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Effects of AZD0837, a Novel Direct Thrombin Inhibitor, on the Electrophysiological Properties of the Human Heart A Randomized, Double-Blind, Parallel-Group, Placebo-Controlled Study

Walfridsson, Hakan; Johansson, Birgitta; Englund, Anders; Kenneback, Goran; Schwieler, Jonas; Kongstad Rasmussen, Ole LU ; Wahlander, Karin; Malm, Anders R. and Edvardsson, Nils (2010) In Clinical Drug Investigation 30(7). p.461-471
Abstract
Background: AZD0837 is an investigational oral anticoagulant that is bio-converted to its active form, AR-H067637, a selective direct thrombin inhibitor. Objectives: The objectives of the present study were to investigate if there are any clinically relevant adverse effects of intravenous AZD0837 on cardiac conduction, refractoriness and repolarization, and to study its safety and tolerability. Methods: In this randomized, double-blind, parallel-group, placebo-controlled study (study code D1250C00026), invasive electrophysiological measurements were performed twice in 30 subjects with a history of, or ongoing, atrial flutter, starting 30 minutes after successful ablation of atrial flutter and then 60 minutes after start of an intravenous... (More)
Background: AZD0837 is an investigational oral anticoagulant that is bio-converted to its active form, AR-H067637, a selective direct thrombin inhibitor. Objectives: The objectives of the present study were to investigate if there are any clinically relevant adverse effects of intravenous AZD0837 on cardiac conduction, refractoriness and repolarization, and to study its safety and tolerability. Methods: In this randomized, double-blind, parallel-group, placebo-controlled study (study code D1250C00026), invasive electrophysiological measurements were performed twice in 30 subjects with a history of, or ongoing, atrial flutter, starting 30 minutes after successful ablation of atrial flutter and then 60 minutes after start of an intravenous infusion of AZD0837. Pre-study warfarin therapy was not an exclusion criterion. The stimulation protocol was performed mainly at 500 and 400 ms drive cycle length. A 12-lead ECG was also recorded before and during AZD0837 infusion. Plasma concentrations of AZD0837 and its metabolites were obtained at predefined timepoints. Results: Measurements were made at baseline and during stable plasma concentrations of the prodrug AZD0837 (mean +/- standard deviation 7.96 +/- 2.38 mu mol/L, approximate target of 10 mu mol/L), the intermediate metabolite AR-H69927 (1.26 +/- 0.39 mu mol/L, target 1-2 mu mol/L) and the active direct thrombin inhibitor AR-H067637 (0.35 +/- 0.14 mu mol/L, target 0.5-1.0 mu mol/L). There were no clinically relevant effects on cardiac conduction (QRS duration, PR interval, His bundle electrogram, Wenckebach point), refractoriness (atrial, atrioventricular and ventricular effective refractory periods) or re-polarization (QT, QT interval corrected for heart rate using Fridericia's formula, QRS onset to the top of the T wave [QT(top)], QRS onset to the end of the T wave [QT(end)] or QT(top)-QT(end)). Conclusions: AZD0837 was well tolerated, and had no clinically relevant effects on cardiac electrophysiology of the target population, either in subjects previously treated with warfarin or in those without previous treatment. (Less)
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author
organization
publishing date
type
Contribution to journal
publication status
published
subject
in
Clinical Drug Investigation
volume
30
issue
7
pages
461 - 471
publisher
Adis International
external identifiers
  • wos:000279296600004
  • scopus:77953337485
ISSN
1179-1918
DOI
10.2165/11536300-000000000-00000
language
English
LU publication?
yes
id
dac02d50-3be4-4ddf-ba29-961e60a383b6 (old id 1629285)
date added to LUP
2010-07-23 11:45:05
date last changed
2018-05-29 11:43:12
@article{dac02d50-3be4-4ddf-ba29-961e60a383b6,
  abstract     = {Background: AZD0837 is an investigational oral anticoagulant that is bio-converted to its active form, AR-H067637, a selective direct thrombin inhibitor. Objectives: The objectives of the present study were to investigate if there are any clinically relevant adverse effects of intravenous AZD0837 on cardiac conduction, refractoriness and repolarization, and to study its safety and tolerability. Methods: In this randomized, double-blind, parallel-group, placebo-controlled study (study code D1250C00026), invasive electrophysiological measurements were performed twice in 30 subjects with a history of, or ongoing, atrial flutter, starting 30 minutes after successful ablation of atrial flutter and then 60 minutes after start of an intravenous infusion of AZD0837. Pre-study warfarin therapy was not an exclusion criterion. The stimulation protocol was performed mainly at 500 and 400 ms drive cycle length. A 12-lead ECG was also recorded before and during AZD0837 infusion. Plasma concentrations of AZD0837 and its metabolites were obtained at predefined timepoints. Results: Measurements were made at baseline and during stable plasma concentrations of the prodrug AZD0837 (mean +/- standard deviation 7.96 +/- 2.38 mu mol/L, approximate target of 10 mu mol/L), the intermediate metabolite AR-H69927 (1.26 +/- 0.39 mu mol/L, target 1-2 mu mol/L) and the active direct thrombin inhibitor AR-H067637 (0.35 +/- 0.14 mu mol/L, target 0.5-1.0 mu mol/L). There were no clinically relevant effects on cardiac conduction (QRS duration, PR interval, His bundle electrogram, Wenckebach point), refractoriness (atrial, atrioventricular and ventricular effective refractory periods) or re-polarization (QT, QT interval corrected for heart rate using Fridericia's formula, QRS onset to the top of the T wave [QT(top)], QRS onset to the end of the T wave [QT(end)] or QT(top)-QT(end)). Conclusions: AZD0837 was well tolerated, and had no clinically relevant effects on cardiac electrophysiology of the target population, either in subjects previously treated with warfarin or in those without previous treatment.},
  author       = {Walfridsson, Hakan and Johansson, Birgitta and Englund, Anders and Kenneback, Goran and Schwieler, Jonas and Kongstad Rasmussen, Ole and Wahlander, Karin and Malm, Anders R. and Edvardsson, Nils},
  issn         = {1179-1918},
  language     = {eng},
  number       = {7},
  pages        = {461--471},
  publisher    = {Adis International},
  series       = {Clinical Drug Investigation},
  title        = {Effects of AZD0837, a Novel Direct Thrombin Inhibitor, on the Electrophysiological Properties of the Human Heart A Randomized, Double-Blind, Parallel-Group, Placebo-Controlled Study},
  url          = {http://dx.doi.org/10.2165/11536300-000000000-00000},
  volume       = {30},
  year         = {2010},
}