Concentration dependent cardiotoxicity of terodiline in patients treated for urinary incontinence.

Thomas, Simon; Higham, P D; Hartigan-Go, Kenneth; Kamali, Farzad; Wood, Philip Matchett; Campbell, R. W. F.; Ford, Gary A.

doi:10.1136/hrt.74.1.53

Cited by 43 publications

(31 citation statements)

References 27 publications

(5 reference statements)

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…6,13,14 The developability of the terodiline racemate would be viewed differently if only an enantioselective investigation into its toxicity pro®le had been undertaken earlier because, recently, it was shown that although both enantiomers of terodoline are equipotent in their therapeutic bene®ts, the cardiac polarization (prolongation of QTc interval and QRS duration) and proarrhythmic properties were due to the R()-enantiomer. 15 Had this information been available earlier during the clinical development of terodiline, the development of the S(-)-enantiomer instead of the racemate would have been favored.…”

Section: Terodilinementioning

confidence: 98%

Enantiomeric drug development: Issues, considerations, and regulatory requirements

Srinivas

Barbhaiya

Midha

2001

Journal of Pharmaceutical Sciences

View full text Add to dashboard Cite

Section: Terodilinementioning

confidence: 98%

Enantiomeric drug development: Issues, considerations, and regulatory requirements

Srinivas

Barbhaiya

Midha

2001

Journal of Pharmaceutical Sciences

View full text Add to dashboard Cite

“…The calcium antagonist terodiline has been associated with cardiovascular events, including cardiac arrhythmias with prolonged Q–T intervals [7, 8, 9, 10]. Therefore, in view of the calcium–antagonistic properties of propiverine, the thorough investigation of possible arrhythmogenic effects of propiverine was initiated under a therapeutic dosage regime.…”

Section: Discussionmentioning

confidence: 99%

“…These cardiac arrhythmias were probably caused by the concentration–related prolongation of the frequency–corrected Q–T (Q–Tc) interval [10]. However, this phenomenon has not been reported for anticholinergic drugs, such as oxybutynin [11].…”

Section: Introductionmentioning

confidence: 99%

Efficacy and Cardiac Safety of Propiverine in Elderly Patients – A Double–Blind, Placebo–Controlled Clinical Study

et al. 2000

View full text Add to dashboard Cite

“…Terodiline. Terodiline concentrations ranging from 32.9 nM up to the clinically relevant level (Thomas et al, 1995) of 120 nM caused statistically significant increases in the mean QT RR1000 of 9 to 12 ms. As in the case of cisapride, the dose-response curve was bell-shaped, with the greatest mean QT prolongation occurring at the third free drug concentration level achieved of 32.9 nM.…”

Section: Qt Prolongation Assessment In the Conscious Dog 829mentioning

confidence: 99%

The Relationship of Clinical QT Prolongation to Outcome in the Conscious Dog Using a Beat-to-Beat QT-RR Interval Assessment

Fossa

DePasquale²,

Raunig³

et al. 2002

J Pharmacol Exp Ther

View full text Add to dashboard Cite

QT interval prolongation of the electrocardiogram has been associated with the occurrence of life-threatening fatal ventricular arrhythmias. To understand the relationship between preclinical cardiac conduction assessment to clinical outcome, comparisons of free (unbound)-plasma drug concentrations and their associated effects in the conscious mongrel dog were made to the free plasma concentrations in humans reported to produce QT prolongation. E-4031 (an experimental class III antiarrhythmic), cisapride, terfenadine, terodiline, and verapamil all affect cardiac repolarization and can produce QT prolongation in humans. In the conscious dog, the QT interval was assessed on a beat-to-beat basis in relation to each preceding RR interval at concentrations approximating the same unbound human concentrations. E-4031, cisapride and terodiline statistically increased the QT RR1000 interval [the QT interval at a 60 beats/min (bpm) heart rate] 23, 8, and 9 ms, respectively, at concentrations 0.3 to 15.8 times their relevant clinical level. Increases were not observed for terfenadine or verapamil (p Ͼ 0.05 at all doses). Inspection of individual dog QT versus RR interval relationships showed clear QT interval responses specific to each treatment but not readily apparent when data are averaged at a heart rate of 60 bpm. For specific rectifier K ϩ current (IKr) blockers, robust effects on mean QT prolongation can be detected. However, for drugs that affect repolarization through multiple channels, the effect on the mean QT interval may be more difficult to detect. Inspection of the beat-to-beat QT-RR interval relationship in an individual animal can increase the sensitivity for more accurate clinical prediction.In the past four years, several drugs such as sertindole, cisapride, and terfenadine have been withdrawn from the marketplace due to the rare occurrence of the fatal ventricular arrhythmia, Torsades de Pointes (TdP). Retrospective evaluation of the European database on these compounds indicated an association of QT prolongation in patients on these medications (Haverkamp et al., 2000). As a result, the Committee for Proprietary Medicinal Products (1997) issued a Points to Consider document on the conduct of studies for the development of noncardiovascular drugs. This and further impending guidance from the International Committee for Harmonization have focused a great deal of attention on the preclinical assessments used to predict the liability for patient populations to experience QT prolongation. Despite the ongoing controversy concerning whether there is a definitive cause and effect relationship, QT prolongation has by default become a surrogate marker for risk of developing TdP.This study is one of a series of assessments from our laboratories examining the utility of a variety of both in vitro and in vivo preclinical assessments of drugs that are known to produce clinically detectable QT prolongation in humans. Although the magnitude of the QT interval prolongation and the risk associated with TdP are s...

show abstract

Concentration dependent cardiotoxicity of terodiline in patients treated for urinary incontinence.

Cited by 43 publications

References 27 publications

Enantiomeric drug development: Issues, considerations, and regulatory requirements

Enantiomeric drug development: Issues, considerations, and regulatory requirements

Efficacy and Cardiac Safety of Propiverine in Elderly Patients – A Double–Blind, Placebo–Controlled Clinical Study

The Relationship of Clinical QT Prolongation to Outcome in the Conscious Dog Using a Beat-to-Beat QT-RR Interval Assessment

Contact Info

Product

Resources

About

Concentration dependent cardiotoxicity of terodiline in patients treated for urinary incontinence.

Cited by 43 publications

References 27 publications

Enantiomeric drug development: Issues, considerations, and regulatory requirements

Enantiomeric drug development: Issues, considerations, and regulatory requirements

Efficacy and Cardiac Safety of Propiverine in Elderly Patients &ndash; A Double&ndash;Blind, Placebo&ndash;Controlled Clinical Study

The Relationship of Clinical QT Prolongation to Outcome in the Conscious Dog Using a Beat-to-Beat QT-RR Interval Assessment

Contact Info

Product

Resources

About

Efficacy and Cardiac Safety of Propiverine in Elderly Patients – A Double–Blind, Placebo–Controlled Clinical Study