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10 results on '"Milrinone -- Health aspects"'

2. Rationale and design of the OPTIME CHF trial: outcomes of a prospective trial of intravenous milrinone for exacerbations of chronic heart failure

Author

Cuffe, Michael S., Califf, Robert M., Adams, Kirkwood F., Bourge, Robert C., Colucci, Wilson, Massie, Barry, O'Connor, Christopher M., Pina, Ileana, Quigg, Rebecca, Silver, Marc, Robinson, Lee Ann, Leimberger, Jeffrey D., and Gheorghiade, Mihai

Subjects
Heart failure -- Drug therapy, Milrinone -- Health aspects, Clinical trials -- Analysis, Health
Published
2000

4. Effects of variable dose milrinone in patients with low cardiac output after cardiac surgery

Author

Feneck, Robert O.

Subjects
Heart, Milrinone -- Health aspects, Cardiac output -- Abnormalities, Health
Abstract

Milrinone is a noncatecholamine, nonglycoside drug that has both positive inotropic and vasodilator properties. That is, milrinone increases the force of cardiac contraction and decreases the constriction of blood vessels. It acts by blocking a key enzyme (cAMP-specific cardiac phosphodiesterase F III) responsible for reducing the effects of norepinephrine. (Norepinephrine constricts vascular smooth muscle.) Milrinone has been shown to be an effective drug in the treatment of severe heart failure, a disease characterized by ineffective cardiac contraction and insufficient cardiac output. It has not been evaluated in the treatment of individuals recovering from cardiac surgery, another group of patients who suffer from insufficient cardiac output. To determine whether milrinone is beneficial for such patients, its effects were evaluated in 99 otherwise healthy patients undergoing elective cardiac surgery (coronary artery bypass grafting, atrial and mitral valve replacement). Following surgery, patients were intravenously administered one of three doses of milrinone for a minimum of 12 hours. In all cases, drug administration was associated with a rapid, sustained improvement in cardiac output, and a decrease in vascular resistance (reflecting vascular relaxation). Increases in heart rate also occurred. Possible adverse side effects (nausea and cardiac arrhythmias) were noted in about half the patients, but these symptoms are common in patients recovering from heart surgery, and could not be unequivocally associated with drug treatment. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1991

5. Pharmacology of bipyridine phosphodiesterase III inhibitors

Author

Honerjager, Peter

Subjects
Heart failure -- Drug therapy, Milrinone -- Health aspects, Phosphodiesterases, Cardiotonic agents -- Physiological aspects, Health
Abstract

Heart failure is a condition in which the heart is unable to effectively pump blood to supply sufficient oxygen and nutrients to the tissues of the body. One pharmacological treatment for heart failure is the administration of positive inotropic drugs, which increase the contractile force (pumping action) of the heart. It has been proposed that the ideal positive inotropic drug would be one that not only increased the force of cardiac contraction, but also reduced the resistance offered by the blood vessels to the flow of blood and decreased the filling pressure exerted by venous blood returning to the heart. Two new drugs, amrinone and its analog milrinone, appear to have just these properties. Their mechanism of action is unique among cardiovascular drugs; they inhibit a particular subclass of an enzyme (phosphodiesterase III) involved in the breakdown of an intracellular biochemical signal (cyclic adenosine monophosphate). In addition to increased cardiac contractility, these drugs also shorten the duration of the relaxation phase of the heart cycle, and produce vasodilation (cause relaxation of the blood vessels). Unlike other less specific phosphodiesterase inhibitors, such as caffeine and theophylline, milrinone and amrinone do not have stimulatory effects on the central nervous system, which limit the usefulness of the former drugs. Additionally, these compounds do not suffer from the compromised effectiveness that results from the decreased number of receptors seen following administration of drugs such as beta blockers. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1991

6. Vasorelaxant effect of phosphodiesterase-inhibitor milrinone in the human radial artery used as coronary bypass graft

Author

He, Guo-Wei and Yang, Cheng-Qin

Subjects
Milrinone -- Health aspects, Coronary artery bypass -- Health aspects, Blood vessels -- Dilatation, Blood vessels -- Health aspects, Health
Abstract

