Evaluation of a New Bipyridine Inotropic Agent — Milrinone — in Patients with Severe Congestive Heart Failure

Baim, Donald S.; McDowell, Alex; Cherniles, J; Monrad, E. Scott; Parker, Jack; Edelson, Jerome; Braunwald, Eugene; Grossman, William

doi:10.1056/nejm198309293091302

Cited by 328 publications

(75 citation statements)

References 30 publications

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“…We have observed that an excessive reduction in left heart filling pressure with intravenous administration of milrinone can result in a marked attenuation of the drug's apparent positive inotropic effect as reflected by peak positive dP/dt.25 Thus an excessive reduction in preload caused by the intravenous administration of a cardiac bipyridine, particularly in a patient whose initial filling pressures are not elevated, could obscure the drug's positive inotropic action. With regard to the few patients who did demonstrate an apparent positive inotropic response in the study of Wilmshurst et al, 3 it was postulated that increased contractility was the result of an indirect effect of the drug to increase sympathetic tone. '6 This mechanism cannot explain the positive inotropic effects of intracoronary infusion of milrinone in the present study because there were significant decreases in both heart rate and norepinephrine levels, suggesting that sympathetic tone was actually reduced, most likely due to reflex withdrawal.…”

Section: Methodsmentioning

confidence: 99%

Separation of the direct myocardial and vasodilator actions of milrinone administered by an intracoronary infusion technique.

Ludmer¹,

Wright²,

Arnold³

et al. 1986

Circulation

123

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To determine the relative contributions of milrinone's positive inotropic and vasodilator actions in patients with severe congestive heart failure, the drug was administered by constant infusion directly into the left main coronary artery of 11 patients with New York Heart Association functional class III or IV heart failure. Intracoronary infusion of milrinone at rates up to 50 ,ug/min had no effect on mean arterial pressure or systemic vascular resistance but resulted in dose-related increases in peak positive dP/dt ( + 21%), stroke volume index ( + 18%), and stroke work index ( + 21%) and decreases in heart rate (-33%), mean right atrial pressure (-25%), and left ventricular end-diastolic pressure (-17%). In eight patients, intravenous administration (75 jig/kg) after the intracoronary infusion resulted in significant decreases in mean arterial pressure (-14%) and systemic vascular resistance ( 40%), further increase in stroke volume index compared with intracoronary administration, and further decreases in mean right atrial and left ventricular end-diastolic pressures compared with intracoronary administration. These data indicate that milrinone exerts both positive inotropic and vasodilator actions that contribute significantly to the drug's overall hemodynamic effect.

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Section: Methodsmentioning

confidence: 99%

Separation of the direct myocardial and vasodilator actions of milrinone administered by an intracoronary infusion technique.

Ludmer¹,

Wright²,

Arnold³

et al. 1986

Circulation

123

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“…Recently their clinical efficacy has been challenged (Editorial, 1978;Editorial, 1979;Petch, 1979) and at the same time vasodilators (Franciosa, 1982;Packer & Le Jemtel, 1982;Packer, 1983) and positive inotropic drugs have become available as alternative treatments (Baim et al, 1983;Dawson et al, 1983). In addition the understanding of the pathophysiology of heart failure has advanced (Harris, 1983).…”

Section: Introductionmentioning

confidence: 99%

The role of digitalis in the future.

Pa¹

1984

Brit J Clinical Pharma

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Cardiac glycosides exert an acute positive inotropic effect on the normal and failing heart. Recent evidence establishes that the positive inotropic effect is maintained over several months in many patients. The effectiveness of long‐term treatment with cardiac glycosides in relieving symptoms is less certain; only a small subset of patients benefits. An effect on mortality is not established. The use of digoxin in the treatment of mild heart failure is questionable since the drug has serious side‐effects and the efficacy in patients already taking diuretics has not been established. The use of glycosides in the treatment of severe chronic heart failure is being challenged because of the availability of powerful diuretics, new vasodilators and alternative positive inotropes.

