The MicroRNA miR-696 is regulated by SNARK and reduces mitochondrial activity in mouse skeletal muscle through Pgc1α inhibition

OBJECTIVE: MicroRNAs (miRNA) are known to regulate the expression of genes involved in several physiological processes including metabolism, mitochondrial biogenesis, proliferation, differentiation, and cell death. METHODS: Using “in silico” analyses, we identified 219 unique miRNAs that potentially...

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Autores principales: Queiroz, André L., Lessard, Sarah J., Ouchida, Amanda T., Araujo, Hygor N., Gonçalves, Dawit A., Simões Fróes Guimarães, Dimitrius Santiago P., Teodoro, Bruno G., So, Kawai, Espreafico, Enilza M., Hirshman, Michael F., Alberici, Luciane C., Kettelhut, Isis do Carmo, Goodyear, Laurie J., Silveira, Leonardo R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8121711/
https://www.ncbi.nlm.nih.gov/pubmed/33812060
http://dx.doi.org/10.1016/j.molmet.2021.101226
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author Queiroz, André L.
Lessard, Sarah J.
Ouchida, Amanda T.
Araujo, Hygor N.
Gonçalves, Dawit A.
Simões Fróes Guimarães, Dimitrius Santiago P.
Teodoro, Bruno G.
So, Kawai
Espreafico, Enilza M.
Hirshman, Michael F.
Alberici, Luciane C.
Kettelhut, Isis do Carmo
Goodyear, Laurie J.
Silveira, Leonardo R.
author_facet Queiroz, André L.
Lessard, Sarah J.
Ouchida, Amanda T.
Araujo, Hygor N.
Gonçalves, Dawit A.
Simões Fróes Guimarães, Dimitrius Santiago P.
Teodoro, Bruno G.
So, Kawai
Espreafico, Enilza M.
Hirshman, Michael F.
Alberici, Luciane C.
Kettelhut, Isis do Carmo
Goodyear, Laurie J.
Silveira, Leonardo R.
author_sort Queiroz, André L.
collection PubMed
description OBJECTIVE: MicroRNAs (miRNA) are known to regulate the expression of genes involved in several physiological processes including metabolism, mitochondrial biogenesis, proliferation, differentiation, and cell death. METHODS: Using “in silico” analyses, we identified 219 unique miRNAs that potentially bind to the 3′UTR region of a critical mitochondrial regulator, the peroxisome proliferator-activated receptor gamma coactivator (PGC) 1 alpha (Pgc1α). Of the 219 candidate miRNAs, miR-696 had one of the highest interactions at the 3′UTR of Pgc1α, suggesting that miR-696 may be involved in the regulation of Pgc1α. RESULTS: Consistent with this hypothesis, we found that miR-696 was highly expressed in the skeletal muscle of STZ-induced diabetic mice and chronic high-fat-fed mice. C2C12 muscle cells exposed to palmitic acid also exhibited a higher expression of miR-696. This increased expression corresponded with a reduced expression of oxidative metabolism genes and reduced mitochondrial respiration. Importantly, reducing miR-696 reversed decreases in mitochondrial activity in response to palmitic acid. Using C2C12 cells treated with the AMP-activated protein kinase (AMPK) activator AICAR and skeletal muscle from AMPKα2 dominant-negative (DN) mice, we found that the signaling mechanism regulating miR-696 did not involve AMPK. In contrast, overexpression of SNF1-AMPK-related kinase (SNARK) in C2C12 cells increased miR-696 transcription while knockdown of SNARK significantly decreased miR-696. Moreover, muscle-specific transgenic mice overexpressing SNARK exhibited a lower expression of Pgc1α, elevated levels of miR-696, and reduced amounts of spontaneous activity. CONCLUSIONS: Our findings demonstrate that metabolic stress increases miR-696 expression in skeletal muscle cells, which in turn inhibits Pgc1α, reducing mitochondrial function. SNARK plays a role in this process as a metabolic stress signaling molecule inducing the expression of miR-696.
