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Antimicrobial Agents and Chemotherapy, March 2002, p. 938-939, Vol. 46, No. 3
0066-4804/02/$04.00+0     DOI: 10.1128/AAC.46.3.938-939.2002
Copyright © 2002, American Society for Microbiology. All Rights Reserved.

LETTER TO THE EDITOR

Importance of Species Selection in Arrythmogenic Models of Q-T Interval Prolongation

Top Letter References

 
In a recent article by Ohtani and colleagues (4), prolongation of the Q-T interval in an anesthetized-rat electrocardiogram (ECG) model was used to determine the arrhythmogenic potential of macrolide antibiotics. Prolongation of the Q-T interval on an ECG has been linked to the rare (but potentially fatal) ventricular arrhythmia known as Torsade de Pointes. In vitro studies suggest that most Q-T-prolonging drugs block the delayed rectifier potassium current (iK_r) carried by the pore-forming subunit encoded by hERG (human ether-a-go-go-related gene) in humans (6). While hERG-like mRNA and functional iK_r current have been found in many species including dogs, guinea pigs, and rabbits (3), little (if any) functional iK_r or hERG-like current is found in the rat ventricle (8). Therefore, we were surprised at the sensitivity of this rat ECG model to the selected macrolide antibiotics, given that these drugs do not elicit iK_r blocking until supratherapeutic concentrations are achieved (7). To clarify these issues, we chose to compare the effects of erythromycin and two established iK_r-blocking drugs on repolarization of rat ventricular muscle, because Q-T prolongation in vivo is reflective of action potential prolongation.

We used standard microelectrode techniques (2) to evaluate the effects of erythromycin (at a concentration achieved by Ohtani et al. in plasma [3.6 µM]) as well as two standard iK_r blockers, dofetilide (10 nM) and E-4031 (1.0 µM), at concentrations 2.5-fold greater than those shown to block 50% of native iK_r current (1, 5). These concentrations have also been shown to significantly prolong the action potential duration (APD) in other species prominently expressing iK_r (5). In brief, male CD rats (300 to 350 g; Charles River Labs) were anesthetized, hearts were removed, and ventricular papillary muscles were excised and placed in a warmed (37°C) superfusion chamber perfused at the rate of 8 to 10 ml/min with Tyrode's solution containing (millimolar concentrations) NaCl, 131; NaHCO₃, 18; NaH₂PO₄, 1.8; MgCl₂, 0.5; dextrose, 5.5; KCl, 4; and CaCl₂, 2 (aerated with 95% O₂-5% CO₂ [pH = 7.4] at room temperature). Muscle preparations were field stimulated at a basic cycle length of 180 ms (corresponding to a typical rat heart rate of approximately 330 beats per min) with a biphasic waveform at a twofold threshold using platinum electrodes in the bath floor. Preparations were paced and equilibrated for a minimum of 1 h before recording. Preparations were considered suitable for study if the maximum diastolic potential was more negative than -70 mV and the APD was greater than 20 ms. Records were obtained during a 10-min drug-free control period and ensuing 25-min period of drug exposure. Impalements were maintained throughout each experiment. APD was measured from the upstroke until repolarization reached 10 mV positive to the maximum diastolic potential. All drugs were made up fresh daily as stocks in 100% dimethyl sulfoxide and then diluted in Tyrode's solution to achieve a final dimethyl sulfoxide concentration of 0.1%. Values are presented as means ± standard errors of the means. Erythromycin lactobionate and dofetilide were synthesized in-house; E-4031 was purchased from Wako Chemicals.

The typical effects of erythromycin, E-4031, and dofetilide on rat ventricular muscle action potentials are illustrated in Fig. 1. Rat papillary muscle repolarization is very sensitive to erythromycin (Fig. 1B) but not the iK_r-blocking drug E-4031 (Fig. 1A). Figure 1C summarizes results obtained from 15 preparations (10 hearts); drugs are arranged on the abscissa in the order of increasing potency for native-iKr blockade. Whereas erythromycin elicited 76.6% ± 6.4% APD prolongation at concentrations substantially lower than those required for iK_r blockade, the iK_r blockers dofetilide and E-4031 elicited much smaller prolongation (2.4% ± 2.9% and 1.8% ± 2.1%, respectively) at concentrations 2.5-fold the 50% inhibitory concentration for iK_r blockade. The greater APD prolongation of rat papillary muscle with erythromycin compared to potent iK_r-blocking drugs suggests that iK_r is not the current predominantly affected by erythromycin in the rat papillary muscle.

