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Effects of proarrhythmic drugs on relaxation time and beating pattern in rat engineered heart tissue

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Effects of proarrhythmic drugs on relaxation time and beating pattern in rat engineered heart tissue. / Eder, Alexandra; Hansen, Arne; Uebeler, June; Schulze, Thomas; Neuber, Christiane; Schaaf, Sebastian; Yuan, Lei; Christ, Torsten; Vos, Marc A; Eschenhagen, Thomas.

in: BASIC RES CARDIOL, Jahrgang 109, Nr. 6, 01.11.2014, S. 436.

Publikationen: SCORING: Beitrag in Fachzeitschrift/ZeitungSCORING: ZeitschriftenaufsatzForschungBegutachtung

Harvard

Eder, A, Hansen, A, Uebeler, J, Schulze, T, Neuber, C, Schaaf, S, Yuan, L, Christ, T, Vos, MA & Eschenhagen, T 2014, 'Effects of proarrhythmic drugs on relaxation time and beating pattern in rat engineered heart tissue', BASIC RES CARDIOL, Jg. 109, Nr. 6, S. 436. https://doi.org/10.1007/s00395-014-0436-7

APA

Eder, A., Hansen, A., Uebeler, J., Schulze, T., Neuber, C., Schaaf, S., Yuan, L., Christ, T., Vos, M. A., & Eschenhagen, T. (2014). Effects of proarrhythmic drugs on relaxation time and beating pattern in rat engineered heart tissue. BASIC RES CARDIOL, 109(6), 436. https://doi.org/10.1007/s00395-014-0436-7

Vancouver

Eder A, Hansen A, Uebeler J, Schulze T, Neuber C, Schaaf S et al. Effects of proarrhythmic drugs on relaxation time and beating pattern in rat engineered heart tissue. BASIC RES CARDIOL. 2014 Nov 1;109(6):436. https://doi.org/10.1007/s00395-014-0436-7

Bibtex

@article{6b98f847626d4a97b413f381e35e9020,
title = "Effects of proarrhythmic drugs on relaxation time and beating pattern in rat engineered heart tissue",
abstract = "The assessment of proarrhythmic risks of drugs remains challenging. To evaluate the suitability of rat engineered heart tissue (EHT) for detecting proarrhythmic effects. We monitored drug effects on spontaneous contractile activity and, in selected cases, on action potentials (sharp microelectrode) and Ca2+ transients (Fura-2) and contraction under electrical pacing. The Ito-blocker inhibitor 4-aminopyridine increased action potential duration and T2 and caused aftercontractions, which were abolished by inhibitors of ryanodine receptors (RyR2; JTV-519) or sodium calcium exchanger (NCX; SEA0400). 77 Drugs were then tested at 1-10-100× free therapeutic plasma concentrations (FTPC): Inhibitors of IKr, IKs, Ito, antiarrhythmics (8), drugs withdrawn from market for torsades des pointes arrhythmias (TdP, 5), drugs with measurable (7) or isolated TdP incidence (13), drugs considered safe (14), 28 new chemical entities (NCE). Inhibitors of IKr or IKs had no effect alone, but substantially prolonged relaxation time (T2) when combined at high concentration. 15/33 drugs associated with TdP and 6/14 drugs considered non-torsadogenic (cibenzoline, diltiazem, ebastine, ketoconazole, moxifloxacin, and phenytoin) induced concentration-dependent T2 prolongations (10-100× FTPC). Bepridil, desipramine, imipramine, thioridazine, and erythromycin induced irregular beating. Three NCE prolonged T2, one reduced force. Drugs inhibiting repolarization prolong relaxation in rat EHTs and cause aftercontractions involving RyR2 and NCX. Insensitivity to IKr inhibitors makes rat EHTs unsuitable as general proarrhythmia screen, but favors detection of effects on Ito, IKs + Ito or IKs + IKr. Screening a large panel of drugs suggests that effects on these currents, in addition to IKr, are more common than anticipated.",
author = "Alexandra Eder and Arne Hansen and June Uebeler and Thomas Schulze and Christiane Neuber and Sebastian Schaaf and Lei Yuan and Torsten Christ and Vos, {Marc A} and Thomas Eschenhagen",
year = "2014",
month = nov,
day = "1",
doi = "10.1007/s00395-014-0436-7",
language = "English",
volume = "109",
pages = "436",
journal = "BASIC RES CARDIOL",
issn = "0300-8428",
publisher = "D. Steinkopff-Verlag",
number = "6",

