Genome-wide DNA methylation encodes cardiac transcriptional reprogramming in human ischemic heart failure.
Mark E PepinChae-Myeong HaDavid K CrossmanSilvio H LitovskySooryanarayana VaramballyJoseph P BarchueSalpy V PamboukianNikolaos A DiakosStavros G DrakosSteven M PogwizdAdam R WendePublished in: Laboratory investigation; a journal of technical methods and pathology (2018)
Ischemic cardiomyopathy (ICM) is the clinical endpoint of coronary heart disease and a leading cause of heart failure. Despite growing demands to develop personalized approaches to treat ICM, progress is limited by inadequate knowledge of its pathogenesis. Since epigenetics has been implicated in the development of other chronic diseases, the current study was designed to determine whether transcriptional and/or epigenetic changes are sufficient to distinguish ICM from other etiologies of heart failure. Specifically, we hypothesize that genome-wide DNA methylation encodes transcriptional reprogramming in ICM. RNA-sequencing analysis was performed on human ischemic left ventricular tissue obtained from patients with end-stage heart failure, which enriched known targets of the polycomb methyltransferase EZH2 compared to non-ischemic hearts. Combined RNA sequencing and genome-wide DNA methylation analysis revealed a robust gene expression pattern consistent with suppression of oxidative metabolism, induced anaerobic glycolysis, and altered cellular remodeling. Lastly, KLF15 was identified as a putative upstream regulator of metabolic gene expression that was itself regulated by EZH2 in a SET domain-dependent manner. Our observations therefore define a novel role of DNA methylation in the metabolic reprogramming of ICM. Furthermore, we identify EZH2 as an epigenetic regulator of KLF15 along with DNA hypermethylation, and we propose a novel mechanism through which coronary heart disease reprograms the expression of both intermediate enzymes and upstream regulators of cardiac metabolism such as KLF15.
Keyphrases
- dna methylation
- heart failure
- genome wide
- gene expression
- left ventricular
- transcription factor
- endothelial cells
- cardiac resynchronization therapy
- single cell
- copy number
- ischemia reperfusion injury
- hypertrophic cardiomyopathy
- acute heart failure
- mitral valve
- acute myocardial infarction
- left atrial
- high glucose
- atrial fibrillation
- microbial community
- long noncoding rna
- wastewater treatment
- poor prognosis
- pluripotent stem cells
- induced pluripotent stem cells
- cell free
- oxidative stress
- binding protein
- heat stress
- heat shock