Abstract

Gliomas including glioblastoma (GBM) are the most common primary malignant brain tumors. Glioma extracellular vesicles (EVs) including exosomes have biological effects (e.g., immunosuppression) and contain tumor-specific cargo that could facilitate liquid biopsies. We aimed to develop a simple, reproducible technique to isolate plasma exosomes in glioma patients. Glioma patients' and normal donors' plasma exosomes underwent brief centrifugation to remove cells/debris followed by serial density gradient ultracentrifugation (DGU). EV size/concentration was determined by nanoparticle tracking. Protein cargo was screened by array, western blot, and ELISA. Nanoscale flow cytometry analysis quantified exosome and microvesicle populations pre- and post-DGU. One-step DGU efficiently isolates exosomes for nanoparticle tracking. Wild type isocitrate dehydrogenase glioma patients' (i.e., more aggressive tumors) plasma exosomes are smaller but higher concentration than normal donors. A second DGU efficiently concentrates exosomes for subsequent cargo analysis but results in vesicle aggregation that skews nanoparticle tracking. Cytokines and co-stimulatory molecules are readily detected but appeared globally reduced in GBM patients' exosomes. Surprisingly, immunosuppressive programmed death-ligand 1 (PD-L1) is present in both patients' and normal donors' exosomes. Nanoscale flow cytometry confirms efficient exosome (<100 nm) isolation post-DGU but also demonstrates increase in microvesicles (>100 nm) in GBM patients' plasma pre-DGU. Serial DGU efficiently isolates plasma exosomes with distinct differences between GBM patients and normal donors, suggesting utility for non-invasive biomarker assessment. Initial results suggest global immunosuppression rather than increased circulating tumor-derived immunosuppressive exosomes, though further assessment is needed. Increased glioma patients' plasma microvesicles suggest these may also be a key source for biomarkers.

Highlights

  • Gliomas, including glioblastoma (GBM), are the most common malignant brain tumors and are highly lethal [1]

  • Exosomes isolated by one-step density gradient ultracentrifugation (DGU) are physically smaller but more abundant than exosomes isolated by two-step DGU for both normal donors (Figures 2B,C) and glioma patients (Figures 2E,F; Supplementary Videos)

  • Our findings demonstrate that DGU is a practical method to isolate plasma exosomes in GBM patients

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Summary

Introduction

Gliomas, including glioblastoma (GBM), are the most common malignant brain tumors and are highly lethal [1]. Post-operative imaging is performed to evaluate the extent of surgical resection and tumor progression. MRI can be difficult to interpret after treatment due to inflammation and necrosis in response to radiation, chemotherapy, or immunotherapy. False positive MRI due to treatment-related inflammation called “pseudo-progression” occurs frequently [7, 8] and makes clinical interpretation challenging [9]. Given this limitation, there is a definitive need for improved, non-invasive methods for GBM diagnosis and monitoring. There is a definitive need for improved, non-invasive methods for GBM diagnosis and monitoring Such a method would just involve a simple blood draw

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