Heart Failure, Congestive Clinical Trial
Official title:
Prospective Randomized Outcomes Study of Acutely Decompensated Congestive Heart Failure Treated Initially in Outpatients With Natrecor (Nesiritide) - The PROACTION Trial
The purpose of this pilot study is to compare the clinical effects, safety profile, and economic impact of standard therapy plus Natrecor® (nesiritide, a recombinant form of the natural human peptide normally secreted by the heart in response to heart failure) to standard therapy plus placebo in patients who present to the Emergency Department with worsening congestive heart failure (CHF) and are treated in the Emergency Department /Observation Unit.
Congestive heart failure (CHF) is a public health epidemic in the U.S., affecting almost 5
million Americans. It is associated with a 5-year mortality rate of 50% (according to the
American Heart Association, 1999) and is currently the most costly cardiovascular disease in
the U.S. (according to Rich MW et al 1999 and O'Connell JB 2000). In 1999, the total
estimated direct and indirect costs associated with the treatment of CHF approached $56
billion (according to O'Connell JB 2000). Advanced CHF accounts for over 1 million hospital
admissions annually in the U.S.and for a large portion of the total expense to third-party
payers, due to the high cost of acute inpatient care and related Emergency Department
visits.
Emergency Departments are the last line of defense against hospital admission for CHF.
Operational and liability issues that pertain to the typical Emergency Department lead to
hospital admission for most CHF patients. Yet, problems with bed availability may lead to
the delayed transfer of patients from the Emergency Department to the inpatient unit,
further delaying important treatment. To address this, many Emergency Departments have
developed extended-stay policies for the observation and continuing care of patients who
cannot be discharged from the Emergency Department within a few hours of arrival. With an
extended stay (< 24 hours) for evaluation and treatment in the Emergency Department,
hospital admission for CHF may be significantly reduced by adequately ruling out coronary
ischemia and aggressively treating the precipitating factor of the decompensation. This
allows physicians to better assess the appropriateness of admission for the patient
(according to Graff LG 1993 ). Initiation of a safe and effective acute therapy in addition
to usual standard care may make it possible to further reduce hospital admissions or the
severity of the patient's condition at the time of the admission.
Natrecor® has been approved for use in the treatment of acutely decompensated CHF patients
with dyspnea at rest or with minimal activity. It is a recombinant form (produced by genetic
engineering) of naturally occurring human B-type natriuretic peptide (BNP, also known as
brain natriuretic peptide) produced primarily by the ventricular myocardium (according to
Hosoda K et al 1991). Natrecor® has been well tolerated in controlled clinical trials
involving more than 1000 patients with CHF. The data from these previous studies suggest
that doses of Natrecor® may be a potent agent for the treatment of acute CHF with a unique
combination of desirable effects on the flow of blood throughout the body; the hormones
secreted by the nervous system; and support of copious salt outputs by the renal system not
provided by currently available therapies (according to LeJemtel TH et al 1998). Although
Natrecor® has not been studied in the setting of an Emergency Department, it has been
administered as a fixed-dose infusion without invasive monitoring to over 500 patients.
Furthermore, Natrecor® has not been associated with an increase in cardiac ectopy or
arrhythmias in both placebo-controlled and active-controlled trials (according to Burger AJ
et al 1999 and Mills RM et al 1999).
This multicenter, randomized, double-blinded pilot study compares the clinical effects,
safety profile, and economic impact of standard therapy plus Natrecor® to standard therapy
plus placebo in the treatment of acutely decompensated CHF in an Emergency
Department/Observation Unit setting. Study drug (Natrecor® or placebo) is administered as a
bolus of 2 mcg/kg over approximately 60 seconds, immediately followed by a fixed-rate
infusion of 0.01 mcg/kg/min for at least 12 hours. Subjects who continue to receive study
drug and who remain in the Emergency Department/Observation Unit beyond 12 hours, up to 24
hours, have vital signs measured at 18 hours, 24 hours, immediately before discontinuation
of study drug, and at 30 minutes, 1 hour, and 2 hours after discontinuation of study drug.
Also, global clinical and dyspnea (difficulty breathing and shortness of breath)
evaluations, and a visual monitoring scale for dyspnea, are completed at the time of
termination of study drug in the Emergency Department/Observation Unit, or admission to the
hospital. The health-economic analysis focuses on resource utilization and cost of care for
initial treatment in the Emergency Department/Observation Unit and inpatient facility (if
admitted), as well as any subsequent treatment in an Emergency Department or acute inpatient
facility within the 30-day study period.
The study hypothesis is that the efficacy and safety profile of Natrecor® may be conducive
to its early administration for acute treatment of heart failure in the Emergency Department
and that in addition to standard care, may make it possible to further reduce hospital
admissions or the severity of the patient's condition at the time of admission. Natrecor®
1.5 mg for injection made up to final concentration of 0.3 mg/mL with 5% dextrose in water,
or placebo. Dispensed as an intravenous bolus of 2 mcg/kg over approximately 60 seconds,
immediately followed by a fixed-rate infusion of 0.01 mcg/kg/min for at least 12 hours.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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