Your search keyword '"Hariman RJ"' showing total 6 results

1. Impact of food on the pharmacokinetics and electrocardiographic effects of sustained release verapamil in normal subjects.

Author

Hoon TJ, McCollam PL, Beckman KJ, Hariman RJ, and Bauman JL

Subjects

Administration, Oral, Adult, Delayed-Action Preparations, Fasting physiology, Humans, Male, Electrocardiography, Ambulatory, Food, Heart drug effects, Verapamil pharmacokinetics, Verapamil pharmacology

Abstract

To evaluate the impact of food on the pharmacokinetics and electrocardiographic effects of sustained release (SR) verapamil tablets, 9 healthy men each received 3 single doses of verapamil in a randomized, crossover manner: 10 mg of intravenous verapamil, 240 mg SR verapamil on an empty stomach, and 240 mg SR verapamil with a standardized meal. PR intervals and racemic verapamil serum concentrations were measured serially over 30 hours after administration. The time to peak concentration was longer (7.5 +/- 3.0 vs 4.4 +/- 2.3 hours), resulting in a lower peak verapamil serum concentration (118 +/- 43 vs 175 +/- 50 ng/ml) when SR verapamil was administered with food (p < 0.05). Food tended to decrease the bioavailability of SR verapamil (34 +/- 12 vs 49 +/- 14%), although this difference did not reach statistical significance (p = 0.065). Precipitous or exaggerated release of verapamil from the SR tablet was not observed in any subject during the fasting state. Prolongation of the PR interval paralleled these alterations in serum concentration. The maximal change in the PR interval was greater (21 +/- 8 vs 14 +/- 5%; p < 0.05) when SR verapamil was given in the fasting state. Although an exaggerated verapamil release or effect was not observed, food significantly altered the absorption and electrocardiographic effects of a single dose of SR verapamil. Manipulation of the administration condition may be helpful in achieving desired outcomes.

Published

1992

2. Comparison of the pharmacokinetics and electrocardiographic effects of sublingual and intravenous verapamil.

Author

Berk SI, Beckman K, Hoon TJ, Hariman RJ, Hu D, Siegel FP, and Bauman JL

Subjects

Administration, Oral, Administration, Sublingual, Adult, Animals, Dogs, Dose-Response Relationship, Drug, Humans, Injections, Intravenous, Isomerism, Male, Powders, Tablets, Verapamil pharmacology, Electrocardiography drug effects, Verapamil administration & dosage, Verapamil pharmacokinetics

Abstract

Using a dog model, a sublingual form of the free base of verapamil (SLV) was developed with the intent of avoiding stereoselective first-pass metabolism and the necessity of intravenous administration. Intravenous verapamil (IVV) 5 mg and SLV 40 mg or 60 mg were sequentially administered to seven healthy human volunteers. Electrocardiograms and serum concentrations were obtained before and periodically from 5 to 480 minutes after each dose. The time to peak serum concentration (mean +/- SD) was 77.6 +/- 38.1 minutes after SLV. Bioavailability of SLV was 58.2 +/- 36.9% compared to IVV. Verapamil half-lives after IVV and SLV were 2.83 +/- 0.93 and 2.28 +/- 0.45 hours (NS), respectively. In one subject, the time to peak effect was delayed and overall change in PR interval was minimum. In the remaining six subjects, the maximum percentage increases in PR interval after IVV and SLV were 20.6 +/- 6.4% and 14.8 +/- 5.5% (p less than 0.05), respectively. Times to peak increase in PR interval were 28.3 +/- 15.7 and 57.0 +/- 17.5 minutes after IVV and SLV (p less than 0.05), respectively. Analysis of plots of percentage change in PR interval versus serum concentration revealed a shift to the right and therefore, lesser effect of SLV than of IVV in six subjects. All seven subjects complained of oral numbness and bitter taste. In conclusion, SLV is inferior to IVV in terms of rate and extent of absorption and pharmacologic effect in delaying atrioventricular nodal conduction. Probably SLV has little clinical utility because of its slow onset and poor tolerance.

Published

1992

3. Evaluation of the pharmacokinetics and electrocardiographic effects of intravenous verapamil with intravenous calcium chloride pretreatment in normal subjects.

Author

Schoen MD, Parker RB, Hoon TJ, Hariman RJ, Bauman JL, and Beckman KJ

Subjects

Adolescent, Adult, Analysis of Variance, Calcium Chloride administration & dosage, Double-Blind Method, Humans, Hypotension chemically induced, Infusions, Intravenous, Male, Random Allocation, Reference Values, Verapamil administration & dosage, Verapamil blood, Verapamil pharmacokinetics, Blood Pressure drug effects, Calcium Chloride therapeutic use, Electrocardiography drug effects, Heart Rate drug effects, Hypotension prevention & control, Verapamil pharmacology

