Class III Electrophysiologic Actions of Imidazole-Substituted Diheterabicyclononanes in Canine Myocardium

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Vol. 281, Issue 1, 155-162, 1997

Class III Electrophysiologic Actions of Imidazole-Substituted Diheterabicyclononanes in Canine Myocardium

Eugene Patterson , Benjamin J. Scherlag , Subiah Sangiah, Gregory L. Garrison, Kevin M. Couch, K. Darrell Berlin and Ralph Lazzara

Departments of Pharmacology (E.P.) and Medicine (E.P., B.J.S., R.L.), College of Medicine, University of Oklahoma Health Sciences Center, Oklahoma City, Oklahoma, Research Service (E.P., B.J.S.), Department of Veterans Affairs Medical Center, Oklahoma City, Oklahoma and Departments of Pharmacology (S.S.) and Chemistry (G.L.G., K.M.C., K.D.B.), Oklahoma State University, Stillwater, Oklahoma

	Abstract

Top Abstract Introduction Methods Results Discussion References

The electrophysiologic effects of the imidazole-substituted diheterabicyclo[3.3.1]nonane compounds GLG-V-13 and KMC-IV-84were evaluated in canine ventricular tissues using intracellularand extracellular recordings. The drugs produced a concentration-dependentprolongation of action potential duration at 90% of repolarizationin Purkinje (338 ± 26 to 611 ± 43 msec, 10 mg/l GLG-V-13; 328± 17 to 468 ± 18 msec, 10 mg/l KMC-IV-84), in right ventricularsubendocardium (260 ± 18 to 335 ± 18 msec, 10 mg/l GLG-V-13; 221± 9 to 264 ± 13 msec, 10 mg/l KMC-IV-84) and in left ventricularepicardium (195 ± 13 to 256 ± 18 msec, 10 mg/l GLG-V-13; 203 ±11 to 273 ± 26 msec, 10 mg/l KMC-IV-84) without altering restingmembrane potential, action potential amplitude, overshoot potential,V_max, conduction velocity or Purkinje fiber automaticity. Prolongationof the effective refractory period was proportional to the changein action potential duration at 90% of repolarization. Prolongationof action potential duration at 90% of repolarization was maximalat paced cycle lengths exceeding 1000 msec and was minimal ata paced cycle length of 250 msec (Purkinje: 266 ± 20 vs. 6 ± 8msec, GLG-V-13; 178 ± 12 vs. 10 ± 10 msec, KMC-IV-84. Right ventricularsubendocardium: 70 ± 12 vs. 10 ± 2 msec, GLG-V-13; 60 ± 8 vs.19 ± 6 msec. Left ventricular epicardium: 67 ± 13 vs. 10 ± 5 msec,GLG-V-13; 68 ± 12 vs. 16 ± 8 msec, KMC-IV-84). An increase inK⁺_o to 12 mM reduced action potential prolongation by GLG-V-13 andKMC-IV-84 in left ventricular epicardium. The results demonstrateselective class III electrophysiologic properties for imidazole-substituteddiheterabicyclo[3.3.1]nonane compounds.

	Introduction

Top Abstract Introduction Methods Results Discussion References

Diheterabicyclo[3.3.1]nonane-based compounds have shown potential as antiarrhythmic drugs, suppressing sustained, reentrantventricular tachycardias in the dog during subacute myocardialinfarction (Scherlag et al., 1988; Smith et al., 1990; Baileyet al., 1984; Fazekas et al., 1993a; Fazekas et al., 1993b). Mostof the diheterabicyclo[3.3.1]nonane compounds studied to datehave little effect on blood pressure in the dog during subacutemyocardial infarction (Scherlag et al., 1988, Smith et al., 1990;Bailey et al., 1984; Fazekas et al., 1993a; Fazekas et al., 1993b)and reduce the force of contraction in rabbit papillary muscles,only at supratherapeutic concentrations producing inexcitability(Chen et al., 1992, Fazekas et al., 1993c).

