Astrocyte-derived small extracellular vesicles regulate dendritic complexity through miR-26a-5p activity
Author
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Luarte Navarro, Alejandro
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Henzi, Roberto
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Fernández, Anllely
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Gaete, Diego
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Cisternas, Pablo
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Pizarro, Matías
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Batiz, Luis Federico
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Villalobos, Isabel
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Masalleras, Matías
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Vergara, Rodrigo
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Varas Godoy, Manuel
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Abarzúa Catalán, Lorena
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Herrera Molina, Rodrigo
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Lafourcade, Carlos
Author
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Wyneken, Úrsula
Admission date
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2020-07-27T23:58:26Z
Available date
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2020-07-27T23:58:26Z
Publication date
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2020
Cita de ítem
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Cells 9 (2020): 930
es_ES
Identifier
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10.3390/cells9040930
Identifier
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https://repositorio.uchile.cl/handle/2250/176157
Abstract
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In the last few decades, it has been established that astrocytes play key roles in the regulation of neuronal morphology. However, the contribution of astrocyte-derived small extracellular vesicles (sEVs) to morphological differentiation of neurons has only recently been addressed. Here, we showed that cultured astrocytes expressing a GFP-tagged version of the stress-regulated astrocytic enzyme Aldolase C (Aldo C-GFP) release small extracellular vesicles (sEVs) that are transferred into cultured hippocampal neurons. Surprisingly, Aldo C-GFP-containing sEVs (Aldo C-GFP sEVs) displayed an exacerbated capacity to reduce the dendritic complexity in developing hippocampal neurons compared to sEVs derived from control (i.e., GFP-expressing) astrocytes. Using bioinformatics and biochemical tools, we found that the total content of overexpressed Aldo C-GFP correlates with an increased content of endogenous miRNA-26a-5p in both total astrocyte homogenates and sEVs. Notably, neurons magnetofected with a nucleotide sequence that mimics endogenous miRNA-26a-5p (mimic 26a-5p) not only decreased the levels of neuronal proteins associated to morphogenesis regulation, but also reproduced morphological changes induced by Aldo-C-GFP sEVs. Furthermore, neurons magnetofected with a sequence targeting miRNA-26a-5p (antago 26a-5p) were largely resistant to Aldo C-GFP sEVs. Our results support a novel and complex level of astrocyte-to-neuron communication mediated by astrocyte-derived sEVs and the activity of their miRNA content.
es_ES
Patrocinador
dc.description.sponsorship
Comision Nacional de Investigacion Cientifica y Tecnologica (CONICYT)
CONICYT FONDECYT
3170887
1140108
1200693
EMBO short-stay Fellowship
CBBS-Magdeburg