Your search keyword '"Gagnol JP"' showing total 7 results

1. Hemodynamic effects of a new inotropic compound, PST-2744, in dogs with chronic ischemic heart failure.

Author

Adamson PB, Vanoli E, Mattera GG, Germany R, Gagnol JP, Carminati P, and Schwartz PJ

Subjects

Animals, Cardiotonic Agents pharmacology, Dobutamine pharmacology, Dogs, Etiocholanolone pharmacology, Cardiotonic Agents therapeutic use, Dobutamine therapeutic use, Etiocholanolone analogs & derivatives, Etiocholanolone therapeutic use, Heart Failure drug therapy, Hemodynamics drug effects, Ventricular Dysfunction, Left drug therapy

Abstract

Inotropic agents for acute decompensated heart failure are associated with a lack of efficacy or increased mortality. New compounds are needed to support patients with acute exacerbations of heart failure. This study examined the hemodynamic effects of a new inotropic agent (PST-2744) in dogs with chronic ischemic heart failure. Eight mongrel dogs at low risk for postmyocardial infarction (MI) sudden death entered the protocol. Dogs were studied after ischemic left ventricular dysfunction was induced by repeated injections of latex microspheres into the circumflex artery until the ejection fraction reached 35%. Hemodynamic parameters were measured at baseline and peak drug effect (PST-2744 5 microg.kg-1.min-1). In 5 animals, PST-2744 effects were compared with dobutamine. Heart rates, PR intervals and QT intervals were unchanged following PST-2744 administration. PST-2744 increased contractility (+dP/dt) by 56% from 1881 +/- 282 mm Hg/s to 2939 +/- 734 mm Hg/s (P < 0.01). The inotropic effect of PST-2744 was equal to that produced by 5-microg.kg-1.min-1 dobutamine (56% increase in +dP/dt), but peak heart rates were significantly higher with dobutamine (129 +/- 24 bpm PST-2744 versus 160 +/- 6 bpm 5-microg.kg-1.min-1 dobutamine, P < 0.002). No arrhythmias or conduction delays were seen with either compound. PST-2744 is an effective inotropic agent without positive chronotropic effect in subjects with stable moderate left ventricular dysfunction.

Published

2003

2. Autonomic nervous system activity imbalance in cardiomyopathic hamster.

Author

Giudice PL, Gagnol JP, Bellucci A, Buffone G, Careddu A, Magni G, Quagliata T, Pacifici L, and Carminati P

Subjects

Animals, Cricetinae, Heart physiopathology, Heart Rate, Male, Mesocricetus, Propranolol pharmacology, Autonomic Nervous System physiopathology, Cardiomyopathies physiopathology, Heart Failure physiopathology

Abstract

There is strong evidence that autonomic imbalance plays an important role in progression of heart failure. Analysis of heart rate variability (HRV) has achieved substantial acceptance as a noninvasive method for the assessment of autonomic tone. The purpose of this investigation was to study HRV in an experimental model of heart failure using cardiomyopathic (BIO TO.2) hamsters. Animals showed an autonomic imbalance of cardiac control that seems due to attenuation of parasympathetic activity and an enhanced sympathetic tone. The reduction of parasympathetic activity in BIO TO.2 hamsters is suggested by (a) the reduction of the high-frequency (HF) spectrum, and (b) the lack of atropine to generate a response. The increased sympathetic activity is indicated by (a) the decreased time-domain indexes, (b) the increased LF/HF ratio of the power spectrum, and (c) the alteration of HRV indexes induced by propranolol. These results support the notion that in heart failure, there is a similar autonomic imbalance in both human and hamster and suggest that the cardiomyopathic hamster is a suitable experimental model for studying the involvement of the autonomic nervous system in the progression of heart failure.