The first diheterabicyclo[3.3.1]nonane to be evaluated using intracellular microelectrode recordings was BRB-I-28. BRB-I-28differs from the present drugs in having a 3-thia substituent(3-azo in GLG-V-13 and KMC-IV-84) and a 7-benzyl substituent onthe 7-azo position (amide-linked imidazole in GLG-V-13 and sulfonamide-linkedimidazole in KMC-IV-84) (fig. 1). BRB-I-28 reduces V_max and/orconduction times in normal cardiac tissues only at paced cyclelengths less than 300 msec in vivo (Scherlag et al., 1988; Pattersonet al., 1993) and in vitro (Patterson et al., 1993). The depressionof V_max and conduction velocity only at rapid HRs is consistentwith the drug's molecular weight (223.1 daltons), pK_a (11.8),and low lipid solubility (octanol:water partition coefficient2.82). Ischemic injury or subacute myocardial infarction increasesboth tonic conduction block and use-dependent conduction block(Patterson et al., 1993). BRB-I-28 produces little change in actionpotential duration in Purkinje tissue, right ventricular endocardiumand left ventricular epicardium (Patterson et al., 1991; Pattersonet al., 1993).

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Fig. 1. Chemical structures of BRB-I-28, GLG-V-13 and KMC-IV-84. In GLG-V-13 and KMC-IV-84, nitrogen has been substituted for sulfurin the diheterabicyclo[3.3.1]nonane ring. GLG-V-13 contains anamide-imidazole linkage, and KMC-IV-84 contains a sulfonamide-imidazolelinkage.

Modifications were included into the diheterabicyclo[3.3.1]nonane structure of BRB-I-28 and related drugs to incorporate actionpotential prolongation. To increase separation of the two positivelycharged nitrogens, the positive charge of the 7-benzyl amine substituenton the diheterabicyclo[3.3.1]nonane ring was changed to a nonchargedsulfonamide or amide linked through a benzene ring to a chargedimidazole. This change was proposed to increase hydrophilicityand possibly to add class III electrophysiologic activity (inhibitionof I_K) (Morgan et al., 1990; Lis et al., 1990) to the existingclass Ib activity of BRB-I-28. The following experiments wereperformed to determine the cellular electrophysiologic actionsof the imidazole-substituted diheterabicyclo[3.3.1]nonane drugsGLG-V-13 (3-[4 $'$ -(1H-imidazol-1-yl)benzoyl]-7-isopropyl-3,7-diazabicyclo[3.3.1]nonanedihydroperchlorate) and KMC-IV-84 (7-[4 $'$ -(1H-imidazol-1-yl)benzenesulfonyl]-3-isopropyl-3,7-diazabicyclo[3.3.1]nonanedihydroperchlorate) in canine ventricular tissues.

	Methods

Top Abstract Introduction Methods Results Discussion References

Purkinje tissues. Male mongrel dogs were anesthetized with i.v. sodium pentobarbital (30 mg/kg). Tissue sections containing free-running Purkinjefiber strands were removed from right (N = 12) or left (N = 12)ventricular endocardium. The tissues were superfused with Tyrode'ssolution (115 mM sodium chloride, 4.0 mM potassium chloride, 1.0mM sodium dihydrogen phosphate, 1.5 mM magnesium chloride, 24mM sodium bicarbonate and 1.35 mM calcium chloride) bubbled with95% oxygen: 5% carbon dioxide (pH = 7.4). A Grass S-88 stimulatorwas used to initiate electrical activity at the proximal insertionof a free-running Purkinje fiber (2-msec stimuli, twice diastolicthreshold). A glass microelectrode (10-20-Mohm resistance) wasused to record intracellular potentials from the free-runningPurkinje fiber. A bipolar electrode was used to record activationof the same fiber at its distal insertion. A differentiating amplifierwith peak-and-hold detector was used to record V_max. Differentiationwas linear in the range of 50 to 1000 V/sec. Membrane responsivenesscurves were obtained by the introduction of premature stimuli.Electrical recordings were performed during pacing at rates from0.2 to 4.0 Hz and at a pacing rate of 1.0 Hz with the introductionof premature stimuli from 500 msec to local refractoriness in5-msec intervals. All electrical recordings were digitized andstored, and permanent records were obtained using a Gould ES 2000recording system (Gould Electronics).

