang, Y Alan et al. (2016) Epigenetic Activation of WNT5A Drives Glioblastoma Stem Cell Differentiation and Invasive Growth. Cell 167:1281-1295.e18
Poornima, Gopalakrishna; Shah, Shanaya; Vignesh, Venkadasubramanian et al. (2016) Arginine methylation promotes translation repression activity of eIF4G-binding protein, Scd6. Nucleic Acids Res 44:9358-9368

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