Byline: Guo-Wei He, Cheng-Qin Yang Abstract: Objective: The radial artery is a spastic coronary bypass graft. We investigated the effect of the phosphodiesterase III inhibitor milrinone on the human radial artery. Methods: Radial artery segments (n = 76) taken from 15 patients were studied in an organ chamber. Concentration-relaxation curves for milrinone were established in the radial artery precontracted with 3 vasoconstrictors (phenylephrine, K.sup.+, and U46619). In radial artery rings incubated with therapeutic plasma concentrations of milrinone (7 and 70 [mu]mol/L) for 10 minutes, concentration-contraction curves for the 3 vasoconstrictors were constructed. Results: Milrinone caused a submaximal relaxation in phenylephrine- (98.6% [+ or -] 1.4%), K.sup.+- (89.1 [+ or -] 4.5%), or U46619- (74.2 [+ or -] 8.0%) precontracted radial arteries at -4.5 log.sub.10 M. The EC.sub.50 was higher against K.sup.+ (-5.85 [+ or -] 0.24 log.sub.10 M, P = .02) or U46619 (-5.21 [+ or -] 0.61 log.sub.10 M, P = .03) than phenylephrine (-6.68 [+ or -] 0.11 log.sub.10 M). Pretreatment with milrinone depressed the contraction by phenylephrine from 70.0% [+ or -] 7.9% to 23.5% [+ or -] 9.3% (P = .003) and by K.sup.+ from 138.6% [+ or -] 5.8% to 73.0% [+ or -] 13.9% (P = .006) and shifted the EC.sub.50 3.8-fold higher (P = .03) for phenylephrine and 2.2-fold higher for K.sup.+ (P = .01). Milrinone reduced the U46619 contraction at low concentration (-8.5 log.sub.10 M) but had little effect on the maximal contraction. Conclusion: Milrinone is a potent vasodilator for the radial artery, with possibly higher potency in [alpha]-adrenoceptor- and depolarizing agent K.sup.+-mediated, but less potency in thromboxane A.sub.2-mediated, contraction. Because it also has a positive inotropic effect, this vasodilator may be particularly indicated for use in patients receiving radial artery grafts in coronary artery bypass grafting. (J Thorac Cardiovasc Surg 2000;119:1039-45) Author Affiliation: Starr Academic Center for Cardiac Surgery, St Vincent Hospital, Portland, Ore, and the Division of Cardiothoracic Surgery and Cardiovascular Research Laboratory, Grantham Hospital, Department of Surgery, University of Hong Kong, Hong Kong Article History: Received 16 April 1999; Revised 3 June 1999; Revised 15 December 1999; Accepted 10 January 2000 Article Note: (footnote) [star] Supported by Hong Kong Research Grants Council (Grant HKU7280/97M & HKU7246/99M) and St Vincent Medical Foundation, Providence Health System, Portland, Ore., [star][star] Address for reprints: Professor Guo-Wei He, MD, PhD, Chair of Cardiothoracic Surgery, The University of Hong Kong, Grantham Hospital, 125 Wong Chuk Hang Road, Aberdeen, Hong Kong (E-mail: gwhe@hkucc.hku.hk ).

Published
2000

7. Combined use of glucagon and milrinone may not be preferable for severe propranolol poisoning in the canine model

Author

Sato, Shigehito, Tsuji, Mariko H., Okubo, Naomitsu, and Nishimoto, Chikako

Subjects
Glucagon -- Health aspects, Milrinone -- Health aspects, Propranolol hydrochloride -- Health aspects, Environmental issues, Health, Pharmaceuticals and cosmetics industries
Abstract

In a previous study of propranolol poisoning, glucagon and milrinone significantly increased cardiac output, but the improvement caused by glucagon was almost entirely due to the chronotropic effect. This study investigates the combined effect of glucagon, in a dose not inducing tachycardia, and milrinone on beta-blocker poisoning. Following the administration of 10 mg/kg propranolol IV over ten minutes, dogs (N = 20) were divided into four treatment groups, group S (saline), group G (glucagon 2.5 [micro]g/kg), group M (milrinone 100 [micro]g/kg), and group G + M (glucagon 2.5 [micro]g/kg plus milrinone 100 [micro]g/kg). Hemodynamic parameters were observed over the next thirty minutes. Heart rate, cardiac output, and mean arterial pressure were decreased in all groups after the administration of propranolol. Heart rate, mean arterial pressure, cardiac output, and stroke volume recovered to the baseline values in group G + M. However, heart rate in group G + M showed a significant increase versus the other three groups. In a canine model of severe propranolol poisoning, the combined effect of glucagon 2.5 [micro]g/kg and milrinone 100 [micro]g/kg brought about a significant hemodynamic improvement, but it was accompanied by an excessive increase of heart rate. Combined therapy of milrinone and glucagon may not be preferable therapy in beta-blocker poisoning in the canine model., (Key Words: glucagon; milrinone; propranolol poisoning, animal; adrenergic beta-antagonists.) INTRODUCTION As glucagon can increase cyclic adenosine monophosphate (cAMP) without involvement of the beta-adrenoceptor (1), it has been the most consistently [...]

