Adverse mortality effect of central sympathetic inhibition with sustained-release moxonidine in patients with heart failure (MOXCON)

doi:10.1016/S1388-9842(03)00163-6

European Journal of Heart Failure 2003 5(5):659-667; doi:10.1016/S1388-9842(03)00163-6

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Adverse mortality effect of central sympathetic inhibition with sustained-release moxonidine in patients with heart failure (MOXCON)

Jay N. Cohn^a^,*, Marc A. Pfeffer^b, Jean Rouleau^c, Norman Sharpe^d, Karl Swedberg^e, Matthias Straub^f, Curtis Wiltse^g, Theressa J. Wright^g and for the MOXCON Investigators

^a Cardiovascular Division Mayo Mail Code 508, University of Minnesota Medical School 420 Delaware Street SE, Minneapolis, MN 55455, USA
^b Brigham and Women's Hospital, Harvard Medical School Boston, MA, USA
^c University of Toronto Toronto, Ont., Canada
^d University of Auckland Auckland, New Zealand
^e Sahlgrenska University Hospital Göteborg, Sweden
^f Solvay Pharmaceuticals B.V., Weesp The Netherlands
^g Eli Lilly and Company Indianapolis, IN, USA

^* Corresponding author. Tel.: +1-612-625-5646; fax: +1-612-624-2174. E-mail address: cohnx001{at}umn.edu

Abstract

Background: The association between sympathetic activation and mortalityin chronic heart failure and the favorable effect of beta blockingdrugs has raised the possibility of therapeutic efficacy forcentral sympathetic inhibition with sustained-release (SR) moxonidine,an imidazoline receptor agonist.

Methods: A randomized double-blind, placebo-controlled trial was initiatedin 425 centers in 17 countries with a plan to enter 4533 patientswith New York Heart Association class II–IV heart failureand a reduced ejection fraction. Moxonidine SR or matching placebowas titrated to a target dose of 1.5 mg BID. The trial was poweredto detect a 20% reduction in mortality, which required a totalof 724 deaths.

Findings: An early increase in death rate and adverse events in the moxonidineSR group led to premature termination of the trial because ofsafety concerns after 1934 patients were entered. Final analysisrevealed 54 deaths (5.5%) in the moxonidine SR group and 32deaths (3.4%) in the placebo group during the active treatmentphase. Survival curves revealed a significantly (P=0.012) worseoutcome in the moxonidine SR group. Hospitalization for heartfailure, acute myocardial infarction and adverse events werealso more frequent in the moxonidine SR group. Plasma norepinephrinewas significantly decreased by moxonidine SR (–18.8% frombaseline) vs. placebo (+6.9%).

Interpretation: Early termination of the trial limited conclusions regardingthe long-term effects of central sympathetic inhibition. Nonetheless,the excess early mortality and morbidity suggest the likelihoodof an adverse effect of moxonidine SR and raise concerns regardingthe efficacy of generalized sympathetic inhibition in heartfailure.

Key Words: Mortality • Moxonidine • Chronic heart failure

Received September 12, 2003; Accepted September 13, 2003

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