Studies on digitalis. 13. A comparison of the effects of potassium on the inotropic and arrhythmia-producing actions of ouabain.

Williams, Jr Jf; Klocke, F. J.; Braunwald, Eugene

doi:10.1172/jci105349

Cited by 57 publications

(12 citation statements)

References 34 publications

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“…The single dose of each drug used was obtained from the literature as a common or usual dose. 15,[17][18][19] An additional study might be to select doses escalating from no effect to one in which signs of toxicity are manifested.…”

Section: Discussionmentioning

confidence: 99%

Effects of 4 Classes of Cardiovascular Drugs on Ventricular Function in Dogs with Mitral Regurgitation

Nakayama

Nishijima

Miyamoto

et al. 2007

Veterinary Internal Medicne

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Background: There have been few trials in which dogs with mitral regurgitation (MR) have been treated with various cardioactive drugs to determine effects on left ventricular (LV) function.Hypothesis: Four classes of cardiovascular drugs may improve LV function in dogs with MR without increasing MR. Animals: Nine mature dogs were included in the study. Methods: MR was produced in 9 dogs. Five months later under butorphanol narcosis, parameters of LV function and left atrial dimension (LAD) were monitored by LV micromanometry and echocardiography/Doppler. Dogs were given (in random order) enalaprilat, nitroglycerine, ouabain, milrinone, and placebo.Results: Nitroglycerin produced no significant change; milrinone and ouabain increased contractility; ouabain decreased heart rate; and there was evidence that enalaprilat and milrinone decreased LAD. Milrinone and ouabain decreased isovolumetric contraction time and therefore the time available for MR. There was no evidence that a positive inotrope increased MR despite increasing LV contractility and stroke volume.Conclusion and Clinical Importance: This study contradicts the hypotheses that (1) strengthening the left ventricle may increase MR and (2) treatment of MR (even before symptoms of heart failure develop) may decrease LAD. It is reasonable that strengthening the force of LV contraction should increase the driving pressure for MR; however, this effect did not appear to increase MR. Although some investigators believe that treating dogs with MR with afterload reducers and decreasing hindrance to ejection of blood from the LV to aorta may lengthen life by decreasing MR, there did not appear to be a reduction in MR, at least in response to the angiotensin-converting enzyme (ACE) inhibitor.

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Section: Discussionmentioning

confidence: 99%

Effects of 4 Classes of Cardiovascular Drugs on Ventricular Function in Dogs with Mitral Regurgitation

Nakayama

Nishijima

Miyamoto

et al. 2007

Veterinary Internal Medicne

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“…The results of this study would suggest that the effect of DPH and K on the positive inotropic response of ouabain should be examined under conditions in which only positive inotropy and not arrhythmia is present. Apparent increases in ouabain inotropy due to DPH and K measured near the time of ouabain toxicity (see Scherlag et al, 1968;Williams et a!., 1966) may be misleading if the enhancement in inotropy seen in the presence of the antiarrhythmic agents is thought to occur at all time periods of drug interaction.…”

Section: Discussionmentioning

confidence: 99%

The effects of diphenylhydantoin and potassium on the biological activity of ouabain in the guinea‐pig heart

Baskin

Dutta

Marks

1973

British J Pharmacology

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Summary1. Diphenylhydantoin (DPH) and potassium significantly prevent ouabain intoxication without preventing the inotropic effects of ouabain in the guineapig isolated heart. 2. The antiarrhythmic effect of DPH and K on ouabain-induced toxicity appears to be related to their ability to reduce ouabain accumulation by the myocardium and thereby prevent the intracellular Na and K changes which lead to the arrhythmic state.

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“…A similar change in toxicity by variation of the extracellular potassium concentration has already been reported in the intact animal (Marcus et al, 1969 andHall et al, 1977;Steiness, 1978) On the contrary, reports on the influence of extracellular potassiumvariations on the ouabain-induced toxicity are rather divergent and support in part the (unexpected) missing effect of the altered serum-potassium concentration in the present study. Whereas some findings in the dog as well as in the rabbit indicate the well-known potassium-digitalis antagonism for ouabain (Baker, 1947;Williams et al, 1966; Lown and Wittenberg, 1968), contradictory results have been reported in the guinea pig by Greeff and Knippers (1964) and Schaumann and Chatoor (1966). Thus these differences of the potassium variation on the ouabain-induced toxicity may result from the different species used.…”

Section: Discussionmentioning

confidence: 96%

The influence of reduced serum potassium level on the toxicity of some cardenolides in guinea pigs

Fricke

Klaus

1981

Basic Res Cardiol

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Recent experiments on the pharmacological properties of the semisynthetic cardiotonic steroid strophanthidin-3-bromoacetate (SBA) have challenged the well-known potassium digitalis antagonism in isolated heart muscle preparations. In order to establish these results in vivo, the minimum lethal doses (LDmin) of ouabain (OUA), digoxin (DO), digotoxin (DT), k-strophanthidin (STR) and SBA were determined by the infusion toxicity method in guinea pigs at normokalemia and hypokalemia. The experimentally induced decrease of the serum potassium concentration (5.0 mmoles/l vs. 3.3 mmoles/l) significantly reduced the LDmin of DO (1.42 vs. 1.05 mumoles/kg), DT (1.78 vs. 1.24 mumoles/kg) and STR (20.16 vs. 15.98 mumoles/kg), whereas the LDmin of OUA (0.37 vs. 0.34 mumoles/kg) was not altered. Contrary, the LDmin of SBA was even slightly, but not significantly increased during hypokalemia (16.77 vs. 19.04 mumoles/kg). In addition, from the experimental data an optimum time of infusion (Topt), corresponding to the LDmin, can be derived, which is equivalent to the time for optimum "utilization" of the drug. The obtained sequence: STR less than OUA less than DO less than DT less than SBA represents the well-known differences in the onset of the pharmacological action in man resp. animal. Hypokalemia in general resulted in a shortening of the Topt, thus indicating a more rapid "utilization" of the drug tested. The above differences of the cardenolide action at reduced serum potassium concentration may be dependent on the recently reported divergent influence of potassium on the association- resp. dissociation rate constants for the interaction of these drugs with their binding site at the Na+-K+-ATPase.

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Studies on digitalis. 13. A comparison of the effects of potassium on the inotropic and arrhythmia-producing actions of ouabain.

Cited by 57 publications

References 34 publications

Effects of 4 Classes of Cardiovascular Drugs on Ventricular Function in Dogs with Mitral Regurgitation

Effects of 4 Classes of Cardiovascular Drugs on Ventricular Function in Dogs with Mitral Regurgitation

The effects of diphenylhydantoin and potassium on the biological activity of ouabain in the guinea‐pig heart

The influence of reduced serum potassium level on the toxicity of some cardenolides in guinea pigs

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