Subendocardial right ventricular myocardium. Male mongrel dogs were anesthetized with i.v. sodium pentobarbital (30 mg/kg). Subendocardial tissue sections measuring approximately8 × 15 mm were removed from the right ventricle, immediately beneaththe tricuspid valve annulus. The tissue preparations were superfusedwith Tyrode's solution (composition described previously). A GrassS-88 stimulator was used to pace the tissue preparation (2-msecstimuli, twice diastolic threshold). A glass microelectrode (10-20-Mohmresistance) was used to record intracellular potentials, and abipolar electrode was used to record local activation near themicroelectrode recording site. A differentiating amplifier withpeak-and-hold detector was used to record V_max as described previously.Electrical recordings were obtained during pacing at rates from0.2 to 5.0 Hz and at a pacing rate of 1.0 Hz with the introductionof premature stimuli from 500 msec to local refractoriness in5-msec intervals.

Subepicardial left ventricular myocardium. Male mongrel dogs were anesthetized with i.v. sodium pentobarbital (30 mg/kg). Left ventricular epicardial tissue sectionsapproximately 10 mm × 15 mm × 1 mm thick were removed from theanterior left ventricle. The long axis of the preparation wasremoved parallel to the diagonal branches of the anterior descendingcoronary artery and, hence, parallel to epicardial fiber orientation.The tissue preparations were superfused with Tyrode's solutionas previously described. A Grass S-88 stimulator was used to pacethe tissue preparation (2-msec stimuli, twice diastolic threshold)from bipolar electrode sites located in two opposing corners ofthe preparation. A glass microelectrode (10-20-Mohm resistance)was used to record intracellular potentials, and a bipolar electrodewas used to record local activation near the microelectrode recordingsite. The stimulation sites and recording sites were arrangedso that excitation could be performed both longitudinal and transverseto epicardial fiber orientation. A differentiating amplifier withpeak-and-hold detector was used to record V_max as described previously.Electrical recordings were performed during pacing at rates from0.2 to 5.0 Hz and at a pacing rate of 1.0 Hz with the introductionof premature stimuli from 500 msec to local refractoriness in5-msec intervals.

Drug administration. Following a 1 hr period of superfusion with normal Tyrode's solution, GLG-V-13 and KMC-IV-84 (as hydroperchlorate salts) wereadministered in half-log increments from 0.32 to 10 mg/l. Eachdrug concentration was administered for 20 min before electrophysiologictesting at each drug concentration. After drug administrationended superfusion with normal Tyrode's solution was performedfor 30 min and electrophysiologic testing was repeated.

Statistical analysis. Differences between drug treatment groups were determined using one-way analysis of variance for repeated measures. Individualdifferences were determined using Scheffé's test. P $<=$ .05 wasthe criterion for significance.

	Results

Top Abstract Introduction Methods Results Discussion References

Canine cardiac Purkinje fibers. GLG-V-13 and KMC-IV-84 administration failed to alter maximal diastolic potential ( $-$ 91 ± 1, $-$ 90 ± 1 mV), action potentialamplitude (119 ± 2, 121 ± 2 mV), overshoot potential (29 ± 2,31 ± 2 mV), V_max (486 ± 44, 524 ± 42 V/sec) or conduction time(24 ± 6, 15 ± 3 msec) from predrug values (respectively) in caninecardiac Purkinje fibers (table 1). V_max and conduction time wereunchanged from predrug values over the entire range of cycle lengthsstudied (250-5000 msec). There was no shift in the membrane responsivenesscurve (constructed using premature ventricular stimuli) (fig.2) (cycle length = 1000 msec). Both GLG-V-13 and KMC-IV-84 produceda concentration-dependent prolongation of APD₂₅, APD₅₀, APD₉₀and APD₁₀₀ in free-running Purkinje strands (table 1). The prolongationof the effective refractory period was proportional to APD₉₀.GLG-V-13 and KMC-IV-84 (at concentrations of 0.32, 1.0, 3.2, and10 mg/l) failed to alter spontaneous automaticity (16 ± 5, 16± 1/min, respectively) or take-off potentials ( $-$ 76 ± 4, $-$ 75 ±3 mV, respectively) in Purkinje tissues.

