miR-9-5p is involved in the rescue of stress-dependent dendritic shortening of hippocampal pyramidal neurons induced by acute antidepressant treatment with ketamine

Converging clinical and preclinical evidence demonstrates that depressive phenotypes are associated with synaptic dysfunction and dendritic simplification in cortico-limbic glutamatergic areas. On the other hand, the rapid antidepressant effect of acute ketamine is consistently reported to occur tog...

Descripción completa

Detalles Bibliográficos
Autores principales: Mingardi, Jessica, La Via, Luca, Tornese, Paolo, Carini, Giulia, Trontti, Kalevi, Seguini, Mara, Tardito, Daniela, Bono, Federica, Fiorentini, Chiara, Elia, Leonardo, Hovatta, Iiris, Popoli, Maurizio, Musazzi, Laura, Barbon, Alessandro
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Original Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8379501/
https://www.ncbi.nlm.nih.gov/pubmed/34458512
http://dx.doi.org/10.1016/j.ynstr.2021.100381
_version_ 1783741022125162496
author Mingardi, Jessica
La Via, Luca
Tornese, Paolo
Carini, Giulia
Trontti, Kalevi
Seguini, Mara
Tardito, Daniela
Bono, Federica
Fiorentini, Chiara
Elia, Leonardo
Hovatta, Iiris
Popoli, Maurizio
Musazzi, Laura
Barbon, Alessandro
author_facet Mingardi, Jessica
La Via, Luca
Tornese, Paolo
Carini, Giulia
Trontti, Kalevi
Seguini, Mara
Tardito, Daniela
Bono, Federica
Fiorentini, Chiara
Elia, Leonardo
Hovatta, Iiris
Popoli, Maurizio
Musazzi, Laura
Barbon, Alessandro
author_sort Mingardi, Jessica
collection PubMed
description Converging clinical and preclinical evidence demonstrates that depressive phenotypes are associated with synaptic dysfunction and dendritic simplification in cortico-limbic glutamatergic areas. On the other hand, the rapid antidepressant effect of acute ketamine is consistently reported to occur together with the rescue of dendritic atrophy and reduction of spine number induced by chronic stress in the hippocampus and prefrontal cortex of animal models of depression. Nevertheless, the molecular mechanisms underlying these morphological alterations remain largely unknown. Here, we found that miR-9-5p levels were selectively reduced in the hippocampus of rats vulnerable to Chronic Mild Stress (CMS), while acute subanesthetic ketamine restored its levels to basal condition in just 24h; miR-9-5p expression inversely correlated with the anhedonic phenotype. A decrease of miR-9-5p was reproduced in an in vitro model of stress, based on primary hippocampal neurons incubated with the stress hormone corticosterone. In both CMS animals and primary neurons, decreased miR-9-5p levels were associated with dendritic simplification, while treatment with ketamine completely rescued the changes. In vitro modulation of miR-9-5p expression showed a direct role of miR-9-5p in regulating dendritic length and spine density in mature primary hippocampal neurons. Among the putative target genes tested, Rest and Sirt1 were validated as biological targets in primary neuronal cultures. Moreover, in line with miR-9-5p changes, REST protein expression levels were remarkably increased in both CMS vulnerable animals and corticosterone-treated neurons, while ketamine completely abolished this alteration. Finally, the shortening of dendritic length in corticosterone-treated neurons was shown to be partly rescued by miR-9-5p overexpression and dependent on REST protein expression. Overall, our data unveiled the functional role of miR-9-5p in the remodeling of dendritic arbor induced by stress/corticosterone in vulnerable animals and its rescue by acute antidepressant treatment with ketamine.
format Online
Article
Text
id pubmed-8379501
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-83795012021-08-27 miR-9-5p is involved in the rescue of stress-dependent dendritic shortening of hippocampal pyramidal neurons induced by acute antidepressant treatment with ketamine Mingardi, Jessica La Via, Luca Tornese, Paolo Carini, Giulia Trontti, Kalevi Seguini, Mara Tardito, Daniela Bono, Federica Fiorentini, Chiara Elia, Leonardo Hovatta, Iiris Popoli, Maurizio Musazzi, Laura Barbon, Alessandro Neurobiol Stress Original Research Article Converging clinical and preclinical evidence demonstrates that depressive phenotypes are associated with synaptic dysfunction and dendritic simplification in cortico-limbic glutamatergic areas. On the other hand, the rapid antidepressant effect of acute ketamine is consistently reported to occur together with the rescue of dendritic atrophy and reduction of spine number induced by chronic stress in the hippocampus and prefrontal cortex of animal models of