Published

2000

3. Electrophysiologic and arrhythmogenic effects of the potassium channel agonist BRL 38227 in anesthetized dogs.

Author

de La Coussaye JE, Eledjam JJ, Bruelle P, Peray PA, Bassoul BP, Gagnol JP, and Sassine A

Subjects

Anesthesia, Animals, Antihypertensive Agents administration & dosage, Benzopyrans administration & dosage, Cromakalim, Dogs, Dose-Response Relationship, Drug, Electrophysiology, Female, Heart physiology, Hemodynamics drug effects, Injections, Intravenous, Male, Potassium Channels drug effects, Pyrroles administration & dosage, Vasodilator Agents administration & dosage, Antihypertensive Agents adverse effects, Arrhythmias, Cardiac chemically induced, Benzopyrans adverse effects, Heart drug effects, Pentobarbital, Pyrroles adverse effects, Vasodilator Agents adverse effects

Abstract

Although potassium channel openers have been demonstrated to induce arterial vasodilation and shortening of the QT interval, the complete in vivo hemodynamic and electrophysiologic profile of these drugs has not been fully established. We evaluated the effects of BRL 38227, the active enantiomer of cromakalim, on the electrophysiologic and hemodynamic parameters in anesthetized dogs. Four intravenous (i.v.) doses (0.01, 0.03, 0.1, and 0.3 mg/kg) of BRL 38227 (lemakalim) were given to four different groups of 6 anesthetized and mechanically ventilated dogs. Electrophysiologic and hemodynamic parameters were measured with bipolar catheters positioned in the right atria and the right ventricle and double micromanometers placed in the left ventricle and the aorta. Nine dogs died of ventricular fibrillation (VF; 6 of 6 after 0.3 mg/kg, 2 of 8 dogs after 0.1 mg/kg, and 1 of 7 dogs after 0.03 mg/kg BRL 38227). Three dogs had atrial tachycardia (1 had atrial flutter and 1 had atrial fibrillation after 0.03 mg/kg, and 1 had atrial fibrillation after 0.01 mg/kg BRL 38227). BRL 38227 did not modify heart rate (HR), corrected sinus recovery time (CSRT), and atrial or atrio-ventricular (A-V) conduction times. In contrast, PR interval, Luciani-Wenckebach cycle length (LW), HV interval, QRS duration, ventricular effective refractory period (VERP), QT interval, and monophasic action potential (AP) were significantly shortened in a dose-dependent manner. Left ventricular end-diastolic pressure (LVEDP) was not modified, whereas LVdP/dtmax decreased significantly at 0.1 mg/kg BRL 38227. Finally, there was a significant dose-dependent decrease in systolic, diastolic, and mean aortic blood pressure (SBP, DBP, MAP). We conclude that BRL 38227 shortens the ventricular parameters of conduction velocity and of repolarization and decreases BP, both in a dose-dependent manner. All doses were arrhythmogenic, suggesting that BRL 38227 has a low safety margin.

Published

1993

4. Hemodynamic response to SR 42128A in normal and sodium-depleted baboons.

Author

Serre M, Galindo G, Marion A, Lacour C, Cazaubon C, Gagnol JP, and Nisato D

Subjects

Animals, Female, Male, Papio, Renin blood, Hemodynamics drug effects, Oligopeptides pharmacology, Renin antagonists & inhibitors, Sodium physiology

Abstract

Hemodynamic changes following intravenous administration of SR 42128A (SR), a potent renin inhibitor, were evaluated in normal (N) and sodium-depleted (SD) anesthetized baboons. SR, at 9 mg/kg, decreased arterial pressure (AP) only in the SD group. This effect persisted for at least 2.30 h. At this dose, SR decreased the systemic vascular resistance (SVR) and increased the cardiac output in the SD group more than in the normal group. In both groups, heart rate was slightly increased. However, in the normal group, the highest dose (12 mg/kg) induced the same hemodynamic responses as the dose of 9 mg/kg in the SD group. Every time, plasma renin activity (PRA) was inhibited. Thus, in SD baboons, SR produced a hypotensive effect more pronounced than in the normal group. The dose-related effect on AP seemed to be correlated with the change in SVR. We can conclude that total inhibition of PRA is necessary but not sufficient, under normal conditions, to get an adequate lowering of SVR and a hypotensive effect.

