Systemic and regional myocardial responses to AR-L 115 BS, a positive inotropic imidazo-pyridine, in the absence or in the presence of the bradycardiac action of alinidine

Verdouw, Pieter D.; Hartog, J. M.; Rutteman, A. M.

doi:10.1007/bf01907776

Cited by 17 publications

(8 citation statements)

References 25 publications

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“…Yet AR-L directly activates the myofibrils in a concentration range close to the plasma concentrations of AR-L 115BS associated with positive inotropic effects in intact pigs (Verdouw et al, 1981). Effects of AR-L on cardiac cell membranes have not been studied extensively, but there are data showing that AR-L 115BS enhances the process of Ca ++ -induced Ca ++ release in mechanically skinned heart muscle cells.…”

Section: Discussionmentioning

confidence: 98%

“…In the intact animal, AR-L has a number of effects depending on the dose. Contractility, heart rate, and preload are increased and afterload is decreased (Diederen and Kadatz, 1981;Verdouw et al, 1981). Thus, whereas direct effects of AR-L on the heart appear to be a likely mode of action of the drug, in the intact animal effects of AR-L on cardiac output most likely are the result of a variety of pharmacological actions.…”

Section: Discussionmentioning

confidence: 99%

“…(Circ Res 51: 290-294, 1982) AR-L 115BS IS a benzimidazole derivative ( Fig. 1) which, when infused into intact animals, increases contractility and reduces afterload (Diederen and Kodatz, 1981;Verdouw et al, 1981). These effects make this compound interesting as a potentially useful agent in the treatment of heart failure, since it apparently combines two modes of alleviation of the disease.…”

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confidence: 99%

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Stimulation of Ca++ binding and ATPase activity of dog cardiac myofibrils by AR-L 115BS, a novel cardiotonic agent.

Solaro

Rüegg²

1982

Circulation Research

144

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AR-L 115BS, a benzimidazole derivative, is a positive inotropic agent that has been shown to increase active tension development and unloaded shortening velocity of chemically skinned heart muscle preparations at submaximal activating levels of free Ca++. We measured the effect of AR-L on relations between free Ca++, bound Ca++ and ATPase activity of dog cardiac myofibrils. At pCa 6, 100-300 micrometers AR-L increased myofibrillar ATPase activity maximally by about 30%. The concentration of AR-L giving half-maximal activation of myofibrillar ATPase activity was about 10 micrometers, and is similar to plasma concentrations associated with elevated contractility in intact animals. There was no effect of AR-L on myofibrillar ATPase activity at pCa 5 or 8, and the relation between pCa and percent activation of myofibrillar ATPase activity was shifted to the left by 0.4-0.5 pCa units in the presence of 100 micrometers AR-L. Calcium binding by cardiac myofibrils was increased by AR-L in the presence and absence of MgATP by 0.2-0.3 nmol/mg myofibrillar protein over a broad range of free Ca++ concentrations, a result suggesting that AR-L increases the affinity of myofibrillar troponin C for Ca++. The shift in the pCa giving half maximal and myofibrillar ATPase activity induced by raising the free Mg++ from 1.0 to 10 mm was unaffected by AR-L. These results indicate that the positive actions of AR-L 115BS on cardiac contractility may involve direct activation of myofibrils by virtue of an increased affinity of thin filament receptors for Ca++.

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Section: Discussionmentioning

confidence: 98%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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Stimulation of Ca++ binding and ATPase activity of dog cardiac myofibrils by AR-L 115BS, a novel cardiotonic agent.

Solaro

Rüegg²

1982

Circulation Research

144

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“…The analysis of the echocardiograms was carried out as described elsewhere (5,6). and 150 mg metomidate i.v.…”

Section: Methodsmentioning

confidence: 99%

“…It has been suggested that the concomitant decrease in myocardial O2-extraction was caused by an increase in 02-supply due to a coronary vasodilatation and a decrease in O2-demand as a consequence of a reduction in afterload and a negative inotropic action (1)(2)(3)(4). Regional myocardial function was described with the aid of myocardial wall thickness tracings obtained from the same myocardial segment (5,6). O2-consumption of the LAD-perfused area was calculated from the LAD-flow and the difference between the O2-content in the LAD and the great cardiac vein.…”

Section: Introductionmentioning

confidence: 99%

Intracoronary infusion of small doses of nifedipine lowers regional myocardial O2-consumption without altering regional myocardial function

et al. 1982

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Intracoronary infusion of low doses (0.1-0.3 microgram X kg-1) of nifedipine caused dose-dependent decreases in regional myocardial O2-consumption, without significant changes in any of its major global hemodynamic determinants: heart rate, left ventricular systolic and end-diastolic pressure and maxLVdP/dt. Furthermore, regional myocardial function was unaltered. It is suggested that nifedipine decreased myocardial O2-consumption by a direct effect on myocardial metabolism. Some of the possible mechanisms involved are discussed.

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On the cardiovascular and antiarrhythmic actions of the cardioselective beta‐adrenoceptor antagonist bevantolol in the pig

Hartog

Bremen

Verdouw

1986

Drug Development Research

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The cardioselective beta-adrenoceptor antagonist bevantolol (1-[(3,4-dimethoxyphenethyl)amino]-3-(m-tolyloxy)-2-propanol monohydrochloride) was studied for its effects on cardiac performance and on coronary artery occlusion-induced ventricular fibrillation in anesthetized open-chest pigs. In doses of 0.5-3.0 mg. kg-' the drug caused dose-dependent decreases in cardiac output (10-35%) that were primarily due to a negative chronotropic action, as heart rate decreased considerably more (10-25%) than stroke volume (0-15%). The decrease in stroke volume appeared to be due to a decrease in maxLVdPldt (up to 40%) and a mild vasoconstriction (<20%) of the systemic arterial vascular bed.Myocardial blood flow (2545%) and O2 extraction both decreased, but cerebral blood flow was well preserved. Decreases in perfusion of some organs (kidneys, liver, and stomach) were similar to those in cardiac output, but that of the small intestine was not significantly affected. After ligation of the left anterior descending coronary artery at its midpoint, bevantolol prevented ventricular fibrillation during the earliest phase of ectopic activity, but was ineffective during the second phase of the early arrhythmias.

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Systemic and regional myocardial responses to AR-L 115 BS, a positive inotropic imidazo-pyridine, in the absence or in the presence of the bradycardiac action of alinidine

Cited by 17 publications

References 25 publications

Stimulation of Ca++ binding and ATPase activity of dog cardiac myofibrils by AR-L 115BS, a novel cardiotonic agent.

Stimulation of Ca++ binding and ATPase activity of dog cardiac myofibrils by AR-L 115BS, a novel cardiotonic agent.

Intracoronary infusion of small doses of nifedipine lowers regional myocardial O2-consumption without altering regional myocardial function

On the cardiovascular and antiarrhythmic actions of the cardioselective beta‐adrenoceptor antagonist bevantolol in the pig

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