depression. Nevertheless, the molecular mechanisms underlying these morphological alterations remain largely unknown. Here, we found that miR-9-5p levels were selectively reduced in the hippocampus of rats vulnerable to Chronic Mild Stress (CMS), while acute subanesthetic ketamine restored its levels to basal condition in just 24h; miR-9-5p expression inversely correlated with the anhedonic phenotype. A decrease of miR-9-5p was reproduced in an in vitro model of stress, based on primary hippocampal neurons incubated with the stress hormone corticosterone. In both CMS animals and primary neurons, decreased miR-9-5p levels were associated with dendritic simplification, while treatment with ketamine completely rescued the changes. In vitro modulation of miR-9-5p expression showed a direct role of miR-9-5p in regulating dendritic length and spine density in mature primary hippocampal neurons. Among the putative target genes tested, Rest and Sirt1 were validated as biological targets in primary neuronal cultures. Moreover, in line with miR-9-5p changes, REST protein expression levels were remarkably increased in both CMS vulnerable animals and corticosterone-treated neurons, while ketamine completely abolished this alteration. Finally, the shortening of dendritic length in corticosterone-treated neurons was shown to be partly rescued by miR-9-5p overexpression and dependent on REST protein expression. Overall, our data unveiled the functional role of miR-9-5p in the remodeling of dendritic arbor induced by stress/corticosterone in vulnerable animals and its rescue by acute antidepressant treatment with ketamine. Elsevier 2021-08-12 /pmc/articles/PMC8379501/ /pubmed/34458512 http://dx.doi.org/10.1016/j.ynstr.2021.100381 Text en © 2021 Published by Elsevier Inc. https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Research Article
Mingardi, Jessica
La Via, Luca
Tornese, Paolo
Carini, Giulia
Trontti, Kalevi
Seguini, Mara
Tardito, Daniela
Bono, Federica
Fiorentini, Chiara
Elia, Leonardo
Hovatta, Iiris
Popoli, Maurizio
Musazzi, Laura
Barbon, Alessandro
miR-9-5p is involved in the rescue of stress-dependent dendritic shortening of hippocampal pyramidal neurons induced by acute antidepressant treatment with ketamine
title miR-9-5p is involved in the rescue of stress-dependent dendritic shortening of hippocampal pyramidal neurons induced by acute antidepressant treatment with ketamine
title_full miR-9-5p is involved in the rescue of stress-dependent dendritic shortening of hippocampal pyramidal neurons induced by acute antidepressant treatment with ketamine
title_fullStr miR-9-5p is involved in the rescue of stress-dependent dendritic shortening of hippocampal pyramidal neurons induced by acute antidepressant treatment with ketamine
title_full_unstemmed miR-9-5p is involved in the rescue of stress-dependent dendritic shortening of hippocampal pyramidal neurons induced by acute antidepressant treatment with ketamine
title_short miR-9-5p is involved in the rescue of stress-dependent dendritic shortening of hippocampal pyramidal neurons induced by acute antidepressant treatment with ketamine
title_sort mir-9-5p is involved in the rescue of stress-dependent dendritic shortening of hippocampal pyramidal neurons induced by acute antidepressant treatment with ketamine
topic Original Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8379501/
https://www.ncbi.nlm.nih.gov/pubmed/34458512
http://dx.doi.org/10.1016/j.ynstr.2021.100381
work_keys_str_mv AT mingardijessica mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine
AT lavialuca mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine
AT tornesepaolo mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine
AT carinigiulia mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine
AT tronttikalevi mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine
AT seguinimara mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine
AT tarditodaniela mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine
AT bonofederica mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine
AT fiorentinichiara mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine
AT elialeonardo mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine
AT hovattaiiris mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine
AT popolimaurizio mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine
AT musazzilaura mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine
AT barbonalessandro mir95pisinvolvedintherescueofstressdependentdendriticshorteningofhippocampalpyramidalneuronsinducedbyacuteantidepressanttreatmentwithketamine

Ejemplares similares