Downregulation of peroxisome proliferator–activated receptor-α gene expression in a mouse model of ischemic cardiomyopathy is dependent on reactive oxygen …

O Dewald, S Sharma, J Adrogue, R Salazar, GD Duerr… - Circulation, 2005 - Am Heart Assoc
O Dewald, S Sharma, J Adrogue, R Salazar, GD Duerr, JD Crapo, ML Entman
Circulation, 2005Am Heart Assoc
Background—The peroxisome proliferators–activated receptor-α (PPARα), a transcription
factor that modulates fatty acid metabolism, regulates substrate preference in the heart.
Although in acute ischemia there is a switch in substrate preference from fatty acids to
glucose, metabolic gene expression in repetitive ischemia is not well described. In a mouse
model of ischemic cardiomyopathy induced by repetitive ischemia/reperfusion (I/R), we
postulated that downregulation of PPARα is regulated by reactive oxygen species and is …
Background— The peroxisome proliferators–activated receptor-α (PPARα), a transcription factor that modulates fatty acid metabolism, regulates substrate preference in the heart. Although in acute ischemia there is a switch in substrate preference from fatty acids to glucose, metabolic gene expression in repetitive ischemia is not well described. In a mouse model of ischemic cardiomyopathy induced by repetitive ischemia/reperfusion (I/R), we postulated that downregulation of PPARα is regulated by reactive oxygen species and is necessary for maintaining contractile function in the heart.
Methods and Results— Repetitive closed-chest I/R (15 minutes) was performed daily in C57/BL6 mice, mice overexpressing extracellular superoxide dismutase, and mice treated with the PPARα agonist-WY-14,643. Echocardiography, histology, and candidate gene expression were measured at 3, 5, 7, and 28 days of repetitive I/R and 15 and 30 days after discontinuation of I/R. Repetitive I/R was associated with a downregulation of PPARα-regulated genes and both myosin heavy chain isoform transcript levels, which was reversible on discontinuation of I/R. Overexpression of EC-SOD prevented the downregulation of PPARα-regulated genes and myosin iso-genes by repetitive I/R. Furthermore, reactivation of PPARα in mice exposed to repetitive I/R worsened contractile function, induced microinfarctions, and increased intramyocardial triglyceride deposition, features suggestive of cardiac lipotoxicity.
Conclusions— Metabolic and myosin isoform gene expression in repetitive I/R is mediated by reactive oxygen species. Furthermore, we suggest that downregulation of PPARα in repetitive I/R is an adaptive mechanism that is able to prevent lipotoxicity in the ischemic myocardium.
Am Heart Assoc