%0 Journal Article %1 Stringfield:2019:Tomography:30854451 %A Stringfield, O %A Arrington, J A %A Johnston, S K %A Rognin, N G %A Peeri, N C %A Balagurunathan, Y %A Jackson, P R %A Clark-Swanson, K R %A Swanson, K R %A Egan, K M %A Gatenby, R A %A Raghunand, N %D 2019 %J Tomography %K cancer-research evolution gatenby glioblastoma shouldread wired %N 1 %P 135-144 %R 10.18383/j.tom.2018.00052 %T Multiparameter MRI Predictors of Long-Term Survival in Glioblastoma Multiforme %U https://www.ncbi.nlm.nih.gov/pubmed/30854451 %V 5 %X Standard-of-care multiparameter magnetic resonance imaging (MRI) scans of the brain were used to objectively subdivide glioblastoma multiforme (GBM) tumors into regions that correspond to variations in blood flow, interstitial edema, and cellular density. We hypothesized that the distribution of these distinct tumor ecological "habitats" at the time of presentation will impact the course of the disease. We retrospectively analyzed initial MRI scans in 2 groups of patients diagnosed with GBM, a long-term survival group comprising subjects who survived >36 month postdiagnosis, and a short-term survival group comprising subjects who survived ≤19 month postdiagnosis. The single-institution discovery cohort contained 22 subjects in each group, while the multi-institution validation cohort contained 15 subjects per group. MRI voxel intensities were calibrated, and tumor voxels clustered on contrast-enhanced T1-weighted and fluid-attenuated inversion-recovery (FLAIR) images into 6 distinct "habitats" based on low- to medium- to high-contrast enhancement and low-high signal on FLAIR scans. Habitat 6 (high signal on calibrated contrast-enhanced T1-weighted and FLAIR sequences) comprised a significantly higher volume fraction of tumors in the long-term survival group (discovery cohort, 35% ± 6.5%; validation cohort, 34% ± 4.8%) compared with tumors in the short-term survival group (discovery cohort, 17% ± 4.5%, P < .03; validation cohort, 16 ± 4.0%, P < .007). Of the 6 distinct MRI-defined habitats, the fractional tumor volume of habitat 6 at diagnosis was significantly predictive of long- or short-term survival. We discuss a possible mechanistic basis for this association and implications for habitat-driven adaptive therapy of GBM.

@article{Stringfield:2019:Tomography:30854451, abstract = {Standard-of-care multiparameter magnetic resonance imaging (MRI) scans of the brain were used to objectively subdivide glioblastoma multiforme (GBM) tumors into regions that correspond to variations in blood flow, interstitial edema, and cellular density. We hypothesized that the distribution of these distinct tumor ecological "habitats" at the time of presentation will impact the course of the disease. We retrospectively analyzed initial MRI scans in 2 groups of patients diagnosed with GBM, a long-term survival group comprising subjects who survived >36 month postdiagnosis, and a short-term survival group comprising subjects who survived ≤19 month postdiagnosis. The single-institution discovery cohort contained 22 subjects in each group, while the multi-institution validation cohort contained 15 subjects per group. MRI voxel intensities were calibrated, and tumor voxels clustered on contrast-enhanced T1-weighted and fluid-attenuated inversion-recovery (FLAIR) images into 6 distinct "habitats" based on low- to medium- to high-contrast enhancement and low-high signal on FLAIR scans. Habitat 6 (high signal on calibrated contrast-enhanced T1-weighted and FLAIR sequences) comprised a significantly higher volume fraction of tumors in the long-term survival group (discovery cohort, 35% ± 6.5%; validation cohort, 34% ± 4.8%) compared with tumors in the short-term survival group (discovery cohort, 17% ± 4.5%, P < .03; validation cohort, 16 ± 4.0%, P < .007). Of the 6 distinct MRI-defined habitats, the fractional tumor volume of habitat 6 at diagnosis was significantly predictive of long- or short-term survival. We discuss a possible mechanistic basis for this association and implications for habitat-driven adaptive therapy of GBM.}, added-at = {2019-03-25T21:44:17.000+0100}, author = {Stringfield, O and Arrington, J A and Johnston, S K and Rognin, N G and Peeri, N C and Balagurunathan, Y and Jackson, P R and Clark-Swanson, K R and Swanson, K R and Egan, K M and Gatenby, R A and Raghunand, N}, biburl = {https://www.bibsonomy.org/bibtex/21e24b38102a1ae714b700ca731bdac7b/marcsaric}, description = {Multiparameter MRI Predictors of Long-Term Survival in Glioblastoma Multiforme. - PubMed - NCBI}, doi = {10.18383/j.tom.2018.00052}, interhash = {781b37b24f6d9f53ed20b287fe82c875}, intrahash = {1e24b38102a1ae714b700ca731bdac7b}, journal = {Tomography}, keywords = {cancer-research evolution gatenby glioblastoma shouldread wired}, month = mar, number = 1, pages = {135-144}, pmid = {30854451}, timestamp = {2019-03-25T21:44:17.000+0100}, title = {Multiparameter MRI Predictors of Long-Term Survival in Glioblastoma Multiforme}, url = {https://www.ncbi.nlm.nih.gov/pubmed/30854451}, volume = 5, year = 2019 }