Abstract

To evaluate the effects of calcium pretreatment on the disposition and electrocardiographic effects of verapamil, 8 healthy male volunteers received treatment in each of 3 phases in a randomized, double-blind, crossover manner. Phase I denoted 10 ml of 0.9% intravenous sodium chloride followed by 10 mg of intravenous verapamil; phase II denoted 10 ml of 10% intravenous calcium chloride followed by 4 ml of 0.9% intravenous sodium chloride; and phase III denoted 10 ml of 10% intravenous calcium chloride followed by 10 mg of intravenous verapamil. Blood samples for the determination of verapamil concentrations were drawn at 5, 10, 15, 20, 30, 45, 60 and 90 minutes, and at 2, 4, 6, 10 and 24 hours. Blood pressure, heart rate and PR intervals were also measured at these times. Pretreatment of verapamil with intravenous calcium did not alter the disposition of intravenous verapamil. Blood pressure was not significantly altered in any treatment phase, although calcium tended to increase mean arterial pressure and verapamil abolished this effect. Calcium had no significant affect on verapamil-induced PR prolongation (maximum percent change in PR interval: phase I = 19 +/- 11%, phase III = 18 +/- 7%; time to maximal prolongation: phase I = 0.38 +/- 0.21 hours, phase III = 0.37 +/- 0.26 hours; and area under the percent change in PR vs time curve: phase I = 15.5 +/- 10, phase III = 21 +/- 9). Verapamil caused a reflex increase in heart rate of similar magnitude in both phases I and III (24 +/- 10% and 21 +/- 7%, respectively).(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1991

4. Reversal of the cardiovascular effects of verapamil by calcium and sodium: differences between electrophysiologic and hemodynamic responses.

Author

Hariman RJ, Mangiardi LM, McAllister RG Jr, Surawicz B, Shabetai R, and Kishida H

Subjects

Animals, Atrioventricular Node drug effects, Blood Pressure drug effects, Calcium blood, Cardiac Output drug effects, Dogs, Electrophysiology, Sodium blood, Vascular Resistance drug effects, Verapamil blood, Calcium pharmacology, Hemodynamics drug effects, Sodium pharmacology, Verapamil pharmacology

Published

1979

5. Electrophysiologic and hemodynamic effects of verapamin. Correlation with plasma drug concentrations.

Author

Mangiardi LM, Hariman RJ, McAllister RG Jr, Bhargava V, Surawicz B, and Shabetai R

Subjects

Animals, Atrioventricular Node drug effects, Blood Flow Velocity, Blood Pressure drug effects, Cardiac Output drug effects, Dogs, Dose-Response Relationship, Drug, Electrophysiology, Heart Atria drug effects, Heart Rate drug effects, Heart Ventricles drug effects, Sinoatrial Node drug effects, Time Factors, Vascular Resistance drug effects, Verapamil blood, Hemodynamics drug effects, Verapamil pharmacology

Abstract

Verapamil was administered intravenously to 30 open-chest dogs and the electrophysiologic and hemodynamic effects of the drug were correlated with the corresponding plasma concentrations. At concentrations below 152 ng/ml, verapamil prolonged the A-H interval, abolished ventriculoatrial conduction, but did not significantly change sinus rate, cardiac output, left ventricular dp/dt, of systemic vascular resistance. Concentrations above 200 ng/ml were associated with slowing of the sinus rat, high degree atrioventricular block during atrial pacing, 24% decrease in mean aortic pressure, and decreased cardiac output and left ventricular dp/dt. Sinus arrest, high degree atrioventicular block during sinus rhythm, decreased systemic vascular resistance and increased left ventricular end-diastolic pressure occurred when plasma verapamil concentrations exceeded 400 ng/ml. These results show that plasma verapamil concentrations reliably reflect the electrophysiologic and hemodynamic actions of the drug, and that "therapeutic" drug effects can be achieved at plasma concentrations at which myocardial depressant effects are unlikely.

Published

1978

6. The pharmacodynamic and pharmacokinetic differences of the D- and L-isomers of verapamil: implications in the treatment of paroxysmal supraventricular tachycardia.

Author

Hoon TJ, Bauman JL, Rodvold KA, Gallestegui J, and Hariman RJ

Subjects

Administration, Oral, Animals, Biological Availability, Humans, Injections, Intravenous, Kinetics, Stereoisomerism, Structure-Activity Relationship, Verapamil metabolism, Verapamil therapeutic use, Tachycardia, Paroxysmal drug therapy, Verapamil pharmacology

Abstract

There is increasing interest in defining the pharmacodynamic and pharmacokinetic characteristics of drugs that are marketed as racemic mixtures. Verapamil is one such drug that is commercially available as a mixture of D- and L-isomers. The L-isomer of verapamil has a greater-negative inotropic, negative chronotropic, and negative dromotropic potency than the D-isomer. The values for fraction unbound in serum, distribution volume, and systemic clearance are substantially greater for the L-isomer after intravenous dosing. After oral dosing, the D-isomer achieves peak plasma concentrations five times greater than the L-isomer. The pharmacodynamic and pharmacokinetic characteristics of each isomer are reviewed. The differences in the concentrations of the D- and L-isomers after oral vs intravenous dosing may contribute to the relatively lower efficacy of orally administered verapamil in the treatment of PSVT.

Published

1986