What question did this study set out to answer?

To assess how small and large extracellular vesicles from glioblastoma impact endothelial function and mitochondrial activity.

April 17, 2026Open Access

Small and medium/large glioblastoma extracellular vesicles differentially regulate endothelial and mitochondrial function in blood–brain barrier and peripheral vasculature models

Key Points

To assess how small and large extracellular vesicles from glioblastoma impact endothelial function and mitochondrial activity.
Investigated effects of small and medium/large EVs derived from GBM on endothelial cell types.
Assessed endothelial barrier integrity using transendothelial electrical resistance.
Evaluated cell migration with wound healing assays and angiogenic capacity by tube formation analysis.
Measured mitochondrial function via oxygen consumption rate in endothelial cells.
sEVs impaired endothelial barrier integrity significantly, shown by reduced TEER and disrupted tight junctions.
m/lEVs enhanced endothelial cell migration but suppressed tube formation, leading to disorganized capillary structures.
m/lEVs selectively suppressed mitochondrial respiration in blood-brain barrier endothelial cells without affecting peripheral endothelial cells.

Abstract

Extracellular vesicles (EVs) released by glioblastoma (GBM) cells circulate systemically and modulate tumour-host interactions, influencing vascular function both within and beyond the tumour microenvironment. The EVs span a size range from tens to hundreds of nanometres; however, the specific effects of distinct GBM-derived EV size subpopulations on endothelial function across different endothelial cell types remain poorly understood. In this study, we investigated the effects of enriched small EVs (sEV) and medium/large EVs (m/lEV) fractions derived from human GBM cell line HROG36 on endothelial barrier integrity (assessed by transendothelial electrical resistance (TEER) and tight junction (TJ) protein analysis), migration (wound healing assay), angiogenic capacity (tube formation on extracellular matrix), and mitochondrial function (assessed by measuring the oxygen consumption rate (OCR)) in human brain microvascular endothelial cells (hCMEC/D3), representing blood–brain barrier (BBB) model, and peripheral endothelial cells (HUVECs). We show that sEV-enriched fractions significantly impaired endothelial barrier integrity in both cell types, as evidenced by reduced TEER and disrupted TJ protein organisation. In contrast, m/lEV-enriched fractions enhanced endothelial cell migration while suppressing angiogenic network formation, resulting in disorganised, shortened capillary-like structures. These pro-migratory and anti-angiogenic effects of m/lEVs were accompanied by a selective suppression of mitochondrial respiration in hCMEC/D3 cells, with no such effect observed in HUVECs, indicating that the functional alterations are linked to altered bioenergetic activity specifically in BBB endothelial cells. Our data indicate that sEV and m/lEV-enriched subpopulations derived from GBM exert distinct vascular effects, underscoring their potential as functionally distinct EV-based biomarkers and informing the development of personalised therapeutic strategies in GBM. (created in BioRender. Kulakauskienė, D. (2026) https://BioRender.com/e8jyszx )

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Small and medium/large glioblastoma extracellular vesicles differentially regulate endothelial and mitochondrial function in blood–brain barrier and peripheral vasculature models

Key Points

Abstract

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