TISSUE NICHE-DERIVED SIGNALS LOCALLY PROGRAM HUMAN MICROGLIA PHENOTYPES IN AN ORGANOID MODEL OF THE DEVELOPING HUMAN BRAIN
Center for Organoid Systems, Technical University of Munich, 85748 Garching, Germany
Presentation
Date TBA
Event Information
Poster Board
PS01-07AM-132
Poster
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Using this model, we identified spatially defined microglial phenotypes that arise during early stages of human cortical development. iPSC-derived hMG displayed remarkable plasticity, adapting their morphology, behavior, and transcriptional profiles according to their spatial localization within the assembloid. Notably, we uncovered discrete microglial microdomains, including axon tract–enriched regions, where microglia exhibited distinct characteristics compared to those residing in soma-dense areas. These axon-associated microglia closely resembled axon tract–associated microglia (ATMs) previously described in the developing mouse brain, particularly at cortical boundary zones. Correlative light and electron microscopy, together with functional assays, suggested that these ATM-like hMG dynamically respond to local structural and cellular cues, adjusting to region-specific functional demands.
Taken together, our findings demonstrate that human microglia, despite originating from a common progenitor population, can diversify in response to microenvironmental signals. This assembloid-based platform provides a powerful framework to dissect microglial heterogeneity in human neurodevelopment and offers new opportunities to explore microglia-driven mechanisms underlying neurodevelopmental disorders and context-specific therapeutic interventions.
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