Gian Franco Gensini, Piera Angelica Merlini, Corrado Poggesi, Luciano Moretti, Francesco Fattirolli, Paolo G. Camici, Benedetta Tomberli, Giorgio Reggiardo, Vicent Climent, Lars S. Maier, Philipp Ehlermann, Iacopo Olivotto, Antonio Hernández Madrid, Claudius Jacobshagen, Gianfranco Sinagra, Monica Patten, Raffaele Coppini, Luiz Belardinelli, Alessandra Fornaro, Claudio Rapezzi, Antonello Ganau, Francisco Marin, Alessandro Mugelli, Olivotto, Iacopo, Camici, Paolo G, Merlini, Piera Angelica, Rapezzi, Claudio, Patten, Monica, Climent, Vicent, Sinagra, Gianfranco, Tomberli, Benedetta, Marin, Francisco, Ehlermann, Philipp, Maier, Lars S, Fornaro, Alessandra, Jacobshagen, Claudiu, Ganau, Antonello, Moretti, Luciano, Hernandez Madrid, Antonio, Coppini, Raffaele, Reggiardo, Giorgio, Poggesi, Corrado, Fattirolli, Francesco, Belardinelli, Luiz, Gensini, Gianfranco, Mugelli, Alessandro, Camici, Paolo G., and Maier, Lars S.
Background The late sodium current inhibitor ranolazine reverses the main electrophysiological and mechanical abnormalities of human hypertrophic cardiomyopathy (HCM) cardiomyocytes in vitro, suggesting potential clinical benefit. We aimed to assess the effect of ranolazine on functional capacity, symptomatic status, diastolic function, and arrhythmias in HCM. Methods and Results In this multicenter, double-blind, phase 2 study, 80 adult patients with nonobstructive HCM (age 53±14 years, 34 women) were randomly assigned to placebo (n=40) or ranolazine 1000 mg bid (n=40) for 5 months. The primary end point was change in peak VO 2 compared with baseline using cardiopulmonary exercise test. Echocardiographic lateral and septal E/E′ ratio, prohormone brain natriuretic peptide levels, 24-hour Holter arrhythmic profile, and quality of life were assessed. Ranolazine was safe and well tolerated. Overall, there was no significant difference in VO 2 peak change at 5 months in the ranolazine versus placebo group (delta 0.15±3.96 versus −0.02±4.25 mL/kg per minute; P =0.832). Ranolazine treatment was associated with a reduction in 24-hour burden of premature ventricular complexes compared with placebo (>50% reduction versus baseline in 61% versus 31%, respectively; P =0.042). However, changes in prohormone brain natriuretic peptide levels did not differ in the ranolazine compared with the placebo group (geometric mean median [interquartile range], −3 pg/mL [−107, 142 pg/mL] versus 78 pg/mL [−71, 242 pg/mL]; P =0.251). Furthermore, E/E′ ratio and quality of life scores showed no significant difference. Conclusions In patients with nonobstructive HCM, ranolazine showed no overall effect on exercise performance, plasma prohormone brain natriuretic peptide levels, diastolic function, or quality of life. The drug showed an excellent safety profile and was associated with reduced premature ventricular complex burden. Late sodium current inhibition does not seem to improve functional capacity in HCM. Clinical Trial Registration: URL: https://www.clinicaltrialsregister.eu . Unique identifier: 2011-004507-20