Authors
Beau Olivier van Driel, Stephan A C Schoonvelde, Sonia Borodzicz-Jazdzyk, Roy Huurman, Julia Visch, Lourens Robbers, Hans Harms, Judith Verhagen, Alexa Vermeer, Joost van den Aardweg, Albert C van Rossum, Tjeerd Germans, Michelle Michels, Jolanda van der Velden
Published in
Cardiovascular research. Jul 02, 2025. Epub Jul 02, 2025.
Abstract
Previous studies have shown that individuals with a hypertrophic cardiomyopathy (HCM) pathogenic variant (PV) or likely pathogenic variant (LPV) without a HCM phenotype (PV/LPV carrier) have decreased myocardial external efficiency (MEE), which is thought to be a key pathomechanism in the onset and progression of HCM. Metabolic treatments improved exercise capacity in HCM patients, but evidence that such drugs correct reduced MEE is lacking. The ENERGY trial is a double-blind, placebo-controlled randomized clinical trial to define if the metabolic drug trimetazidine (TMZ) corrects reduced MEE in PV/LPV carriers for HCM.
51 MYBPC3 or MYH7 PV/LPV carriers were screened after which 40 were included and randomized into a treatment group (n=20) or placebo group (n=20) stratified for sex. Participants were treated with TMZ 20mg or placebo three times daily during eight weeks. The main outcome of this study was MEE as measured by [11C]-acetate positron emission tomography/computed tomography (PET/CT) and cardiac magnetic resonance (CMR) scan. Secondary outcomes were exercise parameters as measured by cardio-pulmonary exercise testing (CPET). Drug safety was monitored by (serious) adverse event registration.Treatment groups were comparable in terms of age, sex, body mass index, P/LP gene variant, and echocardiographic parameters without significant differences. Baseline CMR parameters and MEE were not significantly different between treatment groups. Eight weeks of treatment with TMZ did not significantly alter MEE compared to placebo. The mean MEE changed from 30.3±3.8 to 29.8±4.3 percent in the placebo group and from 30.1±4 to 29.1±4 percent in the TMZ group. Compared to placebo, the TMZ group did not have a significantly different MEE (difference -0.44, 95% interaction CI, -2.863 to 1.986, P=0.68). The mean V'O2max as a percentage of predicted V'O2max (V'O2max %pred) changed from 108±17 to 111±19 (95% CI, -6 to 10, P=0.84) percent in the placebo group and from 105±17 to 113±14 (95% CI, 1 to 16, P=0.03) percent in the TMZ group. After adjustment for baseline, the TMZ group had a significantly increased V'O2max %pred (difference 6.37, 95% interaction CI, -3 to 16, P=0.04).
The ENERGY trial is the first proof-of-concept randomized controlled trial to test the hypothesis that TMZ improves MEE in MYBPC3 or MYH7 PV/LPV carriers. We conclude that metabolic therapy with TMZ may not correct the P/LP gene variant-related decrease in MEE.
Netherlands Trial Register NL7492 (URL https://onderzoekmetmensen.nl/nl/trial/25078).
PMID:
40601822
Bibliographic data and abstract were imported from PubMed on 03 Jul 2025.
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