Negative Auto-Regulation of Myostatin Expression is Mediated by Smad3 and MicroRNA-27

Growth factors, such as myostatin (Mstn), play an important role in regulating post-natal myogenesis. In fact, loss of Mstn has been shown to result in increased post-natal muscle growth through enhanced satellite cell functionality; while elevated levels of Mstn result in dramatic skeletal muscle w...

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Autores principales: McFarlane, Craig, Vajjala, Anuradha, Arigela, Harikumar, Lokireddy, Sudarsanareddy, Ge, XiaoJia, Bonala, Sabeera, Manickam, Ravikumar, Kambadur, Ravi, Sharma, Mridula
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3909192/
https://www.ncbi.nlm.nih.gov/pubmed/24498167
http://dx.doi.org/10.1371/journal.pone.0087687
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author McFarlane, Craig
Vajjala, Anuradha
Arigela, Harikumar
Lokireddy, Sudarsanareddy
Ge, XiaoJia
Bonala, Sabeera
Manickam, Ravikumar
Kambadur, Ravi
Sharma, Mridula
author_facet McFarlane, Craig
Vajjala, Anuradha
Arigela, Harikumar
Lokireddy, Sudarsanareddy
Ge, XiaoJia
Bonala, Sabeera
Manickam, Ravikumar
Kambadur, Ravi
Sharma, Mridula
author_sort McFarlane, Craig
collection PubMed
description Growth factors, such as myostatin (Mstn), play an important role in regulating post-natal myogenesis. In fact, loss of Mstn has been shown to result in increased post-natal muscle growth through enhanced satellite cell functionality; while elevated levels of Mstn result in dramatic skeletal muscle wasting through a mechanism involving reduced protein synthesis and increased ubiquitin-mediated protein degradation. Here we show that miR-27a/b plays an important role in feed back auto-regulation of Mstn and thus regulation of post-natal myogenesis. Sequence analysis of Mstn 3′ UTR showed a single highly conserved miR-27a/b binding site and increased expression of miR-27a/b was correlated with decreased expression of Mstn and vice versa both in vitro and in mice in vivo. Moreover, we also show that Mstn gene expression was regulated by miR-27a/b. Treatment with miR-27a/b-specific AntagomiRs resulted in increased Mstn expression, reduced myoblast proliferation, impaired satellite cell activation and induction of skeletal muscle atrophy that was rescued upon either blockade of, or complete absence of, Mstn. Consistent with this, miR-27a over expression resulted in reduced Mstn expression, skeletal muscle hypertrophy and an increase in the number of activated satellite cells, all features consistent with impaired Mstn function. Loss of Smad3 was associated with increased levels of Mstn, concomitant with decreased miR-27a/b expression, which is consistent with impaired satellite cell function and muscular atrophy previously reported in Smad3-null mice. Interestingly, treatment with Mstn resulted in increased miR-27a/b expression, which was shown to be dependent on the activity of Smad3. These data highlight a novel auto-regulatory mechanism in which Mstn, via Smad3 signaling, regulates miR-27a/b and in turn its own expression. In support, Mstn-mediated inhibition of Mstn 3′ UTR reporter activity was reversed upon miR-27a/b-specific AntagomiR transfection. Therefore, miR-27a/b, through negatively regulating Mstn, plays a role in promoting satellite cell activation, myoblast proliferation and preventing muscle wasting.
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spelling pubmed-39091922014-02-04 Negative Auto-Regulation of Myostatin Expression is Mediated by Smad3 and MicroRNA-27 McFarlane, Craig Vajjala, Anuradha Arigela, Harikumar Lokireddy, Sudarsanareddy Ge, XiaoJia Bonala, Sabeera Manickam, Ravikumar Kambadur, Ravi Sharma, Mridula PLoS One Research Article Growth factors, such as myostatin (Mstn), play an important role in regulating post-natal myogenesis. In fact, loss of Mstn has been shown to result in increased post-natal muscle growth through enhanced satellite cell functionality; while elevated levels of Mstn result in dramatic skeletal muscle wasting through a mechanism involving reduced protein synthesis and increased ubiquitin-mediated protein degradation. Here we show that miR-27a/b plays an important role in feed back auto-regulation of Mstn and thus regulation of post-natal myogenesis. Sequence analysis of Mstn 3′ UTR showed a single highly conserved miR-27a/b binding site and increased expression of miR-27a/b was correlated with decreased expression of Mstn and vice versa both in vitro and in mice in vivo. Moreover, we also show that Mstn gene expression was regulated by miR-27a/b. Treatment with miR-27a/b-specific AntagomiRs resulted in increased Mstn expression, reduced myoblast proliferation, impaired satellite cell activation and induction of skeletal muscle atrophy that was rescued upon either blockade of, or complete absence of, Mstn. Consistent with this, miR-27a over expression resulted in reduced Mstn expression, skeletal muscle hypertrophy and an increase in the number of activated satellite cells, all features consistent with impaired Mstn function. Loss of Smad3 was associated with increased levels of Mstn, concomitant with decreased miR-27a/b expression, which is consistent with impaired satellite cell function and muscular atrophy previously reported in Smad3-null mice. Interestingly, treatment with Mstn resulted in increased miR-27a/b expression, which was shown to be dependent on the activity of Smad3. These data highlight a novel auto-regulatory mechanism in which Mstn, via Smad3 signaling, regulates miR-27a/b and in turn its own expression. In support, Mstn-mediated inhibition of Mstn 3′ UTR reporter activity was reversed upon miR-27a/b-specific AntagomiR transfection. Therefore, miR-27a/b, through negatively regulating Mstn, plays a role in promoting satellite cell activation, myoblast proliferation and preventing muscle wasting. Public Library of Science 2014-01-31 /pmc/articles/PMC3909192/ /pubmed/24498167 http://dx.doi.org/10.1371/journal.pone.0087687 Text en © 2014 McFarlane et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
McFarlane, Craig
Vajjala, Anuradha
Arigela, Harikumar
Lokireddy, Sudarsanareddy
Ge, XiaoJia
Bonala, Sabeera
Manickam, Ravikumar
Kambadur, Ravi
Sharma, Mridula
Negative Auto-Regulation of Myostatin Expression is Mediated by Smad3 and MicroRNA-27
title Negative Auto-Regulation of Myostatin Expression is Mediated by Smad3 and MicroRNA-27
title_full Negative Auto-Regulation of Myostatin Expression is Mediated by Smad3 and MicroRNA-27
title_fullStr Negative Auto-Regulation of Myostatin Expression is Mediated by Smad3 and MicroRNA-27
title_full_unstemmed Negative Auto-Regulation of Myostatin Expression is Mediated by Smad3 and MicroRNA-27
title_short Negative Auto-Regulation of Myostatin Expression is Mediated by Smad3 and MicroRNA-27
title_sort negative auto-regulation of myostatin expression is mediated by smad3 and microrna-27
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3909192/
https://www.ncbi.nlm.nih.gov/pubmed/24498167
http://dx.doi.org/10.1371/journal.pone.0087687
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