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TABLE 1
Electrophysiologic actions of GLG-V-13 and KMC-IV-84 in canine Purkinje tissue

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Fig. 2. Membrane responsiveness curves for GLG-V-13 and KMC-IV-84. Membrane responsiveness curves are shown at predrug ( $open circle$ ), 10 mg/ldrug ( $bullet$ ) and washout ( $square$ ) for GLG-V-13 (10 mg/l) and KMC-IV-84(10 mg/l). No effect of drug administration was observed in caninePurkinje tissue.

The prolongation of action potential duration demonstrated reverse use-dependence. Prolongation of the Purkinje action potentialwas maximal at paced cycle lengths exceeding 2000 msec and wasminimal at paced cycle lengths less than 400 msec. The relationshipbetween APD₉₀ and paced cycle length before, during and afterGLG-V-13 or KMC-IV-84 administration is shown in figure 3.

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Fig. 3. Reverse use-dependence of action potential prolongation in canine Purkinje fibers $---$ effects of GLG-V-13 and KMC-IV-84. The relationshipbetween paced cycle length and APD₉₀ is shown for GLG-V-13 andKMC-IV-84. No significant prolongation of action potential durationis observed at cycle lengths of 333 msec or less (P < .01 vs.predrug and washout for paced cycle lengths of 400, 500, 1000,2000 and 5000 msec for both drugs).

Canine right ventricular endocardium. Both GLG-V-13 and KMC-IV-84 produced a concentration-dependent prolongation of APD₂₅, APD₅₀, APD₉₀ and APD₁₀₀ in subendocardiumfrom the right ventricle (table 2). Prolongation of the actionpotential by GLG-V-13 and KMC-IV-84 was observed without alterationof resting membrane potential ( $-$ 85 ± 1, $-$ 83 ± 1 mV), action potentialamplitude (110 ± 2, 112 ± 1 mV), overshoot potential (25 ± 2,29 ± 1 mV), V_max (273 ± 40, 213 ± 14 V/sec) or conduction time(35 ± 6, 39 ± 3 msec) from predrug values (respectively). Theprolongation of the effective refractory period was proportionalto APD₉₀ (table 2).

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TABLE 2
Electrophysiologic actions of GLG-V-13 and KMC-IV-84 in canine ventricular endocardium

The prolongation of action potential duration demonstrated reverse use-dependence. Prolongation of the action potential wasmaximal at paced cycle lengths exceeding 1000 msec and was minimalat paced cycle lengths less than 400 msec (fig. 4). No changein V_max or conduction time was observed at paced cycle lengthsfrom 5000 to 250 msec after drug administration.

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Fig. 4. Reverse use-dependence of action potential prolongation in canine right ventricular endocardium $---$ effects of GLG-V-13 and KMC-IV-84.The relationship between paced cycle length and APD₉₀ is shownfor GLG-V-13 and KMC-IV-84. No significant prolongation of actionpotential duration is observed at cycle lengths of 333 msec orless (P < .01 vs. predrug and washout for paced cycle lengthsof 400, 500, 1000, 2000 and 5000 msec for both drugs).

