DECIPHERING INFLAMMATORY MECHANISMS TO IMPROVE THE EFFICACY OF STEM CELL THERAPY
Institute of Neurosciences, University of Barcelona
Presentation
Date TBA
Event Information
Poster Board
PS04-08PM-090
Poster
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We induce focal cortical ischemic stroke in immunodeficient Rag1KO mice and transplant human long-term neuroepithelial stem (lt-NES) cell–derived neuronal progenitors into peri-infarct regions. Stroke triggers a robust sterile inflammatory response that critically influences graft outcomes. While microglial roles have been extensively studied, we specifically investigate border-associated macrophages, with a focus on perivascular macrophages (PVMs), which reside at the neurovascular interface and directly interact with both vascular and neuronal compartments.
Using selective PVM depletion via clodronate liposomes, we manipulate the inflammatory niche at the time of transplantation. This approach is combined with 3D tissue clearing, immunofluorescence, and functional MRI to quantify graft survival, neuronal maturation, synaptic connectivity, and local and brain-wide functional integration. In addition, monosynaptic rabies virus tracing enables circuit-level mapping of host–graft connectivity. By defining how PVM-driven inflammatory signaling regulates neuronal graft integration after stroke, this work identifies PVMs as modulators of regenerative success. These findings provide mechanistic insight into immune–neural interactions and highlight novel therapeutic targets to optimize stem cell–based strategies for post-stroke recovery.
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