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Literature DB >> 2612546

Pharmacokinetic characterization of the antiarrhythmic drug diprafenone in man.

D Trenk¹, F Wagner, W Sachs, E Jähnchen.

Abstract

The pharmacokinetics of the antiarrhythmic drug diprafenone have been investigated in 6 healthy volunteers following single intravenous (50 mg) and oral doses (50 and 150 mg). Diprafenone was mainly eliminated by metabolism in the liver. Following i.v. infusion of 50 mg diprafenone, the terminal half-life of elimination was 1.50 h, the volume of distribution at steady-state was 1.23 l.kg-1, and the free fraction in plasma was 1.68%. Mean total plasma clearance was 741 ml.min-1.70 kg-1, which approaches normal liver blood flow after correction for the blood/plasma concentration ratio. Thus, diprafenone can be classified as a high extraction drug. Following oral administration, a dose-dependent increase in bioavailability from 10.9 (50 mg dose) to 32.5% (150 mg dose) was observed. The data suggest that diprafenone is subject to saturable hepatic first-pass metabolism.

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Year: 1989 PMID： 2612546 DOI： 10.1007/bf00679792

Source DB: PubMed Journal: Eur J Clin Pharmacol ISSN： 0031-6970 Impact factor: 2.953

19 in total

1. Antiarrhythmic efficacy of propafenone: evaluation of effective plasma levels following single and multiple doses.

Authors: L Frabetti; B Marchesini; A Capucci; C Cavallini; S Gubelli; E Ambrosioni; B Magnani
Journal: Eur J Clin Pharmacol Date: 1986 Impact factor: 2.953

2. Tissue binding of drugs.

Authors: M Gibaldi; P J McNamara
Journal: J Pharm Sci Date: 1977-08 Impact factor: 3.534

3. Inter- and intra-subject variation in the first-pass elimination of highly cleared drugs during chronic dosing. Studies with deuterated verapamil.

Authors: M Eichelbaum; A Somogyi
Journal: Eur J Clin Pharmacol Date: 1984 Impact factor: 2.953

4. Prolongation of verapamil elimination kinetics during chronic oral administration.

Authors: J B Schwartz; D L Keefe; E Kirsten; R E Kates; D C Harrison
Journal: Am Heart J Date: 1982-08 Impact factor: 4.749

Review 5. Propafenone--a new antiarrhythmic drug.

Authors: L Seipel; G Breithardt
Journal: Eur Heart J Date: 1980-08 Impact factor: 29.983

6. The pharmacology of verapamil. IV. Kinetic and dynamic effects after single intravenous and oral doses.

Authors: R G McAllister; E B Kirsten
Journal: Clin Pharmacol Ther Date: 1982-04 Impact factor: 6.875

7. [Treatment of chronic ventricular arrhythmias with the new class Ic anti-arrhythmia agent diprafenon--results of long-term therapy].

Authors: H Heuer; H Gülker; M Hasfeld; B Frenking; T Behrenbeck
Journal: Z Kardiol Date: 1987-07

Pharmacokinetic characterization of the antiarrhythmic drug diprafenone in man.

1. Antiarrhythmic efficacy of propafenone: evaluation of effective plasma levels following single and multiple doses.

2. Tissue binding of drugs.

3. Inter- and intra-subject variation in the first-pass elimination of highly cleared drugs during chronic dosing. Studies with deuterated verapamil.

4. Prolongation of verapamil elimination kinetics during chronic oral administration.

Review 5. Propafenone--a new antiarrhythmic drug.

6. The pharmacology of verapamil. IV. Kinetic and dynamic effects after single intravenous and oral doses.

7. [Treatment of chronic ventricular arrhythmias with the new class Ic anti-arrhythmia agent diprafenon--results of long-term therapy].

8. Verapamil kinetics in normal subjects and patients with coronary artery spasm.

9. Interaction of phenylbutazone with racemic phenprocoumon and its enantiomers in rats.

10. An investigation of the cause of accumulation of verapamil during regular dosing in patients.

1. Electrophysiological effects of diprafenone, a dimethyl congener of propafenone on guinea-pig ventricular cells.

Review 2. Pharmacokinetics of newer drugs in patients with renal impairment (Part II).

Review 3. Individual variation in first-pass metabolism.