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BDNF RECEPTOR DYSREGULATION IN ALZHEIMER'S-DISEASE: EXTRACELLULAR VESICLE-MEDIATED TRANSPORT OF A SYNAPTOTOXIC TRKB FRAGMENT
Tiago Costa-Coelhoand 13 co-authors
Faculdade de Medicina da Universidade de Lisboa
FENS Forum 2026 (2026)
Barcelona, Spain
Board PS03-08AM-105
Presentation
Date TBA
Board: PS03-08AM-105
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Poster Board
PS03-08AM-105
Poster
View posterAbstract
The neuroprotective BDNF/TrkB-FL system is compromised in Alzheimer’s disease (AD). Amyloid-beta triggers calpain-mediated TrkB-FL receptor cleavage, leading to TrkB-ICD formation, a novel intracellular fragment. Biological fluids are used to pinpoint potential disease biomarkers and extracellular vesicles (EVs) are cell-specific carriers of promising pathological biomarkers. Thus, this work aimed to 1) investigate TrkB-ICD effects and 2) its presence in AD human samples and EVs. To that endeavour, neurons were transduced with either LV-CamKII-GFP or LV-CamKII-TrkB-ICD-IRES-ZsGreen and used for patch clamp, dendritic spine and transcriptomic analysis. For CSF and plasma samples, patients fulfilled the criteria for Mild Cognitive Impairment due to AD (MCIAD), whereas controls (MCICONTROL) reported cognitive complaints but had no evidence of Aβ pathology or neuronal injury. MCIAD plasma-derived EVs (pdEVs) were isolated using the ExoQuick reagent and characterized. Neurons overexpressing TrkB-ICD were enriched in phosphotyrosine proteins (p=7.62x10-3,n=3) and possessed fewer dendritic spines (p=1.15x10-10, n=13-15 cells/3 cultures). TrkB-ICD neurons are also more hyperexcitable given by mEPSC increase (p=2.46x10-2, n=7-8 cells/3cultures) and concomitant decrease in resting membrane potential (p=1.26x10-2, n=7-8 cells/3 cultures). Transcriptomic data revealed that TrkB-ICD upregulates 23 GO terms, encompassing genes implicated in for synaptic structure/function. CSF analysis showed not only an increase in TrkB-ICD immunoreactivity in MCI due to AD patients (p=7.55x10-3,n=23-46), but also a negative correlation between the levels of Aβ1-42 and TrkB-ICD (ρ=-0.47, n=46). PDEVs of MCIAD patients contained higher levels of TrkB-ICD (p=0.010, n=17-18). Collectively, these findings indicate that TrkB-ICD is secreted extracellularly, suggesting a possible mechanism for the dissemination of its toxic effects.
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