Jan Zimak scite author profile

The delivery of therapeutics to the central nervous system (CNS) remains a major challenge in part due to the presence of the blood-brain barrier (BBB). Recently, cell-derived vesicles, particularly exosomes, have emerged as an attractive vehicle for targeting drugs to the brain, but whether or how they cross the BBB remains unclear. Here, we investigated the interactions between exosomes and brain microvascular endothelial cells (BMECs) in vitro under conditions that mimic the healthy and inflamed BBB in vivo. Transwell assays revealed that luciferase-carrying exosomes can cross a BMEC monolayer under stroke-like, inflamed conditions (TNF-α activated) but not under normal conditions. Confocal microscopy showed that exosomes are internalized by BMECs through endocytosis, co-localize with endosomes, in effect primarily utilizing the transcellular route of crossing. Together, these results indicate that cell-derived exosomes can cross the BBB model under stroke-like conditions in vitro. This study encourages further development of engineered exosomes as drug delivery vehicles or tracking tools for treating or monitoring neurological diseases.

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Theoretical investigation of the role of the RANK–RANKL–OPG system in bone remodeling

Pivonka

Zimak

Smith

et al. 2010

Journal of Theoretical Biology

102

109

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Rapid bacterial detection and antibiotic susceptibility testing in whole blood using one-step, high throughput blood digital PCR

Abram

Cherukury

et al. 2020

Lab Chip

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Jan Zimak

Model structure and control of bone remodeling: A theoretical study

Elucidation of Exosome Migration Across the Blood–Brain Barrier Model In Vitro

Theoretical investigation of the role of the RANK–RANKL–OPG system in bone remodeling

Rapid bacterial detection and antibiotic susceptibility testing in whole blood using one-step, high throughput blood digital PCR

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