D-011 | miR-191-5p regulates Neuronal Complexity and dendritic spine maturation during Mammalian Brain development

D-011 | miR-191-5p regulates Neuronal Complexity and dendritic spine maturation during Mammalian Brain development 150 150 SAN 2024 Annual Meeting

Cellular and Molecular Neurobiology
Author: Paula Macarena Gonzalez | Email: paugonzalez.0991@gmail.com


Paula M. Gonzalez1°2°, Rodolfo Sanchez-Iazurlo1°2°, David Alarcón Pastor1°2°,  Paula A. Aguirre1°2°, Sebastian A. Giusti3°4°, Damian Refojo3°4°, Fernando Bustos,  Juan Pablo Fededa1°2°

Instituto de Investigaciones Biotecnológicas, Universidad Nacional de San Martín (UNSAM) – Consejo Nacional de Investigaciones Científicas y Técnicas (CONICET).
Escuela de Bio y Nanotecnologías (EByN), Universidad Nacional de San Martín.
Instituto de Investigación en Biomedicina de Buenos Aires (IBioBA)–CONICET–Partner Institute of the Max Planck Society, Buenos Aires, Argentina.
Molecular Neurobiology, Max Planck Institute of Psychiatry, Munich, Germany.

microRNA-191 (miR-191-5p), a small regulatory non-coding RNA, has been implicated as a marker of different neurodegenerative diseases, and is one of the major microRNA species expressed in the cerebral cortex from neurogenesis and throughout synaptogenesis.
To investigate the role of miR-191-5p during post-natal cortical development using loss of function experiments, we KO miR-191-5p in newborn mice using an adeno-associated virus (AAV) based CRISPR/Cas9 gene editing strategy to disrupt the structure of miR-191-5p precursor (pri-miR-191-5p) and suppress the generation of the mature microRNA.
Using Golgi-Cox staining combined with confocal microscopy to evaluate the morphology of cortical and hippocampal pyramidal neurons, we observed a reduction in the average length of neuronal processes and the total surface area of the dendritic tree in miR-191-5p KO mice vs. control. Similarly, in vitro miR-191-5p-depleted primary cultured neurons also exhibited shortened neuronal processes compared to control cultures.
We also analyzed the density and type of dendritic spines generated in miR-191-5p KO vs. control cultured neurons in vitro and found that miR-191-5p is necessary for the generation of mature spines.
Altogether, our data shows that miR-191-5p acts as a positive regulator of neuronal branching and connectivity during early post-natal brain development.

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