Published

1987

5. Binding of a tritiated pepstatin analog to human renin.

Author

Cumin F, Nisato D, Gagnol JP, and Corvol P

Subjects

Humans, In Vitro Techniques, Protein Binding, Renin antagonists & inhibitors, Oligopeptides metabolism, Renin metabolism

Abstract

The interaction between human renin and a potent pepstatin analog, SR 42128, has been investigated using binding studies. Binding and enzymatic assays were performed at pH 5.7 and pH 7.4. We found one specific inhibitor binding site per molecule of renin at both pH's. The dissociation constant (KD) obtained at equilibrium was 14-fold lower at pH 5.7 than at pH 7.4, showing a pH effect on binding of [3H]SR 42128. A similar decrease was measured in enzymatic studies. In nonequilibrium conditions, we demonstrated that only association kinetic constants have been affected by pH variations. Radioligands provided interesting tools to investigate enzyme-inhibitor relationships.

Published

1987

6. In vitro and in vivo inhibition of human and primate renin by a new potent renin inhibitor: SR 42128.

Author

De Claviere M, Cazaubon C, Lacour C, Nisato D, Gagnol JP, Evin G, and Corvol P

Subjects

Animals, Blood Pressure drug effects, Callitrichinae, Dogs, Female, Heart Rate drug effects, Humans, Macaca fascicularis, Male, Papio, Pepstatins pharmacology, Rats, Renin blood, Sodium physiology, Oligopeptides pharmacology, Renin antagonists & inhibitors

Abstract

A new potent renin inhibitor, Iva-Phe-Nle-Sta-Ala-Sta-OH (SR 42128), and its arginine salt (SR 42128A) have been synthesized. This compound had a concentration required to displace 50% of ligand binding of 2.8 X 10(-8) M toward human plasma renin at pH 7.4 and was 2,000 times more potent than pepstatin. All primate renins tested were inhibited within the same order of magnitude whereas other animal renins were much less inhibited. The effect in vivo of SR 42128A was studied in sodium-depleted conscious monkeys. A single dose of SR 42128A produced a dose-dependent blood pressure decrease as well as a dose-dependent inhibition of plasma renin activity (PRA). Blood pressure was still significantly lowered 3 h after a single administration of 3 or 10 mg/kg whereas PRA was still completely inhibited. SR 42128 is a potent and long-acting tool for studying the role of the renin angiotensin system in primates and humans.

Published

1985

7. Electrophysiological studies of penticainide (CM 7857), a new antiarrhythmic agent, in mammalian myocardium.

Author

Gautier P, Guiraudou P, Pezziardi F, Bertrand JP, and Gagnol JP

Subjects

Action Potentials drug effects, Animals, Dogs, Electrophysiology, Female, Guinea Pigs, Heart physiology, Heart Conduction System physiology, In Vitro Techniques, Male, Purkinje Fibers physiology, Rabbits, Refractory Period, Electrophysiological, Anti-Arrhythmia Agents pharmacology, Heart drug effects, Propylamines pharmacology, Pyridines

Abstract

The intracellular electrophysiologic properties of a new antiarrhythmic substance, penticainide, were studied in isolated rabbit, dog, and guinea pig myocardial preparations superfused or perfused with oxygenated Tyrode's solution. "Therapeutic" concentrations of penticainide (1.5 to 3 X 10(-5) M) had little effect on sinus node automaticity; sinoatrial conduction was slightly delayed. In atrial, Purkinje and ventricular fibers, amplitude, and maximal rate of rise of phase O (dV/dtmax) were decreased by penticainide; Purkinje-ventricle conduction velocity was depressed. Penticainide did not significantly modify action potential duration (APD) of rabbit atria and dog ventricle and reduced APD and effective refractory period (ERP) of dog Purkinje and guinea pig ventricular fibers. Penticainide reduced APD heterogeneity of Purkinje-ventricle junction with a preferential effect at the gate and decreased tension amplitude of perfused papillary muscle in dog heart. The effect of penticainide on dV/dtmax was voltage and rate dependent; the resting block was weak. Thus, penticainide is a class 1 antiarrhythmic agent with properties of class 1B agents such as APD reduction and properties of class 1C agents such as slow recovery kinetic of rate-dependent block.

Published

1987