MODELING BIPOLAR DISORDER IN MICE THROUGH NEURAL PRECURSOR CELLS DERIVED FROM PATIENT OLFACTORY NEUROEPITHELIUM
Neuropsychopharmacology and Psychobiology Research Group, Department of Neuroscience, University of Cadiz
Presentation
Date TBA
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Poster Board
PS07-10AM-599
Poster
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ONE neural progenitor cells from control donors and BD type-I patients, which respond or do not respond to lithium treatment based on the ALDA scale, were grafted into a neurogenic niche in rodents. Mania-like and depressive-like behaviors were assessed 4 weeks after implantation as correlates of BD-like phenotype. Lithium was administered via chow for 3 weeks before behavioral testing. At the endpoint, brains were collected for immunofluorescence and electron microscopy analyses.
Animals grafted with ONE cells from patients develop a BD-like phenotype (depressive-like behavior and motor hyperactivity) 4 weeks after implantation. Strikingly, this phenotype is specifically reversed after chronic lithium treatment in animals grafted with ONE cells from lithium responders. Additionally, immunohistological studies showed that 75-80% of these human ONE cells expressed mature GABAergic neuron markers and were integrated into the mouse neuronal circuit receiving synaptic contacts.
These results indicate that the model would be suitable for studying BD neurobiology, identifying predictive biomarkers of therapeutic response, and evaluating treatment efficacy, while opening avenues for personalized medicine.
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