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spelling pubmed-81217112021-05-20 The MicroRNA miR-696 is regulated by SNARK and reduces mitochondrial activity in mouse skeletal muscle through Pgc1α inhibition Queiroz, André L. Lessard, Sarah J. Ouchida, Amanda T. Araujo, Hygor N. Gonçalves, Dawit A. Simões Fróes Guimarães, Dimitrius Santiago P. Teodoro, Bruno G. So, Kawai Espreafico, Enilza M. Hirshman, Michael F. Alberici, Luciane C. Kettelhut, Isis do Carmo Goodyear, Laurie J. Silveira, Leonardo R. Mol Metab Original Article OBJECTIVE: MicroRNAs (miRNA) are known to regulate the expression of genes involved in several physiological processes including metabolism, mitochondrial biogenesis, proliferation, differentiation, and cell death. METHODS: Using “in silico” analyses, we identified 219 unique miRNAs that potentially bind to the 3′UTR region of a critical mitochondrial regulator, the peroxisome proliferator-activated receptor gamma coactivator (PGC) 1 alpha (Pgc1α). Of the 219 candidate miRNAs, miR-696 had one of the highest interactions at the 3′UTR of Pgc1α, suggesting that miR-696 may be involved in the regulation of Pgc1α. RESULTS: Consistent with this hypothesis, we found that miR-696 was highly expressed in the skeletal muscle of STZ-induced diabetic mice and chronic high-fat-fed mice. C2C12 muscle cells exposed to palmitic acid also exhibited a higher expression of miR-696. This increased expression corresponded with a reduced expression of oxidative metabolism genes and reduced mitochondrial respiration. Importantly, reducing miR-696 reversed decreases in mitochondrial activity in response to palmitic acid. Using C2C12 cells treated with the AMP-activated protein kinase (AMPK) activator AICAR and skeletal muscle from AMPKα2 dominant-negative (DN) mice, we found that the signaling mechanism regulating miR-696 did not involve AMPK. In contrast, overexpression of SNF1-AMPK-related kinase (SNARK) in C2C12 cells increased miR-696 transcription while knockdown of SNARK significantly decreased miR-696. Moreover, muscle-specific transgenic mice overexpressing SNARK exhibited a lower expression of Pgc1α, elevated levels of miR-696, and reduced amounts of spontaneous activity. CONCLUSIONS: Our findings demonstrate that metabolic stress increases miR-696 expression in skeletal muscle cells, which in turn inhibits Pgc1α, reducing mitochondrial function. SNARK plays a role in this process as a metabolic stress signaling molecule inducing the expression of miR-696. Elsevier 2021-03-31 /pmc/articles/PMC8121711/ /pubmed/33812060 http://dx.doi.org/10.1016/j.molmet.2021.101226 Text en © 2021 The Authors 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 Article
Queiroz, André L.
Lessard, Sarah J.
Ouchida, Amanda T.
Araujo, Hygor N.
Gonçalves, Dawit A.
Simões Fróes Guimarães, Dimitrius Santiago P.
Teodoro, Bruno G.
So, Kawai
Espreafico, Enilza M.
Hirshman, Michael F.
Alberici, Luciane C.
Kettelhut, Isis do Carmo
Goodyear, Laurie J.
Silveira, Leonardo R.
The MicroRNA miR-696 is regulated by SNARK and reduces mitochondrial activity in mouse skeletal muscle through Pgc1α inhibition
title The MicroRNA miR-696 is regulated by SNARK and reduces mitochondrial activity in mouse skeletal muscle through Pgc1α inhibition
title_full The MicroRNA miR-696 is regulated by SNARK and reduces mitochondrial activity in mouse skeletal muscle through Pgc1α inhibition
title_fullStr The MicroRNA miR-696 is regulated by SNARK and reduces mitochondrial activity in mouse skeletal muscle through Pgc1α inhibition
title_full_unstemmed The MicroRNA miR-696 is regulated by SNARK and reduces mitochondrial activity in mouse skeletal muscle through Pgc1α inhibition
title_short The MicroRNA miR-696 is regulated by SNARK and reduces mitochondrial activity in mouse skeletal muscle through Pgc1α inhibition
title_sort microrna mir-696 is regulated by snark and reduces mitochondrial activity in mouse skeletal muscle through pgc1α inhibition
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8121711/
https://www.ncbi.nlm.nih.gov/pubmed/33812060
http://dx.doi.org/10.1016/j.molmet.2021.101226
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