Cmah-dystrophin deficient mdx mice display an accelerated cardiac phenotype that is improved following peptide-PMO exon skipping treatment

Duchenne muscular dystrophy (DMD) is caused by loss of dystrophin protein, leading to progressive muscle weakness and premature death due to respiratory and/or cardiac complications. Cardiac involvement is characterized by progressive dilated cardiomyopathy, decreased fractional shortening and metab...

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Autores principales: Betts, Corinne A, McClorey, Graham, Healicon, Richard, Hammond, Suzan M, Manzano, Raquel, Muses, Sofia, Ball, Vicky, Godfrey, Caroline, Merritt, Thomas M, van Westering, Tirsa, O’Donovan, Liz, Wells, Kim E, Gait, Michael J, Wells, Dominic J, Tyler, Damian, Wood, Matthew J
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2019
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General Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6337703/
https://www.ncbi.nlm.nih.gov/pubmed/30281092
http://dx.doi.org/10.1093/hmg/ddy346
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author Betts, Corinne A
McClorey, Graham
Healicon, Richard
Hammond, Suzan M
Manzano, Raquel
Muses, Sofia
Ball, Vicky
Godfrey, Caroline
Merritt, Thomas M
van Westering, Tirsa
O’Donovan, Liz
Wells, Kim E
Gait, Michael J
Wells, Dominic J
Tyler, Damian
Wood, Matthew J
author_facet Betts, Corinne A
McClorey, Graham
Healicon, Richard
Hammond, Suzan M
Manzano, Raquel
Muses, Sofia
Ball, Vicky
Godfrey, Caroline
Merritt, Thomas M
van Westering, Tirsa
O’Donovan, Liz
Wells, Kim E
Gait, Michael J
Wells, Dominic J
Tyler, Damian
Wood, Matthew J
author_sort Betts, Corinne A
collection PubMed
description Duchenne muscular dystrophy (DMD) is caused by loss of dystrophin protein, leading to progressive muscle weakness and premature death due to respiratory and/or cardiac complications. Cardiac involvement is characterized by progressive dilated cardiomyopathy, decreased fractional shortening and metabolic dysfunction involving reduced metabolism of fatty acids—the major cardiac metabolic substrate. Several mouse models have been developed to study molecular and pathological consequences of dystrophin deficiency, but do not recapitulate all aspects of human disease pathology and exhibit a mild cardiac phenotype. Here we demonstrate that Cmah (cytidine monophosphate-sialic acid hydroxylase)-deficient mdx mice (Cmah−/−;mdx) have an accelerated cardiac phenotype compared to the established mdx model. Cmah−/−;mdx mice display earlier functional deterioration, specifically a reduction in right ventricle (RV) ejection fraction and stroke volume (SV) at 12 weeks of age and decreased left ventricle diastolic volume with subsequent reduced SV compared to mdx mice by 24 weeks. They further show earlier elevation of cardiac damage markers for fibrosis (Ctgf), oxidative damage (Nox4) and haemodynamic load (Nppa). Cardiac metabolic substrate requirement was assessed using hyperpolarized magnetic resonance spectroscopy indicating increased in vivo glycolytic flux in Cmah−/−;mdx mice. Early upregulation of mitochondrial genes (Ucp3 and Cpt1) and downregulation of key glycolytic genes (Pdk1, Pdk4, Ppara), also denote disturbed cardiac metabolism and shift towards glucose utilization in Cmah−/−;mdx mice. Moreover, we show long-term treatment with peptide-conjugated exon skipping antisense oligonucleotides (20-week regimen), resulted in 20% cardiac dystrophin protein restoration and significantly improved RV cardiac function. Therefore, Cmah−/−;mdx mice represent an appropriate model for evaluating cardiac benefit of novel DMD therapeutics.
