Microembolus clearance through angiophagy is an auxiliary mechanism preserving tissue perfusion in the rat brain
Male
0301 basic medicine
Endothelial cells
Research
Brain
Endothelial Cells
Thrombosis
Cerebral microcirculation
Microspheres
Rats
Angiophagy
03 medical and health sciences
Intracranial Embolism
Phagocytosis
Embolus
Cerebrovascular Circulation
Microvessels
Human Umbilical Vein Endothelial Cells
Animals
Humans
Female
Neurology. Diseases of the nervous system
Endothelium, Vascular
RC346-429
DOI:
10.1186/s40478-020-01071-9
Publication Date:
2020-11-17T18:02:58Z
AUTHORS (11)
ABSTRACT
AbstractConsidering its intolerance to ischemia, it is of critical importance for the brain to efficiently process microvascular occlusions and maintain tissue perfusion. In addition to collateral microvascular flow and enzymatic degradation of emboli, the endothelium has the potential to engulf microparticles and thereby recanalize the vessel, through a process called angiophagy. Here, we set out to study the dynamics of angiophagy in relation to cytoskeletal remodeling in vitro and reperfusion in vivo. We show that polystyrene microspheres and fibrin clots are actively taken up by (brain) endothelial cells in vitro, and chart the dynamics of the actin cytoskeleton during this process using live cell imaging. Whereas microspheres were taken up through the formation of a cup structure by the apical endothelial membrane, fibrin clots were completely engulfed by the cells, marked by dense F-actin accumulation surrounding the clot. Both microspheres and fibrin clots were retained in the endothelial cells. Notably, fibrin clots were not degraded intracellularly. Using an in vivo microembolization rat model, in which microparticles are injected into the common carotid artery, we found that microspheres are transported by the endothelium from the microvasculature into the brain parenchyma. Microembolization with microspheres caused temporal opening of the blood–brain barrier and vascular nonperfusion, followed by microsphere extravasation and restoration of vessel perfusion over time. Taken together, angiophagy is accompanied by active cytoskeletal remodeling of the endothelium, and is an effective mechanism to restore perfusion of the occluded microvasculature in vivo.
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