Histone deacetylase inhibition blunts ischemia/reperfusion injury by inducing cardiomyocyte autophagy

M Xie, Y Kong, W Tan, H May, PK Battiprolu… - Circulation, 2014 - Am Heart Assoc
M Xie, Y Kong, W Tan, H May, PK Battiprolu, Z Pedrozo, ZV Wang, C Morales, X Luo, G Cho…
Circulation, 2014Am Heart Assoc
Background—Reperfusion accounts for a substantial fraction of the myocardial injury
occurring with ischemic heart disease. Yet, no standard therapies are available targeting
reperfusion injury. Here, we tested the hypothesis that suberoylanilide hydroxamic acid
(SAHA), a histone deacetylase inhibitor approved for cancer treatment by the US Food and
Drug Administration, will blunt reperfusion injury. Methods and Results—Twenty-one rabbits
were randomly assigned to 3 groups:(1) vehicle control,(2) SAHA pretreatment (1 day before …
Background
Reperfusion accounts for a substantial fraction of the myocardial injury occurring with ischemic heart disease. Yet, no standard therapies are available targeting reperfusion injury. Here, we tested the hypothesis that suberoylanilide hydroxamic acid (SAHA), a histone deacetylase inhibitor approved for cancer treatment by the US Food and Drug Administration, will blunt reperfusion injury.
Methods and Results
Twenty-one rabbits were randomly assigned to 3 groups: (1) vehicle control, (2) SAHA pretreatment (1 day before and at surgery), and (3) SAHA treatment at the time of reperfusion only. Each arm was subjected to ischemia/reperfusion surgery (30 minutes coronary ligation, 24 hours reperfusion). In addition, cultured neonatal and adult rat ventricular cardiomyocytes were subjected to simulated ischemia/reperfusion to probe mechanism. SAHA reduced infarct size and partially rescued systolic function when administered either before surgery (pretreatment) or solely at the time of reperfusion. SAHA plasma concentrations were similar to those achieved in patients with cancer. In the infarct border zone, SAHA increased autophagic flux, assayed in both rabbit myocardium and in mice harboring an RFP-GFP-LC3 transgene. In cultured myocytes subjected to simulated ischemia/reperfusion, SAHA pretreatment reduced cell death by 40%. This reduction in cell death correlated with increased autophagic activity in SAHA-treated cells. RNAi-mediated knockdown of ATG7 and ATG5, essential autophagy proteins, abolished SAHA’s cardioprotective effects.
Conclusions
The US Food and Drug Administration–approved anticancer histone deacetylase inhibitor, SAHA, reduces myocardial infarct size in a large animal model, even when delivered in the clinically relevant context of reperfusion. The cardioprotective effects of SAHA during ischemia/reperfusion occur, at least in part, through the induction of autophagic flux.
Am Heart Assoc