ACE inhibitors significantly reduced MMP-2 activity and prevented left ventricular dilatation and myocardial hypertrophy in a rat model of heart failure.
Does ACE inhibitor treatment reduce MMP-2 activity and prevent left ventricular remodeling in a rat model of heart failure?
ACE inhibitors prevent MMP-2 activity, providing a potential mechanism for their ability to prevent negative structural and functional changes in heart failure.
Angiotensin-converting enzyme (ACE) inhibitors represent the front-line pharmacological treatment of heart failure, which is characterized by left ventricular (LV) dilatation and inappropriate hypertrophy. The mechanism of action of ACE inhibitors is still unclear, but evidence suggests that they may act by influencing matrix metalloproteinase (MMP) activity. This study sought to determine whether ACE inhibitors can directly regulate MMP activity and whether this results in positive structural and functional adaptations to the heart. To this end, MMP-2 activity in LV tissue extracted from rats with an aortocaval (AV) fistula was assessed by in vitro incubation as well as in vivo treatment with captopril, lisinopril, or quinapril. Furthermore, LV size and function were determined in untreated AV fistula rats, AV fistula rats treated with lisinopril (3, 5, and 8 wk), and age-matched sham-operated controls. In vitro incubation with captopril, lisinopril, or quinapril significantly reduced MMP-2 activity, as did in vivo treatment. This occurred without a reduction in the available pool of MMP-2 protein. Long-term in vivo administration of lisinopril also prevented LV dilatation, attenuated myocardial hypertrophy, and prevented changes in myocardial compliance and contractility. The results herein demonstrate that ACE inhibitors prevent MMP-2 activity and, in so doing, represent a mechanism responsible for preventing the negative structural and functional changes that occur in the rat AV fistula model of heart failure.
Brower et al. (Sat,) conducted a other in Heart failure (rat model). ACE inhibitors (captopril, lisinopril, or quinapril) vs. Untreated AV fistula rats and age-matched sham-operated controls was evaluated on MMP-2 activity, LV size, and function. ACE inhibitors significantly reduced MMP-2 activity and prevented left ventricular dilatation and myocardial hypertrophy in a rat model of heart failure.