Abstract

Gliomas are uniformly fatal primary brain tumors, the diagnosis of which has been greatly impacted by improvements in medical imaging techniques over the last several decades. However, a significant gap remains between the obvious goal of more effective therapy and the present understanding of the dynamics of the tumor's proliferation and invasion in humans in vivo. That gap pivots on the concept that treatment of gliomas fails because of the diffuse dispersal of glioma cells throughout the neural axis even before diagnosis: the spatial and temporal evolution of which has been shown to be of quantitative and clinical importance as well as predicable with our current modeling methodology. Further, every imaging technique has a threshold of detection leaving much of the dispersed tumor invisible on imaging. The long-term objectives of this proposal are to provide new tools designed to quantify and predict the net proliferation and dispersal of glioma cells accurately enough to quantify and predict response to radiation therapy that are validated by and compared against information obtained through routine medical imaging of individual patients.
The specific aims are to investigate the use of a spatio-temporal bio-mathematical model as a metric for glioma concentration, dispersal, response to radiation therapy, and location of post-treatment recurrence of individual gliomas in living patients in sufficient time to impact clinical decision making. This involves a gross but necessary assumption that medical imaging such as T1-weighted, gadolinium enhanced, T2-weighted MRI and PET imaging techniques directly correlate with disease distribution and biology. As the primary clinical window into disease progression, imaging techniques are used as benchmarks and metrics against which accuracy and success of model predictions are measured. Methods involve modern techniques and tools including, co-registration of clinical imaging, 3D radiation dose- distribution maps and the 4D patient-specific, model-simulated movie of the spatio-temporal growth and dispersal of each glioma. Comparisons are made between the model predicted invasion and therapy response patterns and that observed on follow-up imaging and, ultimately, autopsy.

Public Health Relevance

The relevance of this proposal to public health lies in its applicability to any individual patient (and to the composition of any proposed group of """"""""similar"""""""" patients) who has a primary brain tumor (glioma) and is being treated or is being considered for radiation therapy. Since disease progression and response to therapy are largely gauged by changes in current imaging techniques, there is an inherent limit to the clinical observation of a glioma to a """"""""tip of the iceberg"""""""" view. Tools to predict and assess the dispersal (invasion) of gliomas cells throughout the brain in addition to the response to therapy which we cannot view on imaging is essential to the development of new and effective therapies for this uniformly fatal tumor. Specifically, as radiation therapy is targeted towards the dispersed glioma cells, peripheral to the imaging abnormality, it is necessary to calculate beyond the limits of imaging and to design mathematical models to dynamically assess that component of the tumor as well as take advantage of the tumor's proliferation rate in real time and in real patients.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS060752-02
Application #
7905757
Study Section
Radiation Therapeutics and Biology Study Section (RTB)
Program Officer
Fountain, Jane W
Project Start
2009-08-05
Project End
2014-07-31
Budget Start
2010-08-01
Budget End
2011-07-31
Support Year
2
Fiscal Year
2010
Total Cost
$329,423
Indirect Cost

  Institution

Name
University of Washington
Department
Pathology
Type
Schools of Medicine
DUNS #
605799469
City
Seattle
State
WA
Country
United States
Zip Code
98195

  Publications

Jackson, Pamela R; Juliano, Joseph; Hawkins-Daarud, Andrea et al. (2015) Patient-specific mathematical neuro-oncology: using a simple proliferation and invasion tumor model to inform clinical practice. Bull Math Biol 77:846-56
Rockne, Russell C; Trister, Andrew D; Jacobs, Joshua et al. (2015) A patient-specific computational model of hypoxia-modulated radiation resistance in glioblastoma using 18F-FMISO-PET. J R Soc Interface 12:
Baldock, Anne L; Yagle, Kevin; Born, Donald E et al. (2014) Invasion and proliferation kinetics in enhancing gliomas predict IDH1 mutation status. Neuro Oncol 16:779-86
Adair, Jennifer E; Johnston, Sandra K; Mrugala, Maciej M et al. (2014) Gene therapy enhances chemotherapy tolerance and efficacy in glioblastoma patients. J Clin Invest 124:4082-92
Baldock, Anne L; Ahn, Sunyoung; Rockne, Russell et al. (2014) Patient-specific metrics of invasiveness reveal significant prognostic benefit of resection in a predictable subset of gliomas. PLoS One 9:e99057
Corwin, David; Holdsworth, Clay; Rockne, Russell C et al. (2013) Toward patient-specific, biologically optimized radiation therapy plans for the treatment of glioblastoma. PLoS One 8:e79115
Neal, Maxwell Lewis; Trister, Andrew D; Cloke, Tyler et al. (2013) Discriminating survival outcomes in patients with glioblastoma using a simulation-based, patient-specific response metric. PLoS One 8:e51951
Baldock, A L; Rockne, R C; Boone, A D et al. (2013) From patient-specific mathematical neuro-oncology to precision medicine. Front Oncol 3:62
Hawkins-Daarud, Andrea; Rockne, Russell C; Anderson, Alexander R A et al. (2013) Modeling Tumor-Associated Edema in Gliomas during Anti-Angiogenic Therapy and Its Impact on Imageable Tumor. Front Oncol 3:66
Neal, Maxwell Lewis; Trister, Andrew D; Ahn, Sunyoung et al. (2013) Response classification based on a minimal model of glioblastoma growth is prognostic for clinical outcomes and distinguishes progression from pseudoprogression. Cancer Res 73:2976-86

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