A non-local diffusion magnetic resonance imaging tract density biomarker to stratify, predict, and interpret survival rates in human glioblastoma
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This article is not in any list yet, why not save it to one of your lists.Abstract
Glioblastoma (GBM) is a lethal tumor, actively growing and invading neighboring neural tissue. GBMs appear functionally connected to distributed and spatially distant regions rather than representing an isolated and passive lesion disrupting the brain circuitry. Moreover, increasing evidence suggests that white matter serves as the morphological substrate for GBM to progress and migrate to distant areas in the human brain.
Methods
We hypothesized that the subset of white matter tracts intersecting the tumors depict the physical substrate for large-scale neuron-glioma interactions and would therefore inform prognosis. Using normative models, we design, analyze, interpret, and test a Lesion-Tract Density Index (L-TDI) marker that considers the distributed white matter pathways interacting with the tumor in two independent cohorts of N = 367 and N = 496 patients, respectively.
Results
First, we show that the average tract density within this white matter map robustly stratifies survival rates due to widespread white matter involvement. Second, we demonstrate why tract density-based markers offer critical and necessary insights into the morphology, location, and evolution of human GBM by proving how the proposed L-TDI implicitly considers tumor volume, white matter density, and location. We provide further evidence that the non-uniform distribution of GBMs and their differential prognosis emerge from white matter morphology. Third, we validate the L-TDI marker with multiple Cox survival models and analyze its contribution in relation to other covariates of interest (e.g., MGMT promoter methylation). Lastly, by using a simple logistic model, we predict patient death at 12 months with balanced accuracies of 0.68 and 0.65, and areas under the curve of 0.74 and 0.73 when training and testing in separate and independent cohorts.
Conclusions
Overall, we offer a concrete implementation of the emerging paradigm that views GBM not as a focal lesion, but as a network disease shaped by its complex interactions with distant brain regions.