Canine left ventricular epicardium. Both GLG-V-13 and KMC-IV-84 produced a concentration-dependent prolongation of APD₂₅, APD₅₀, APD₉₀ and APD₁₀₀ in subepicardiumfrom the left ventricle (table 3). Prolongation of the actionpotential by GLG-V-13 and KMC-IV-84 was observed without changein resting membrane potential ( $-$ 83 ± 1, $-$ 83 ± 1 mV), action potentialamplitude (108 ± 1, 110 ± 2 mV), overshoot potential (25 ± 1,28 ± 2 mV), V_max longitudinal to epicardial fiber axis (178 ±17, 218 ± 14 V/sec), V_max transverse to epicardial fiber axis(214 ± 16, 249 ± 14 V/sec), conduction velocity longitudinal toepicardial fiber orientation (0.54 ± 0.05, 0.59 ± 0.08 M/sec)and conduction velocity transverse to epicardial fiber orientation(0.20 ± 0.02, 0.17 ± 0.01 M/sec) from predrug values (respectively).The prolongation of the effective refractory period was proportionalto APD₉₀ (table 3).

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TABLE 3
Electrophysiologic actions of GLG-V-13 and KMC-IV-84 in canine left ventricular epicardium

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Fig. 5. Reverse use-dependence of action potential prolongation in canine left ventricular epicardium $---$ effects of GLG-V-13 and KMC-IV-84.The relationship between paced cycle length and APD₉₀ is shownfor GLG-V-13 and KMC-IV-84. No significant prolongation of actionpotential duration is observed at cycle lengths of 333 msec orless (P < .01 vs. predrug and washout for paced cycle lengthsof 400, 500, 1000, 2000 and 5000 msec for GLG-V-13 and for pacedcycle lengths of 500, 1000, 2000 and 5000 msec for KMC-IV-84).

No changes in V_max and conduction velocity were observed after drug administration at paced cycle lengths from 5000 to 250msec. V_max was increased when intracellular activation occurredtransverse rather than longitudinal to fiber axis. The ratio ofconduction velocity longitudinal to fiber orientation to conductionvelocity transverse to fiber orientation (cycle length = 1000msec) was 2.73 ± 0.31 in the GLG-V-13 group, predrug, and 3.42± 0.29 in the KMC-IV-84 group, predrug. The ratio was not alteredby GLG-V-13 or KMC-IV-84 administration.

Depolarized canine left ventricular epicardium. Increasing extracellular potassium from 4.0 to 12 mM decreased resting membrane potential, action potential amplitude, overshootpotential, V_max and conduction velocity (table 4). GLG-V-13 andKMC-IV-84 (0.32, 1.0, 3.2 and 10 mg/l) failed significantly toalter these parameters over a range of paced cycle lengths from250 to 5000 msec.

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TABLE 4
Electrophysiologic actions in depolarized canine left ventricular epicardium

Both GLG-V-13 and KMC-IV-84 produced a concentration-dependent prolongation of APD₅₀, APD₉₀ and APD₁₀₀ in depolarized leftventricular epicardium. Less prolongation of the action potentialwas observed in depolarized epicardium than in normal epicardium.Prolongation of APD₉₀ was more pronounced at prolonged cycle lengthsand was minimal at paced cycle lengths less than 400 msec (fig.6). At reduced membrane potentials induced by increasing K⁺_o to 12 mM, GLG-V-13 and KMC-IV-84 failed to reduced V_max andconduction velocity over a range of paced cycle lengths of 250to 500 msec.

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Fig. 6. Reverse use-dependence of action potential prolongation in depolarized (12 mM) K⁺_o canine left ventricular epicardium $---$ effects of GLG-V-13 and KMC-IV-84.The relationship between paced cycle length and APD₉₀ is shownfor depolarized left ventricular epicardium exposed to GLG-V-13and KMC-IV-84. No significant prolongation of action potentialduration is observed at cycle lengths of 400 msec or less (P <.05 vs. predrug and washout for paced cycle lengths of 2000 and5000 msec for GLG-V-13 and for paced cycle lengths of 500, 1000,2000 and 5000 msec for KMC-IV-84).

