IRES-mediated translation of utrophin A is enhanced by glucocorticoid treatment in skeletal muscle cells.

IRES-mediated translation of utrophin A is enhanced by glucocorticoid treatment in skeletal muscle cells.

Glucocorticoids are currently the only drug treatment recognized to benefit Duchenne muscular dystrophy (DMD) patients. The nature of the mechanisms underlying the beneficial effects remains incompletely understood but may involve an increase in the expression of utrophin. Here, we show that treatme...

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Main Authors: Pedro Miura, Meghan Andrews, Martin Holcik, Bernard J Jasmin
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2008-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2396518?pdf=render
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spelling doaj-7d73d38e6ae24d2781f5030f13f60ad92020-11-24T21:51:14ZengPublic Library of Science (PLoS)PLoS ONE1932-62032008-01-0136e230910.1371/journal.pone.0002309IRES-mediated translation of utrophin A is enhanced by glucocorticoid treatment in skeletal muscle cells.Pedro MiuraMeghan AndrewsMartin HolcikBernard J JasminGlucocorticoids are currently the only drug treatment recognized to benefit Duchenne muscular dystrophy (DMD) patients. The nature of the mechanisms underlying the beneficial effects remains incompletely understood but may involve an increase in the expression of utrophin. Here, we show that treatment of myotubes with 6alpha-methylprednisolone-21 sodium succinate (PDN) results in enhanced expression of utrophin A without concomitant increases in mRNA levels thereby suggesting that translational regulation contributes to the increase. In agreement with this, we show that PDN treatment of cells transfected with monocistronic reporter constructs harbouring the utrophin A 5'UTR, causes an increase in reporter protein expression while leaving levels of reporter mRNAs unchanged. Using bicistronic reporter assays, we further demonstrate that PDN enhances activity of an Internal Ribosome Entry Site (IRES) located within the utrophin A 5'UTR. Analysis of polysomes demonstrate that PDN causes an overall reduction in polysome-associated mRNAs indicating that global translation rates are depressed under these conditions. Importantly, PDN causes an increase in the polysome association of endogenous utrophin A mRNAs and reporter mRNAs harbouring the utrophin A 5'UTR. Additional experiments identified a distinct region within the utrophin A 5'UTR that contains the inducible IRES activity. Together, these studies demonstrate that a translational regulatory mechanism involving increased IRES activation mediates, at least partially, the enhanced expression of utrophin A in muscle cells treated with glucocorticoids. Targeting the utrophin A IRES may thus offer an important and novel therapeutic avenue for developing drugs appropriate for DMD patients.http://europepmc.org/articles/PMC2396518?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Pedro Miura
Meghan Andrews
Martin Holcik
Bernard J Jasmin
spellingShingle Pedro Miura
Meghan Andrews
Martin Holcik
Bernard J Jasmin
IRES-mediated translation of utrophin A is enhanced by glucocorticoid treatment in skeletal muscle cells.
PLoS ONE
author_facet Pedro Miura
Meghan Andrews
Martin Holcik
Bernard J Jasmin
author_sort Pedro Miura
title IRES-mediated translation of utrophin A is enhanced by glucocorticoid treatment in skeletal muscle cells.
title_short IRES-mediated translation of utrophin A is enhanced by glucocorticoid treatment in skeletal muscle cells.
title_full IRES-mediated translation of utrophin A is enhanced by glucocorticoid treatment in skeletal muscle cells.
title_fullStr IRES-mediated translation of utrophin A is enhanced by glucocorticoid treatment in skeletal muscle cells.
title_full_unstemmed IRES-mediated translation of utrophin A is enhanced by glucocorticoid treatment in skeletal muscle cells.
title_sort ires-mediated translation of utrophin a is enhanced by glucocorticoid treatment in skeletal muscle cells.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2008-01-01
description Glucocorticoids are currently the only drug treatment recognized to benefit Duchenne muscular dystrophy (DMD) patients. The nature of the mechanisms underlying the beneficial effects remains incompletely understood but may involve an increase in the expression of utrophin. Here, we show that treatment of myotubes with 6alpha-methylprednisolone-21 sodium succinate (PDN) results in enhanced expression of utrophin A without concomitant increases in mRNA levels thereby suggesting that translational regulation contributes to the increase. In agreement with this, we show that PDN treatment of cells transfected with monocistronic reporter constructs harbouring the utrophin A 5'UTR, causes an increase in reporter protein expression while leaving levels of reporter mRNAs unchanged. Using bicistronic reporter assays, we further demonstrate that PDN enhances activity of an Internal Ribosome Entry Site (IRES) located within the utrophin A 5'UTR. Analysis of polysomes demonstrate that PDN causes an overall reduction in polysome-associated mRNAs indicating that global translation rates are depressed under these conditions. Importantly, PDN causes an increase in the polysome association of endogenous utrophin A mRNAs and reporter mRNAs harbouring the utrophin A 5'UTR. Additional experiments identified a distinct region within the utrophin A 5'UTR that contains the inducible IRES activity. Together, these studies demonstrate that a translational regulatory mechanism involving increased IRES activation mediates, at least partially, the enhanced expression of utrophin A in muscle cells treated with glucocorticoids. Targeting the utrophin A IRES may thus offer an important and novel therapeutic avenue for developing drugs appropriate for DMD patients.
url http://europepmc.org/articles/PMC2396518?pdf=render
work_keys_str_mv AT pedromiura iresmediatedtranslationofutrophinaisenhancedbyglucocorticoidtreatmentinskeletalmusclecells
AT meghanandrews iresmediatedtranslationofutrophinaisenhancedbyglucocorticoidtreatmentinskeletalmusclecells
AT martinholcik iresmediatedtranslationofutrophinaisenhancedbyglucocorticoidtreatmentinskeletalmusclecells
AT bernardjjasmin iresmediatedtranslationofutrophinaisenhancedbyglucocorticoidtreatmentinskeletalmusclecells
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