AVE0118, Blocker of the Transient Outward Current ( I _to ) and Ultrarapid Delayed Rectifier Current ( I _Kur ), Fully Restores Atrial Contractility After Cardioversion of Atrial Fibrillation in the Goat

Q1 · MEDICINE

Article

Author: Blaauw, Yuri ; Allessie, Maurits ; de Haan, Sunniva ; Verheule, Sander ; van Hunnik, Arne ; Harks, Erik ; Schotten, Ulrich ; Greiser, Maura

Background— The loss of atrial contractile function after cardioversion of atrial fibrillation (AF) contributes to the thromboembolic risk associated with AF. The newly developed blocker of the transient outward current ( Ito ) and ultrarapid delayed rectifier current ( IKur ) AVE0118 prolongs atrial action potential duration and might therefore enhance atrial contractility. We compared the ability of AVE0118 to restore atrial contraction after cardioversion of AF with the efficacy of conventional positive inotropic compounds in the goat model of AF. Methods and Results— Eighteen goats were chronically instrumented with epicardial electrodes, a pressure transducer in the right atrium, and piezoelectric crystals to measure right atrial diameter. Atrial contractility and refractoriness and QT duration were measured before and after 1 week (3 to 8 days) of AF induced by repetitive burst pacing. The measurements were repeated after administration of digoxin (0.02 mg/kg), dobutamine (5 μg · kg −1 · min −1 ), the Ca 2+ sensitizer EMD57033 (1 mg · kg −1 · min −1 ), the L-type Ca 2+ channel agonist BayY5959 (0.1 mg · kg −1 · min −1 ), and AVE0118 (0.01 to 0.2 mg · kg −1 · min −1 ). The effect of AVE0118 on the configuration of atrial monophasic action potentials was determined for comparison. After 1 week of AF, atrial contractility during sinus rhythm or slow atrial pacing was reduced to <10%. Digoxin and dobutamine failed to increase atrial contractility. EMD57033 restored 41% and BayY5959 restored 48% of atrial contractility at baseline. BayY5959 significantly prolonged QT duration by 24.7%. AVE0118 enhanced atrial contraction to 156% of the baseline value. The positive inotropic effect was accompanied by a pronounced prolongation of atrial action potential duration and refractoriness, whereas QT duration remained unchanged. Conclusions— Conventional positive inotropic drugs showed limited effect on atrial contractility after cardioversion of AF or produced QT prolongation. In contrast, the Ito / IKur blocker AVE0118 fully restored atrial contraction without proarrhythmic effects on the ventricle.

01 Aug 2003·American journal of physiology. Heart and circulatory physiologyQ2 · MEDICINE

Gender differences on the effects of aging on cardiac and peripheral adrenergic stimulation in old conscious monkeys

Q2 · MEDICINE

Article

Author: Kudej, Raymond K. ; Rossi, Franco ; Natividad, Filipinas ; Shen, You-Tang ; Takagi, Gen ; Asai, Kuniya ; Peppas, Athanasios ; Vatner, Stephen F. ; Takagi, Ikuyo ; Resuello, Ranillo R. G. ; Vatner, Dorothy E.

We examined the effects of gender and aging on cardiac and peripheral hemodynamic responses to β-adrenergic receptor (β-AR) stimulation in young (male = 5.9 ± 0.4 yr old and female = 6.5 ± 0.7 yr old) and old (male = 19.8 ± 0.7 yr old and female = 21.2 ± 0.2 yr old) conscious monkeys ( Macaca fascicularis), chronically instrumented for measurements of left ventricular (LV) and arterial pressures as well as cardiac output. Baseline LV pressure, the first derivative of LV pressure (LV dP/d t), cardiac index, mean arterial pressure, total peripheral resistance (TPR), and heart rate in conscious monkeys were not different among the four groups. Increases in LV dP/d t in response to 0.1 μg/kg isoproterenol (Iso) were diminished ( P < 0.05) in old males (+99 ± 11%) compared with young males (+194 ± 18%). In addition, the inotropic responses to norepinephrine (NE) and forskolin (FSK) were significantly depressed ( P < 0.05) in old males. Iso-induced reductions of TPR were less ( P < 0.05) in old males (–28 ± 2%) than in young males (–49 ± 2%). The changes of TPR in response to NE and FSK were also significantly attenuated ( P < 0.05) in old males. However, the LV dP/d t responses to BAY y 5959 (15 μg · kg–1 · min–1), a Ca2+ channel promotor independent of β-AR signaling, were not significantly different between old and young males. In contrast to results in male monkeys, LV dP/d t and TPR responses to Iso, NE, and FSK in old females were similar to those observed in young females. Thus both cardiac contractile and peripheral vascular dynamic responses to β-AR stimulation are preserved in old female but not old male monkeys. This may explain, in part, the reduced cardiovascular risk in the older female population.

18 Mar 2003·CirculationQ1 · MEDICINE

Electrical and Contractile Remodeling During the First Days of Atrial Fibrillation Go Hand in Hand

Q1 · MEDICINE

Article

Author: Allessie, Maurits ; Schotten, Ulrich ; Ausma, Jannie ; Duytschaever, Mattias ; Neuberger, Hans-Ruprecht ; Eijsbouts, Sabine

Background— The mechanisms of the atrial contractile dysfunction induced by atrial fibrillation (AF) are not completely understood. In particular, the relation between the atrial dysfunction and electrical remodeling has not yet been studied. Methods and Results— Seven goats were chronically instrumented with electrodes sutured to the atria and with ultrasonic piezoelectric crystals to record the atrial diameters. A pressure transducer was implanted in the right atrium. After 5 minutes, 3 hours, and throughout the first 5 days of artificially maintained AF, atrial contractile function was measured and the atrial effective refractory period (AERP) was monitored for comparison. Also, the positive inotropic effects of the L-type Ca 2+ -channel agonist BayY5959 and short trains of rapid atrial pacing were studied. After resumption of sinus rhythm, the recovery of atrial contractile function was followed. After 5 minutes of AF, atrial contractility was decreased by ≈55% but recovered completely within 10 minutes. Five days of AF nearly completely abolished the atrial contractile function, and recovery took 2 days. During the first days of AF, the development of the contractile dysfunction followed the same time course as the shortening of AERP (electrical remodeling). In remodeled atria, BayY5959 increased atrial contractility to the same extent as it prolonged AERP. The inotropic effect of short trains of rapid atrial pacing was similar in normal and remodeled atria. Conclusions— Depending on the duration of AF, different mechanisms contribute to the AF-induced atrial hypocontractility. Atrial contractile remodeling during several days of AF goes hand in hand with electrical remodeling and might be caused by a reduction of the L-type Ca 2+ -current.

100 Deals associated with BAY-Y-5959

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Indication	Highest Phase	Country/Location	Organization	Date
Arrhythmias, Cardiac	Phase 2	DE	Bayer AG	-
Heart Failure	Phase 2	DE	Bayer AG	-
Myocardial Ischemia	Preclinical	DE	Bayer AG	-

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