	Discussion

Top Abstract Introduction Methods Results Discussion References

Unlike previous diheterabicyclo[3.3.1]nonane compounds having two secondary amine moieties in the ring system (Scherlag etal., 1988; Patterson et al., 1991; Patterson et al., 1993; Fazekaset al., 1993a; Smith et al., 1990), neither GLG-V-13 nor KMC-IV-84altered conduction in canine myocardium. The electrophysiologicactions of GLG-V-13 and KMC-IV-84 were limited to a rate-dependentprolongation of APD₅₀ and APD₉₀ in canine Purkinje, right ventricularsubendocardium and left ventricular epicardium. Prolongation ofinitial repolarization, as reflected in prolongation of APD₂₅,was observed at higher dosages than those producing prolongationof APD₅₀ or APD₉₀. The present results are consistent with a selectiveinhibition of I_Kr current in canine myocardium. Such an actionhas been reported for GLG-V-13 in preliminary studies using voltageclamping in isolated ventricular myocytes from rabbit hearts (Fazekaset al., 1995). No inhibition of the slow component of the delayedrectifier was observed (I_Ks).

Reverse use-dependence of action potential prolongation. The reverse use-dependence observed with GLG-V-13 and KMC-IV-84 in the present experiments has been previously reported formethanesulfonalide class III drugs such as dofetilide (Gwilt etal., 1991; Jurkiewicz and Sanguinetti, 1993), E-4031 (Wettweret al., 1991), d,l-sotalol (Strauss et al., 1970; Hafner et al.,1988), MK-499 (Baskin and Lynch, 1994; Krafte and Volberg, 1994)and sematilide (Krafte and Volberg, 1994). The actual mechanism(s)for reverse use-dependence is/are controversial. The earliestmechanism for reverse use-dependence of action potential durationwas advanced by Hondeghem and Snyders (1990). Experimental datafrom their laboratory demonstrated a time- and voltage-dependentmodulation of I_k with quinidine. Quinidine primarily reduced time-dependentoutward potassium currents at negative membrane potentials, withblockade of outward potassium currents becoming less pronouncedwith depolarization (Roden et al., 1988). Later data, however,have failed to demonstrate a similar voltage-dependent or use-dependentreversal of I_Kr blockade with either of the methanesulfonalideclass III antiarrhythmic drugs dofetilide (Jurkiewicz and Sanguinetti,1993) and WAY-123,398 (Spinelli et al., 1993). Despite these observations,both dofetilide and WAY-123,398 produce reverse use-dependentprolongation of the action potential (Jurkiewicz and Sanguinetti,1993; Spinelli et al., 1993).

An increase in extracellular potassium increases I_Kr (Sanguinetti and Jurkiewicz, 1992

). Over the physiologic range of K⁺_o, rapid pacing may cause potassium ions to collect extracellularlyin intracellular clefts and may reverse drug-induced inactivationof I_Kr. This explanation would fail to account for the reverseuse-dependence observed in isolated cells in the absence of increasedextracellular potassium.

The slow rate of deactivation of the slow component of the delayed rectifier (I_Ks) in the presence of selective blockade ofI_Kr or in the absence of I_Kr could account for an increased outwardcurrent with rapid HRs (Krafte and Volberg, 1994

). Rapid activationunder conditions minimizing I_k (Ca⁺⁺_o = 0) does not produce reverse use-dependence. When other ioniccurrents are suppressed by E-4031 (I_Kr), nisoldipine (I_Ca-L),glibenclamide (I_K-ATP), and K⁺_o = 0, there is an increase in a slowly developing outward tailcurrent in isolated guinea pig cells (Jurkiewicz and Sanguinetti,1993

). Azimilide and ambasilide, class III agents blocking boththe rapid (I_Kr) and the slow (I_Ks) components of the delayed rectifier,demonstrate less rate-dependence in isolated myocytes and ventricularmuscle than do selective inhibitors of I_Kr (Gintant, 1994

; Zhanget al., 1992

; Takanaka et al., 1992

). The concomitant blockadeof both components of the delayed rectifier and an absence ofreverse use-dependence are consistent with the hypothesis thatslow deactivation of I_Ks accounts for reverse use-dependence.Reverse use-dependence of action potential duration, however,has been reported in isolated myocytes from the cat, a preparationsuggested to lack I_Ks (Spinelli et al., 1993