}

RIS

TY - JOUR

T1 - Effects of proarrhythmic drugs on relaxation time and beating pattern in rat engineered heart tissue

AU - Eder, Alexandra

AU - Hansen, Arne

AU - Uebeler, June

AU - Schulze, Thomas

AU - Neuber, Christiane

AU - Schaaf, Sebastian

AU - Yuan, Lei

AU - Christ, Torsten

AU - Vos, Marc A

AU - Eschenhagen, Thomas

PY - 2014/11/1

Y1 - 2014/11/1

N2 - The assessment of proarrhythmic risks of drugs remains challenging. To evaluate the suitability of rat engineered heart tissue (EHT) for detecting proarrhythmic effects. We monitored drug effects on spontaneous contractile activity and, in selected cases, on action potentials (sharp microelectrode) and Ca2+ transients (Fura-2) and contraction under electrical pacing. The Ito-blocker inhibitor 4-aminopyridine increased action potential duration and T2 and caused aftercontractions, which were abolished by inhibitors of ryanodine receptors (RyR2; JTV-519) or sodium calcium exchanger (NCX; SEA0400). 77 Drugs were then tested at 1-10-100× free therapeutic plasma concentrations (FTPC): Inhibitors of IKr, IKs, Ito, antiarrhythmics (8), drugs withdrawn from market for torsades des pointes arrhythmias (TdP, 5), drugs with measurable (7) or isolated TdP incidence (13), drugs considered safe (14), 28 new chemical entities (NCE). Inhibitors of IKr or IKs had no effect alone, but substantially prolonged relaxation time (T2) when combined at high concentration. 15/33 drugs associated with TdP and 6/14 drugs considered non-torsadogenic (cibenzoline, diltiazem, ebastine, ketoconazole, moxifloxacin, and phenytoin) induced concentration-dependent T2 prolongations (10-100× FTPC). Bepridil, desipramine, imipramine, thioridazine, and erythromycin induced irregular beating. Three NCE prolonged T2, one reduced force. Drugs inhibiting repolarization prolong relaxation in rat EHTs and cause aftercontractions involving RyR2 and NCX. Insensitivity to IKr inhibitors makes rat EHTs unsuitable as general proarrhythmia screen, but favors detection of effects on Ito, IKs + Ito or IKs + IKr. Screening a large panel of drugs suggests that effects on these currents, in addition to IKr, are more common than anticipated.

AB - The assessment of proarrhythmic risks of drugs remains challenging. To evaluate the suitability of rat engineered heart tissue (EHT) for detecting proarrhythmic effects. We monitored drug effects on spontaneous contractile activity and, in selected cases, on action potentials (sharp microelectrode) and Ca2+ transients (Fura-2) and contraction under electrical pacing. The Ito-blocker inhibitor 4-aminopyridine increased action potential duration and T2 and caused aftercontractions, which were abolished by inhibitors of ryanodine receptors (RyR2; JTV-519) or sodium calcium exchanger (NCX; SEA0400). 77 Drugs were then tested at 1-10-100× free therapeutic plasma concentrations (FTPC): Inhibitors of IKr, IKs, Ito, antiarrhythmics (8), drugs withdrawn from market for torsades des pointes arrhythmias (TdP, 5), drugs with measurable (7) or isolated TdP incidence (13), drugs considered safe (14), 28 new chemical entities (NCE). Inhibitors of IKr or IKs had no effect alone, but substantially prolonged relaxation time (T2) when combined at high concentration. 15/33 drugs associated with TdP and 6/14 drugs considered non-torsadogenic (cibenzoline, diltiazem, ebastine, ketoconazole, moxifloxacin, and phenytoin) induced concentration-dependent T2 prolongations (10-100× FTPC). Bepridil, desipramine, imipramine, thioridazine, and erythromycin induced irregular beating. Three NCE prolonged T2, one reduced force. Drugs inhibiting repolarization prolong relaxation in rat EHTs and cause aftercontractions involving RyR2 and NCX. Insensitivity to IKr inhibitors makes rat EHTs unsuitable as general proarrhythmia screen, but favors detection of effects on Ito, IKs + Ito or IKs + IKr. Screening a large panel of drugs suggests that effects on these currents, in addition to IKr, are more common than anticipated.

U2 - 10.1007/s00395-014-0436-7

DO - 10.1007/s00395-014-0436-7

M3 - SCORING: Journal article

C2 - 25209140

VL - 109

SP - 436

JO - BASIC RES CARDIOL

JF - BASIC RES CARDIOL

SN - 0300-8428

IS - 6

ER -