Neuronal Prosurvival Role of Ceramide Synthase 2 by Olidogendrocyte-to-Neuron Extracellular Vesicle Transfer
Autor/a
Otros/as autores/as
Fecha de publicación
2023-03ISSN
1422-0067
Resumen
Ageing is associated with notorious alterations in neurons, i.e., in gene expression, mitochondrial function, membrane degradation or intercellular communication. However, neurons live for the entire lifespan of the individual. One of the reasons why neurons remain functional in elderly people is survival mechanisms prevail over death mechanisms. While many signals are either pro-survival or pro-death, others can play both roles. Extracellular vesicles (EVs) can signal both pro-toxicity and survival. We used young and old animals, primary neuronal and oligodendrocyte cultures and neuroblastoma and oligodendrocytic lines. We analysed our samples using a combination of proteomics and artificial neural networks, biochemistry and immunofluorescence approaches. We found an age-dependent increase in ceramide synthase 2 (CerS2) in cortical EVs, expressed by oligodendrocytes. In addition, we show that CerS2 is present in neurons via the uptake of oligodendrocyte-derived EVs. Finally, we show that age-associated inflammation and metabolic stress favour CerS2 expression and that oligodendrocyte-derived EVs loaded with CerS2 lead to the expression of the antiapoptotic factor Bcl2 in inflammatory conditions. Our study shows that intercellular communication is altered in the ageing brain, which favours neuronal survival through the transfer of oligodendrocyte-derived EVs containing CerS2.
Tipo de documento
Artículo
Versión del documento
Versión publicada
Lengua
Inglés
Materias (CDU)
576 - Biología celular y subcelular. Citología
577 - Bioquímica. Biología molecular. Biofísica
612 - Fisiología
Palabras clave
Brain ageing
EVs
Exosomes
CerS2
Intercellular communication
Oligodendrocyte-to-neuron
Cervell--Envelliment
Extracellular vesicles
Interacció cel·lular
Páginas
p.17
Publicado por
MDPI
Publicado en
International Journal of Molecular Sciences 2023, 24(6), 5986
Número del acuerdo de la subvención
info:eu-repo/grantAgreement/MCI/PN I+D/PID2019-104389RB-I00
info:eu-repo/grantAgreement/AEI i RyC/RYC2021-031713-I
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