The rabbit also lacks a primary slow component of delayed rectification (Carmeliet, 1992

). In isolated rabbit ventricularmyocytes, reverse use-dependence of action potential durationwith class III drugs is observed despite the relative absenceof I_Ks (Carmeliet, 1993

). In isolated rabbit ventricular cells,frequency-dependent block of the delayed rectifier (almost exclusivelyI_Kr) may be observed, and the reverse use-dependence of actionpotential prolongation can be attributed to the very slow recoveryof the delayed rectifier from drug-induced block (Carmeliet, 1993

).The bases for the reverse use-dependence of action potential prolongationobserved in past studies with the methanesulfonalides and in thepresent studies using the diheterabicyclo[3.3.1]nonanes GLG-V-13and KMC-IV-84 are unknown.

Antiarrhythmic efficacy. The importance of reverse use-dependence as a determinant of antiarrhythmic activity is unknown. The relative absence of actionpotential prolongation at rapid atrial rates is clearly deleteriousto the suppression of atrial fibrillation (Wang et al., 1994).Atrial fibrillation would not represent an ideal arrhythmia substratefor suppression by GLG-V-13 or KMC-IV-84 or by any class III agentwith marked reverse use-dependence. The role of action potentialprolongation in ischemically injured ventricular tissues constitutinga reentrant pathway as a basis for antiarrhythmic drug efficacyis less well understood. In ischemically injured epicardium duringthe subacute phase of myocardial infarction in the dog, classIII antiarrhythmic drugs produce little action potential prolongation.With clofilium (Patterson et al., 1992), the failure to prolongaction potential duration in vitro is accompanied by an increasein refractoriness within the reentrant pathway in vivo and bypostrepolarization refractoriness in vitro. With d,l-sotalol,little prolongation of action potential duration is observed inmarkedly damaged epicardial tissue examined 4 days after coronaryartery ligation in the dog (Patterson, 1995), despite the presenceof marked postrepolarization refractoriness in injured canineepicardium in vivo after d,l-sotalol administration (Cobbe etal., 1983; Patterson and Scherlag, 1996). GLG-V-13 has demonstratedconduction block and postrepolarization refractoriness in ischemicallyinjured canine epicardium studied 4 to 5 days after anterior coronaryartery ligation. The same experiments have failed to demonstratea significant effect of GLG-V-13 on action potential duration,cellular determinants of conduction velocity or actual conductionvelocity in the same injured epicardial tissue (unpublished datafrom our laboratory). Despite its inability to alter action potentialduration in ischemically injured canine epicardium, GLG-V-13 increasesrefractoriness within injured canine epicardium and suppressesthe induction of sustained ventricular tachycardia (Fazekas etal., 1993b).

Action potential prolongation in left ventricular epicardium associated with GLG-V-13 and KMC-IV-84 administration is reducedby an increase in extracellular potassium ion concentrations.Prolongation of the action potential is observed over the entirerange of paced cycle lengths, but is largest at the long cyclelengths that normally produce the greatest prolongation of theaction potential in normal left ventricular epicardium. The increasein extracellular potassium reduces the potassium ion gradientfor the delayed rectifier and decreases outward current. The lossof membrane potential with an increase in extracellular potassiummay also alter the time-dependent recovery of drug-bound potassiumchannels to the resting state (Carmeliet, 1993

). A local increasein extracellular potassium and a loss of membrane potential couldexplain, in part, the inability of class III antiarrhythmic drugsto prolong action potential duration during acute ischemia (Cobbeand Manley, 1985

