Spatial immunosampling of MRI-defined glioblastoma regions reveals immunologic fingerprint of non-contrast enhancing, infiltrative tumor margins.
Matthew M GrabowskiDionysios C WatsonKunho ChungJuyeun LeeDefne BayikAdam LaukoTyler AlbanJan Joseph MelenhorstTimothy ChanJustin D LathiaManmeet S AhluwaliaAlireza M MohammadiPublished in: medRxiv : the preprint server for health sciences (2023)
Glioblastoma (GBM) treatment includes maximal safe resection of the core and MRI contrast-enhancing (CE) tumor. Complete resection of the infiltrative non-contrast-enhancing (NCE) tumor rim is rarely achieved. We established a safe, semi-automated workflow for spatially-registered sampling of MRI-defined GBM regions in 19 patients with downstream analysis and biobanking, enabling studies of NCE, wherefrom recurrence/progression typically occurs. Immunophenotyping revealed underrepresentation of myeloid cell subsets and CD8+ T cells in the NCE. While NCE T cells phenotypically and functionally resembled those in matching CE tumor, subsets of activated (CD69 hi ) effector memory CD8+ T cells were overrepresented. Contrarily, CD25 hi Tregs and other subsets were underrepresented. Overall, our study demonstrated that MRI-guided, spatially-registered, intraoperative immunosampling is feasible as part of routine GBM surgery. Further elucidation of the shared and spatially distinct microenvironmental biology of GBM will enable development of therapeutic approaches targeting the NCE infiltrative tumor to decrease GBM recurrence.
Keyphrases
- contrast enhanced
- magnetic resonance imaging
- magnetic resonance
- diffusion weighted imaging
- peripheral blood
- single cell
- minimally invasive
- machine learning
- stem cells
- computed tomography
- immune response
- dendritic cells
- drug delivery
- cell therapy
- deep learning
- heart rate
- high throughput
- coronary artery disease
- coronary artery bypass
- clinical practice
- atrial fibrillation
- free survival
- data analysis