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FIG. 1. Effects of select drugs on rat ventricular repolarization. (A and B) Action potential traces from rat papillary muscle preparations. In each panel, pairs of superimposed traces show effects obtained during continuous recordings before and after drug exposure. Panel A highlights the lack of effect of E-4031 (1.0 µM) on APD, while panel B shows prominent prolongation of APD with erythromycin (3.6 µM) exposure. (C) Effects of erythromycin (Ery.), E-4031, and dofetilide on APD. Drugs are arranged on the abscissa in the order of increasing potency for blocking native iKr. While erythromycin significantly prolongs the APD at a concentration far below that which blocks iKr (IC50 = 100 µM [7]), high concentrations of iKr-blocking agents E-4031 and dofetilide (2.5-fold above the 50% inhibitory concentration for blocking native iKr [1, 5]) minimally prolong repolarization. n = 5 per group; the data are means ± standard errors of the means. Statistical significance was defined as P < 0.05 (*) (paired t tests).

In conclusion, this in vitro study corroborates the findings of Ohtani et al. regarding the sensitivity of the rat in vivo ECG model for erythromycin. However, the lack of effects of high concentrations of known iK_r-blocking drugs on the APD corroborates the reported paucity of iK_r in the rat ventricular muscle and suggests that currents other than iK_r are responsible for delaying repolarization with erythromycin. Thus, the present studies suggest that the rat ECG model is inappropriate for evaluating the proarrhythmic potential of noncardiovascular drugs that prolong the Q-T interval by blocking iK_r. In addition, this highlights the need to consider differences in the ionic currents expressed in preparations employed to evaluate cardiac safety. Further studies are necessary to determine the ionic channel(s) responsible for delayed repolarization in the rat myocardium seen with macrolide antibiotics.

 
Editor's Note: The authors of the published article declined to respond.

Top Letter References

 

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1. Carmeliet, E. 1992. Voltage- and time-dependent block of the delayed K+ current in cardiac myocytes by dofetilide. J. Pharmacol. Exp. Ther. 262:809-817.[Abstract/Free Full Text]
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2. Gintant, G. A., J. T. Limberis, J. S. McDermott, C. D. Wegner, and B. F. Cox. 2001. The canine Purkinje fiber: an in vitro model system for acquired long QT syndrome and drug-induced arrhythmogenesis. J. Cardiovasc. Pharmacol. 37:607-618.[CrossRef][Medline]
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3. Nerbonne, J. M. 2000. Molecular basis of functional voltage-gated K⁺ channel diversity in the mammalian myocardium. J. Physiol. 525:285-298.[Abstract/Free Full Text]
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4. Ohtani, H., C. Taninaka, E. Hanada, H. Kotaki, H. Sato, Y. Sawada, and T. Iga. 2000. Comparative pharmacodynamic analysis of Q-T interval prolongation induced by the macrolides clarithromycin, roxithromycin, and azithromycin in rats. Antimicrob. Agents Chemother. 44:2630-2637.[Abstract/Free Full Text]
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5. Sanguinetti, M. C., and N. K. Jurkiewicz. 1990. Two components of cardiac delayed rectifier K+ current. J. Gen. Physiol. 96:195-215.[Abstract/Free Full Text]
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6. Trudeau, M. C., J. W. Warmke, B. Ganetzky, and G. A. Robertson. 1995. hERG, a human inward rectifier in the voltage-gated potassium channel family. Science 269:92-95.[Abstract/Free Full Text]
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7. West, P. D., D. K. Martin, J. A. Bursill, K. R. Wyse, and T. J. Cambell. 1998. Comparative study of the effects of erythromycin and roxithromycin on action potential duration and potassium currents in canine Purkinje fibers and rabbit myocardium. J. Cardiovasc. Pharmacol. Ther. 3:29-36.
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8. Wymore, R. S., G. A. Gintant, R. T. Wymore, J. E. Dixon, D. McKinnon, and I. S. Cohen. 1997. Tissue and species distribution of mRNA for the iK_r-like K⁺ channel, erg. Circ. Res. 80:261-268.[Abstract/Free Full Text]

						Jeff S. McDermott* Heinz J. Salmen Bryan F. Cox Gary A. Gintant Abbott Laboratories, Abbott Park, IL 60064-6119
						* Phone: (847) 937-4367 Fax: (847) 938-5286 E-mail: Jeffrey.S.McDermott{at}0040Abbott.com

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Antimicrobial Agents and Chemotherapy, March 2002, p. 938-939, Vol. 46, No. 3
0066-4804/02/$04.00+0     DOI: 10.1128/AAC.46.3.938-939.2002
Copyright © 2002, American Society for Microbiology. All Rights Reserved.

This Article Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Services Similar articles in this journal Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Reprints and Permissions Copyright Information Books from ASM Press MicrobeWorld Citing Articles Citing Articles via Google Scholar Google Scholar Articles by McDermott, J. S. Articles by Gintant, G. A. Search for Related Content PubMed PubMed Citation Articles by McDermott, J. S. Articles by Gintant, G. A.