) and in ischemically injured canine epicardium(Patterson et al., 1992

; Patterson, 1995

Relationship to other antiarrhythmic agents. The chemical structures and chemical synthesis of GLG-V-13 and KMC-IV-84 were derived from earlier diheterabicyclo[3.3.1]nonaneantiarrhythmic agents (Scherlag et al., 1988; Smith et al., 1990;Bailey et al., 1984). Another diheterabicyclo[3.3.1]nonane classIII antiarrhythmic drug, ambasilide, has been developed and evaluatedindependently. The chemical structure is shown by Takanaka etal. (1992) and Zhang et al. (1992). Although ambasilide producesreverse use-dependence in canine Purkinje tissue, the drug prolongsaction potential duration over a wide range of paced cycle lengthsin canine subendocardium (Takanaka et al., 1992). Ambasilide inhibitsboth components of the delayed rectifier (I_Kr and I_Ks) in isolatedguinea pig myocytes (Zhang et al., 1992). The lack of significantrate-dependence in canine ventricular muscle clearly distinguishesambasilide from its chemical relatives GLG-V-13, KMC-IV-84 andtedisamil.

Tedisamil, a bradycardic agent that prolongs action potential duration in myocardial tissues, has a diheterabicyclononanering structure (Ohler et al., 1994

; Ohler and Ravens, 1994

). Prolongationof action potential duration in ventricular papillary musclesand myocytes of the guinea pig is reverse use-dependent, witha greater prolongation observed at slow HRs (Ohler et al., 1994

;Ohler and Ravens, 1994

), (a result similar to those observed withGLG-V-13 and KMC-IV-84 in the present studies.

Proarrhythmia. The potential of GLG-V-13 and KMC-IV-84 to induce the formation of early afterdepolarizations and bradycardia-dependent ventriculararrhythmia has not been defined. Afterdepolarizations were notobserved in the present experiments. Hypokalemia, acidosis andstimulation of sodium-calcium exchange were not, however, usedin an attempt to provoke potential early formation of afterdepolarization.In a rabbit model of torsades de pointes using alpha adrenergicreceptor stimulation to facilitate arrhythmia formation, GLG-V-13has been shown to facilitate polymorphic ventricular arrhythmiaformation (Fazekas et al., 1993c; Fazekas et al., in press). Ithas been suggested that the proarrhythmic effects of GLG-V-13are slightly less than those observed with other class III drugs(Fazekas et al., 1993c; Fazekas et al., in press, 1997). In lightof their similar ability to prolong the action potential at slowHRs, it is unclear why any one selective inhibitor of I_Kr shoulddemonstrate more or less proarrhythmia from early afterdepolarizationformation.

Conclusion. The present experiments demonstrate the selective class III electrophysiologic actions of the imidazole-substituted diheterabicyclo[3.3.1]nonanedrugs GLG-V-13 and KMC-IV-84 in canine ventricular myocardium.Action potential prolongation in Purkinje, right ventricular subendocardiumand left ventricular epicardium is rate-dependent, and littleprolongation of action potential duration is observed at pacedrates of 3 Hz or greater. The drugs had no effect on V_max or actionpotential amplitude, despite the derivation of the compounds froma diheterabicyclononane structure that has class I antiarrhythmicproperties. The observed pharmacologic effects of GLG-V-13 andKMC-IV-84 are consistent with selective blockade of the rapidphase of the delayed rectifier current in canine myocardium (I_Kr).Further experiments are needed to further define both the antiarrhythmicefficacy and the proarrhythmic potential of GLG-V-13 and KMC-IV-84.

	Footnotes

Accepted for publication December 9, 1996.

Received for publication May 30, 1996.

Send reprint requests to: Eugene Patterson, Ph.D., Research Service 151-F, DVA Medical Center, 921 NE 13th Street, Oklahoma City, OK 73104.

	Abbreviations

MDP, maximum diastolic depolarization; RMP, resting membrane potential; APA, action potential amplitude; OS, overshoot; APD₂₅, action potential duration at 25% of repolarization; APD₅₀, action potential duration at 50% of repolarization; APD₉₀, action potential duration at 90% of repolarization; APD₁₀₀, action potential duration at 100% of repolarization; ERP, effective refractory period; CT, conduction time; CV(L), conduction velocity longitudinal to fiber orientation; CV(T), conduction velocity transverse to fiber orientation.

	References

Top Abstract Introduction Methods Results Discussion References

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