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spelling pubmed-63377032019-01-25 Cmah-dystrophin deficient mdx mice display an accelerated cardiac phenotype that is improved following peptide-PMO exon skipping treatment Betts, Corinne A McClorey, Graham Healicon, Richard Hammond, Suzan M Manzano, Raquel Muses, Sofia Ball, Vicky Godfrey, Caroline Merritt, Thomas M van Westering, Tirsa O’Donovan, Liz Wells, Kim E Gait, Michael J Wells, Dominic J Tyler, Damian Wood, Matthew J Hum Mol Genet General Article Duchenne muscular dystrophy (DMD) is caused by loss of dystrophin protein, leading to progressive muscle weakness and premature death due to respiratory and/or cardiac complications. Cardiac involvement is characterized by progressive dilated cardiomyopathy, decreased fractional shortening and metabolic dysfunction involving reduced metabolism of fatty acids—the major cardiac metabolic substrate. Several mouse models have been developed to study molecular and pathological consequences of dystrophin deficiency, but do not recapitulate all aspects of human disease pathology and exhibit a mild cardiac phenotype. Here we demonstrate that Cmah (cytidine monophosphate-sialic acid hydroxylase)-deficient mdx mice (Cmah−/−;mdx) have an accelerated cardiac phenotype compared to the established mdx model. Cmah−/−;mdx mice display earlier functional deterioration, specifically a reduction in right ventricle (RV) ejection fraction and stroke volume (SV) at 12 weeks of age and decreased left ventricle diastolic volume with subsequent reduced SV compared to mdx mice by 24 weeks. They further show earlier elevation of cardiac damage markers for fibrosis (Ctgf), oxidative damage (Nox4) and haemodynamic load (Nppa). Cardiac metabolic substrate requirement was assessed using hyperpolarized magnetic resonance spectroscopy indicating increased in vivo glycolytic flux in Cmah−/−;mdx mice. Early upregulation of mitochondrial genes (Ucp3 and Cpt1) and downregulation of key glycolytic genes (Pdk1, Pdk4, Ppara), also denote disturbed cardiac metabolism and shift towards glucose utilization in Cmah−/−;mdx mice. Moreover, we show long-term treatment with peptide-conjugated exon skipping antisense oligonucleotides (20-week regimen), resulted in 20% cardiac dystrophin protein restoration and significantly improved RV cardiac function. Therefore, Cmah−/−;mdx mice represent an appropriate model for evaluating cardiac benefit of novel DMD therapeutics. Oxford University Press 2019-02-01 2018-10-02 /pmc/articles/PMC6337703/ /pubmed/30281092 http://dx.doi.org/10.1093/hmg/ddy346 Text en © The Author(s) 2018. Published by Oxford University Press. http://creativecommons.org/licenses/by/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle General Article
Betts, Corinne A
McClorey, Graham
Healicon, Richard
Hammond, Suzan M
Manzano, Raquel
Muses, Sofia
Ball, Vicky
Godfrey, Caroline
Merritt, Thomas M
van Westering, Tirsa
O’Donovan, Liz
Wells, Kim E
Gait, Michael J
Wells, Dominic J
Tyler, Damian
Wood, Matthew J
Cmah-dystrophin deficient mdx mice display an accelerated cardiac phenotype that is improved following peptide-PMO exon skipping treatment
title Cmah-dystrophin deficient mdx mice display an accelerated cardiac phenotype that is improved following peptide-PMO exon skipping treatment
title_full Cmah-dystrophin deficient mdx mice display an accelerated cardiac phenotype that is improved following peptide-PMO exon skipping treatment
title_fullStr Cmah-dystrophin deficient mdx mice display an accelerated cardiac phenotype that is improved following peptide-PMO exon skipping treatment
title_full_unstemmed Cmah-dystrophin deficient mdx mice display an accelerated cardiac phenotype that is improved following peptide-PMO exon skipping treatment
title_short Cmah-dystrophin deficient mdx mice display an accelerated cardiac phenotype that is improved following peptide-PMO exon skipping treatment
title_sort cmah-dystrophin deficient mdx mice display an accelerated cardiac phenotype that is improved following peptide-pmo exon skipping treatment
topic General Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6337703/
https://www.ncbi.nlm.nih.gov/pubmed/30281092
http://dx.doi.org/10.1093/hmg/ddy346
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