Circulation, Vol 63, 96-101, Copyright © 1981 by American Heart Association
NA Awan, MK Evenson, KE Needham, TO Evans, J Hermanovich, CR Taylor, E Amsterdam and DT Mason
The achievement of satisfactory ambulatory therapy of severe chronic
congestive heart failure may be helped by the development of safe and
orally effective cardiotonic agents. Therefore, we evaluated by cardiac
catheterization and limb plethysmography the temporal cardiocirculatory
responses of the new ingestible beta agonist pirbuterol in 10 coronary
heart disease patients with severe congestive heart failure refractory to
digitalis and diuretics. After a single oral dose of 0.4 mg/kg, ventricular
dysfunction was considerably improved during 6 hours of hemodynamic
monitoring. Cardiac index increased from a control of 1.7 l/min/m2 to 2.6
l/min/m2 (p < 0.001) at 1 hour and to 2.4 l/min/m2 (p < 0.005) at 3
hours and was 2.2 l/min/m2 (p < 0.001) at 6 hours; left ventricular
filling pressure decreased from a control of 24 mm Hg to 19 mm Hg (p <
0.005) at 1 hour and to 18 mm Hg (p < 0.005) at 3 hours and was 22 mm Hg
(p < 0.05) at 6 hours. Concomitantly, the peak increment in heart rate
(6 beats/min) was minimal and without ectopy and mean arterial blood
pressure decreased only 10 mm Hg. total systemic vascular resistance
declined by 887 dyn-sec-cm-5, forearm venodilation occurred and the
rate-pressure product was unaltered. Thus, oral pirbuterol provides
beneficial hemodynamic effects in patients with severe left ventricular
dysfunction and appears potentially useful for long-term management of
low-output congestive heart failure.
ARTICLES
Hemodynamic effects of oral pirbuterol in chronic severe congestive heart failure