Heart Diseases Clinical Trial
Official title:
Reversal of Cardiomyopathy by Suppression of Frequent Premature Ventricular Complexes - A Prospective Randomized Clinical Trial
Frequent monomorphic premature ventricular complexes (PVCs) may cause a cardiomyopathy (CMP) that is reversible by suppression of the ectopic focus. This study investigates whether PVC suppression therapy can improve cardiac function and clinical condition of patients with idiopathic or ischemic CMP and frequent monomorphic PVCs. For this purpose, patients will be randomized to either one of two treatment strategies: 1) conventional heart failure therapy plus PVC suppression therapy, consisting of RFCA as primary treatment and Amiodarone as secondary treatment in case of unsuccessful RFCA, or 2) conventional heart failure therapy without PVC suppression therapy.
Heart failure accounts for substantial morbidity and mortality in the western world. In
addition, the financial burden associated with the disease is considerable. Prognosis is
generally poor and quality of life is significantly reduced. The causes of heart failure are
diverse. Identification of the underlying pathophysiological mechanism is essential, because
a specific patient tailored therapy may help to improve the clinical status of the
individual patient. In addition, some patients may have a potentially reversible
cardiomyopathy (CMP). The present study will focus on the role of frequent premature
ventricular contractions (PVCs) as a cause of left ventricular (LV) dysfunction. This is a
potential reversible CMP generally unknown to the cardiological society.
Frequent ventricular ectopy in patients without structural heart disease is generally
thought to be a benign finding with no prognostic significance. Suppression of PVCs with
anti-arrhythmic drugs or catheter ablation is therefore usually only considered when PVCs
are accompanied by disabling symptoms. However, recent data suggest that frequent
monomorphic PVCs (symptomatic or asymptomatic) can cause a form of CMP that may be
reversible by suppression of the ectopic focus. Furthermore, the high prevalence of frequent
PVCs in patients with heart disease suggests that PVC-induced CMP may be a common
phenomenon. Suppression of frequent monomorphic PVCs to improve LV systolic function may
therefore emerge as a new and effective treatment strategy for patients with heart failure.
Beta-blockers are safe and effective anti-arrhythmic agents and are considered the first
line therapy for suppression of PVCs. Most patients with HF are already taking a
beta-blocker as part of standard therapy for their underlying disease. According to
international guidelines, other AADs can be used if beta-blockers are ineffective, but they
have potential adverse (arrhythmic) side-effects, especially in patients with diminished LV
function, and may even be contra-indicated in this patient group. In patients with LV
dysfunction and frequent monomorphic PVCs that are refractory to beta-blockers, long-term
drug therapy and the potential adverse (arrhythmic) side-effects of AADs can be avoided by
using catheter ablation as a first alternative treatment. RFCA is already a frequently
applied, widely accepted, safe, effective and potentially curative treatment for symptomatic
drug refractory PVCs. It has also been safely and effectively employed in patients with
tachycardia-induced CMP and patients with PVC-induced CMP. A high acute success rate of 93%
and a very low PVC recurrence rate of 3% have been reported. Although recent available data
suggest that elimination of the PVC source by RFCA improves LV systolic function in HF
patients, it is still applied in a limited fashion for this indication because the evidence
supporting this is weak. The patient series published so far were not controlled and
retrospective in nature. We intend to conduct a controlled, randomized, prospective study
with careful documentation and long-term follow-up to evaluate the effect of PVC suppression
therapy (with RFCA as primary treatment) on cardiac systolic function in patients with CMP
and beta-blocker refractory frequent monomorphic PVCs. This could establish suppression of
frequent monomorphic PVCs as a potential curative treatment strategy for patients with HF.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Single Blind (Outcomes Assessor), Primary Purpose: Treatment
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