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“…2 The clinical response of patients with congestive heart failure who are treated with this agent has been ascribed to readily demonstrable improvements in indexes of left ventric-ular systolic function (including increases in peak positive dP/dt and in left ventricular ejection fraction) and concurrent arteriolar vasodilation. 3 However, possible effects of milrinone on ventricular diastolic function, which might also contribute to the hemodynamic response to this agent, have not been evaluated. In particular, improved diastolic relaxation and distensibility might lead to more effective sarcomere stretch within the ventricular myocardium and to better systolic performance.6 7 Thus it is possible that improved systolic pump function in patients with heart failure treated with milrinone might reflect a complex interaction of effects of the drug on systolic and diastolic properties of the ventricular myocardium as well as changes in the peripheral vasculature.…”

mentioning

confidence: 99%

Improvement in indexes of diastolic performance in patients with congestive heart failure treated with milrinone.

Monrad¹,

McKay²,

Baim³

et al. 1984

Circulation

186

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To elucidate the mechanisms by which the new bipyridine inotropic agent milrinone improves cardiac function, we examined multiple indexes of left ventricular diastolic function before and after administration of milrinone to patients with advanced (NYHA class III or IV) congestive heart failure. In 13 patients left ventricular pressure measurements were made with a micromanometer to permit assessment of peak negative dP/dt and the time constant of left ventricular isovolumic relaxation, T, before and after milrinone. In nine patients radionuclide ventriculographic studies were performed during left heart catheterization, allowing calculation of left ventricular peak filling rate, volumes, and the diastolic pressure-volume relationship before and after milrinone. After intravenous administration of milrinone, peak negative dP/dt increased ( + 18%; p < .01 ) and T decreased (-30%; p < .01), while heart rate increased by only 8% (87 + 12 to 94 + 15 beats/min; p < .01), left ventricular systolic pressure did not change, and mean aortic pressure fell by 11% (p < .01). Left ventricular peak filling rate increased (1.2 + 0.6 to 1.7 + 0.7 end-diastolic volumes/sec; p .02) despite a decrease in left ventricular filling pressure (mean pulmonary wedge pressure 27 ± 7 to 18 9 mm Hg; p < .01). There was a fall in left ventricular end-diastolic pressure (28.6 + 6 to 19 + 7 mm Hg; p ' .01), with no significant change in left ventricular end-diastolic volume. This was associated with a downward shift in the left ventricular diastolic pressure-volume relationship in most cases. These changes in parameters of left ventricular diastolic relaxation and chamber distensibility after administration of milrinone suggest that improved diastolic function may contribute to the beneficial hemodynamic effect of milrinone in patients with congestive heart failure. Circulation 70, No. 6, 1030-1037, 1984 MILRINONE, a derivative of the bipyridine inotrope amrinone, has previously been shown to have a profound effect on myocardial contractile function in isolated muscle' and animal preparations.2 The clinical response of patients with congestive heart failure who are treated with this agent has been ascribed to readily demonstrable improvements in indexes of left ventric- Received Feb. 22, 1984; revision accepted Sept. 6, 1984. Presented in part at the 56th Annual Scientific Sessions of the American Heart Association. Anaheim, November 1983. 1030 ular systolic function (including increases in peak positive dP/dt and in left ventricular ejection fraction) and concurrent arteriolar vasodilation.3However, possible effects of milrinone on ventricular diastolic function, which might also contribute to the hemodynamic response to this agent, have not been evaluated. In particular, improved diastolic relaxation and distensibility might lead to more effective sarcomere stretch within the ventricular myocardium and to better systolic performance.6 7 Thus it is possible that improved systolic pump function in patients with heart failure treate...

show abstract

Evaluation of a New Bipyridine Inotropic Agent — Milrinone — in Patients with Severe Congestive Heart Failure

Cited by 328 publications

References 30 publications

Separation of the direct myocardial and vasodilator actions of milrinone administered by an intracoronary infusion technique.

Separation of the direct myocardial and vasodilator actions of milrinone administered by an intracoronary infusion technique.

The role of digitalis in the future.

Improvement in indexes of diastolic performance in patients with congestive heart failure treated with milrinone.

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