Published
1995

8. Milrinone versus glucagon: comparative hemodynamic effects in canine propranolol poisoning

Author

Sato, Shigehito, Tsuji, Mariko H., Okubo, Naomitsu, and Naito, Hiroshi

Subjects
Adrenergic beta blockers -- Health aspects, Propranolol hydrochloride -- Health aspects, Milrinone -- Health aspects, Glucagon -- Health aspects, Poisoning, Accidental -- Drug therapy, Environmental issues, Health, Pharmaceuticals and cosmetics industries
Abstract

Glucagon has been reported to be one of the most effective treatments for severe beta-blocker poisoning. Recently, amrinone was suggested as an alternative therapeutic choice for beta-blocker poisoning. Milrinone, a derivative of amrinone, acts independently of beta-adrenoceptors and increases cyclic AMP. Therefore milrinone may also be effective in the treatment of beta-blocker poisoning. In the present study, we compared the effect of glucagon and milrinone in treating severe beta-blocker poisoning. Following the administration of 10 mg/kg propranolol IV over 10 min, heart rate, cardiac output, mean arterial pressure, stroke volume, and end tidal [CO.sub.2] were depressed, while central venous pressure, and pulmonary capillary wedge pressure increased significantly (p < 0.05). Following the administration of saline (Group S, N = 3), glucagon 20 [mu]g/kg (Group G, N = 5), and milrinone 300 [mu]g/kg (Group M, N = 5), hemodynamic parameters were observed for 30 min. In group M, mean arterial pressure, cardiac output and stroke volume recovered to their baseline values, while central venous pressure and pulmonary capillary wedge pressure decreased. Although there were no significant differences between groups G and M, the heart rate, central venous pressure and pulmonary capillary wedge pressure, mean arterial pressure and stroke volume did not return to baseline values in group G. Milrinone administration produced a significant hemodynamic improvement without increasing the heart rate in the canine model of severe heart failure caused by propranolol. In the glucagon treatment group, central venous pressure and pulmonary capillary wedge pressure improved less than the milrinone group. Although more data are needed before a clinical recommendation, milrinone might be an effective drug to treat beta-blocker poisoning., INTRODUCTION As a treatment for severe beta-blocker ([beta]-blocker) poisoning, glucagon is the most consistently effective treatment reported in the literature[1-4]. Glucagon can increase cAMP without involvement of the [beta]-adrenoceptor[5]. Amrinone [...]

Published
1994

9. Effect of milrinone on ventricular arrhythmias in congestive heart failure

Author

Ferrick, Kevin J., Fein, Steven A., Ferrick, Aileen M., and Doyle, Joseph T.

Subjects
Congestive heart failure -- Complications, Milrinone -- Health aspects, Milrinone -- Evaluation, Arrhythmia, Congestive heart failure -- Drug therapy, Congestive heart failure -- Patient outcomes, Health
Abstract

Congestive heart failure is the inability of the heart to pump effectively, and leads to fluid congestion or accumulation in the lungs. In patients with congestive heart failure, the cardiovascular drug milrinone increases heart muscle contraction and dilates blood vessels. Milrinone may increase the entry of calcium into cells, and calcium is essential for heart muscle contraction. Milrinone was shown to improve heart failure resulting from treatment with verapamil and propranolol, but may worsen ventricular arrhythmias or abnormal heart rhythms, which are common in patients with congestive heart failure. The effect of milrinone on ventricular arrhythmias was assessed in 24 patients with congestive heart failure. The results reveal that milrinone increased the frequency of ventricular arrhythmias; these findings are consistent with previous reports. A proarrhythmic effect of milrinone (ability of this drug to increase the frequency of arrhythmias) was observed in eight patients. Patients with proarrhythmia died 41 to 750 days after entry into the study, and sudden death occurred in four of these patients. Among 16 patients without proarrhythmia, 13 died within 166 days after entry into the study, including 6 cases of sudden death. The high death rate among these patients may be related to the severity of congestive heart failure and to impaired function of the left ventricle. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1990

10. Newer Drug Therapy for Congestive Heart Failure

Author

Coodley, Eugene

Subjects
Congestive heart failure -- Drug therapy, Milrinone -- Health aspects, Amrinone -- Health aspects, Xamoterol -- Health aspects, Health
Abstract

Background: The management of congestive heart failure has undergone a number of modifications over the past 5 to 10 years. Methods: These include assaying the role of inotropic drugs, evaluating the role of phosphodiesterase inhibitors, considering the role of intermittent inotropic infusion in ambulatory patients, and recognizing the importance of angiotensin-converting enzyme inhibitors. Very recently, the important role of angiotensin II receptor blocking agents and the use of beta blockade have provided additional modalities for the control of congestive heart failure. The relative usefulness of such therapy has been reviewed in this article. Conclusion: The management of congestive heart failure has undergone considerable change with the use of newer and more effective drugs. Arch Intern Med. 1999;159:1177-1183

Published
1999

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