Abstract

Amplification of EGFR, with or without mutation, occurs in 40% of primary GBM tumors, and at least in this subset of tumors, elevated signaling from EGFR presumably plays a central role in the malignant character of these radiation resistant tumors. This relationship between EGFR amplification and malignant behavior has been well-documented, and, therefore, it is not surprising that several clinical trials are investigating the efficacy of EGFR inhibitors in GBM. However, it is not known whether the presence or absence of EGFR amplification is predictive of tumor sensitivity to EGFR-directed therapies. At Mayo Clinic, 2 Phase II clinical trials are being run through the North Central Cancer Treatment Group (NCCTG) to evaluate the efficacy of small molecule EGFR kinase inhibitors in GBM. Tissue specimens from these trials, which are evaluating radiation combined with sequential (N0074) or concomitant (N0177) EGFR inhibitor therapy, will be available for correlative studies, as will an extensive GBM tissue archive from patients treated with radiation alone. In addition, we have established a panel of serially transplantable GBM xenografts that maintain the original EGFR amplification status and the histopathologic and invasive features of their derivative GBM tumors. Using these resources, this project will identify molecular characteristics that predict for response to EGFR inhibitor therapy. We hypothesize that the anti-tumor effects of EGFR inhibitors result from suppression of a select subset of 1 or 2 essential pathways, and that resistance to EGFR inhibitor therapy results from compensatory signaling through these pathways caused by other GBM gene alterations (e.g. PTEN mutation). Thus, accurate prediction of sensitivity to EGFR inhibition may require information regarding the status of several molecular characteristics including EGFR amplification and mutation status. To succeed in identifying a predictive molecular fingerprint for sensitivity to EGFR inhibitor therapy in GBM, the following approach will be used.
In Aim 1, we will examine tissue specimens collected from patients treated with a) radiation and concomitant OSI-774 on N0177, b) radiation followed by ZD1839 on N0074, and c) radiation alone.
In Aim 2, we will examine serially transplantable orthotopic GBM xenografts to identify EGFR-dependent signaling pathways that are sensitive to OSI-774 therapy.
In Aim 3, we will test whether the efficacy of EGFR inhibitor therapy can be enhanced by simultaneous inhibition of the mammalian target of rapamycin in orthotopic GBM xenografts. Collectively, the studies in this application will enhance our understanding of the molecular pharmacology of EGFR inhibitor therapy and will provide the scientific basis of customization of EGFR inhibitor therapies on the basis of molecular tumor characteristics.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center (P50)
Project #
5P50CA108961-03
Application #
7285248
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2006-09-01
Budget End
2007-08-31
Support Year
3
Fiscal Year
2006
Total Cost
$129,052
Indirect Cost

  Institution

Name
Mayo Clinic, Rochester
Department
Type
DUNS #
006471700
City
Rochester
State
MN
Country
United States
Zip Code
55905

  Publications

Jung, Mi-Yeon; Kang, Jeong-Han; Hernandez, Danielle M et al. (2018) Fatty acid synthase is required for profibrotic TGF-? signaling. FASEB J 32:3803-3815
Msaouel, Pavlos; Opyrchal, Mateusz; Dispenzieri, Angela et al. (2018) Clinical Trials with Oncolytic Measles Virus: Current Status and Future Prospects. Curr Cancer Drug Targets 18:177-187
Zhou, Dan; Alver, Bonnie M; Li, Shuang et al. (2018) Distinctive epigenomes characterize glioma stem cells and their response to differentiation cues. Genome Biol 19:43
Vaubel, Rachael A; Caron, Alissa A; Yamada, Seiji et al. (2018) Recurrent copy number alterations in low-grade and anaplastic pleomorphic xanthoastrocytoma with and without BRAF V600E mutation. Brain Pathol 28:172-182
Chen, Xiaoyue; Zhang, Minjie; Gan, Haiyun et al. (2018) A novel enhancer regulates MGMT expression and promotes temozolomide resistance in glioblastoma. Nat Commun 9:2949
Nowsheen, Somaira; Aziz, Khaled; Aziz, Asef et al. (2018) L3MBTL2 orchestrates ubiquitin signalling by dictating the sequential recruitment of RNF8 and RNF168 after DNA damage. Nat Cell Biol 20:455-464
Chen, Jee-Wei E; Pedron, Sara; Shyu, Peter et al. (2018) Influence of Hyaluronic Acid Transitions in Tumor Microenvironment on Glioblastoma Malignancy and Invasive Behavior. Front Mater 5:
Youland, Ryan S; Pafundi, Deanna H; Brinkmann, Debra H et al. (2018) Prospective trial evaluating the sensitivity and specificity of 3,4-dihydroxy-6-[18F]-fluoro-L-phenylalanine (18F-DOPA) PET and MRI in patients with recurrent gliomas. J Neurooncol 137:583-591
Stathias, Vasileios; Jermakowicz, Anna M; Maloof, Marie E et al. (2018) Drug and disease signature integration identifies synergistic combinations in glioblastoma. Nat Commun 9:5315
Huff, Amanda L; Wongthida, Phonphimon; Kottke, Timothy et al. (2018) APOBEC3 Mediates Resistance to Oncolytic Viral Therapy. Mol Ther Oncolytics 11:1-13

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