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Differential DNA Methylation Correlates with Differential Expression of Angiogenic Factors in Human Heart Failure

Epigenetic mechanisms such as microRNA and histone modification are crucially responsible for dysregulated gene expression in heart failure. In contrast, the role of DNA methylation, another well-characterized epigenetic mark, is unknown. In order to examine whether human cardiomyopathy of different...

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Autores principales: Movassagh, Mehregan, Choy, Mun-Kit, Goddard, Martin, Bennett, Martin R., Down, Thomas A., Foo, Roger S.-Y.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2797324/
https://www.ncbi.nlm.nih.gov/pubmed/20084101
http://dx.doi.org/10.1371/journal.pone.0008564
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author Movassagh, Mehregan
Choy, Mun-Kit
Goddard, Martin
Bennett, Martin R.
Down, Thomas A.
Foo, Roger S.-Y.
author_facet Movassagh, Mehregan
Choy, Mun-Kit
Goddard, Martin
Bennett, Martin R.
Down, Thomas A.
Foo, Roger S.-Y.
author_sort Movassagh, Mehregan
collection PubMed
description Epigenetic mechanisms such as microRNA and histone modification are crucially responsible for dysregulated gene expression in heart failure. In contrast, the role of DNA methylation, another well-characterized epigenetic mark, is unknown. In order to examine whether human cardiomyopathy of different etiologies are connected by a unifying pattern of DNA methylation pattern, we undertook profiling with ischaemic and idiopathic end-stage cardiomyopathic left ventricular (LV) explants from patients who had undergone cardiac transplantation compared to normal control. We performed a preliminary analysis using methylated-DNA immunoprecipitation-chip (MeDIP-chip), validated differential methylation loci by bisulfite-(BS) PCR and high throughput sequencing, and identified 3 angiogenesis-related genetic loci that were differentially methylated. Using quantitative RT-PCR, we found that the expression of these genes differed significantly between CM hearts and normal control (p<0.01). Moreover, for each individual LV tissue, differential methylation showed a predicted correlation to differential expression of the corresponding gene. Thus, differential DNA methylation exists in human cardiomyopathy. In this series of heterogenous cardiomyopathic LV explants, differential DNA methylation was found in at least 3 angiogenesis-related genes. While in other systems, changes in DNA methylation at specific genomic loci usually precede changes in the expression of corresponding genes, our current findings in cardiomyopathy merit further investigation to determine whether DNA methylation changes play a causative role in the progression of heart failure.
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spelling pubmed-27973242010-01-16 Differential DNA Methylation Correlates with Differential Expression of Angiogenic Factors in Human Heart Failure Movassagh, Mehregan Choy, Mun-Kit Goddard, Martin Bennett, Martin R. Down, Thomas A. Foo, Roger S.-Y. PLoS One Research Article Epigenetic mechanisms such as microRNA and histone modification are crucially responsible for dysregulated gene expression in heart failure. In contrast, the role of DNA methylation, another well-characterized epigenetic mark, is unknown. In order to examine whether human cardiomyopathy of different etiologies are connected by a unifying pattern of DNA methylation pattern, we undertook profiling with ischaemic and idiopathic end-stage cardiomyopathic left ventricular (LV) explants from patients who had undergone cardiac transplantation compared to normal control. We performed a preliminary analysis using methylated-DNA immunoprecipitation-chip (MeDIP-chip), validated differential methylation loci by bisulfite-(BS) PCR and high throughput sequencing, and identified 3 angiogenesis-related genetic loci that were differentially methylated. Using quantitative RT-PCR, we found that the expression of these genes differed significantly between CM hearts and normal control (p<0.01). Moreover, for each individual LV tissue, differential methylation showed a predicted correlation to differential expression of the corresponding gene. Thus, differential DNA methylation exists in human cardiomyopathy. In this series of heterogenous cardiomyopathic LV explants, differential DNA methylation was found in at least 3 angiogenesis-related genes. While in other systems, changes in DNA methylation at specific genomic loci usually precede changes in the expression of corresponding genes, our current findings in cardiomyopathy merit further investigation to determine whether DNA methylation changes play a causative role in the progression of heart failure. Public Library of Science 2010-01-13 /pmc/articles/PMC2797324/ /pubmed/20084101 http://dx.doi.org/10.1371/journal.pone.0008564 Text en Movassagh 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
Movassagh, Mehregan
Choy, Mun-Kit
Goddard, Martin
Bennett, Martin R.
Down, Thomas A.
Foo, Roger S.-Y.
Differential DNA Methylation Correlates with Differential Expression of Angiogenic Factors in Human Heart Failure
title Differential DNA Methylation Correlates with Differential Expression of Angiogenic Factors in Human Heart Failure
title_full Differential DNA Methylation Correlates with Differential Expression of Angiogenic Factors in Human Heart Failure
title_fullStr Differential DNA Methylation Correlates with Differential Expression of Angiogenic Factors in Human Heart Failure
title_full_unstemmed Differential DNA Methylation Correlates with Differential Expression of Angiogenic Factors in Human Heart Failure
title_short Differential DNA Methylation Correlates with Differential Expression of Angiogenic Factors in Human Heart Failure
title_sort differential dna methylation correlates with differential expression of angiogenic factors in human heart failure
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2797324/
https://www.ncbi.nlm.nih.gov/pubmed/20084101
http://dx.doi.org/10.1371/journal.pone.0008564
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