Prevention of ischemic ventricular tachycardia of Purkinje origin: role for {alpha}2-adrenoceptors in Purkinje?

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Prevention of ischemic ventricular tachycardia of Purkinje origin: role for $alpha$ ₂-adrenoceptors in Purkinje?

David O. Arnar, Dezhi Xing, Hon-Chi Lee, and James B. Martins

Division of Cardiovascular Diseases, Department of Internal Medicine, University of Iowa College of Medicine; and Veterans Administration Medical Center, Iowa City, Iowa 52242

ABSTRACT

TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES

Recent studies have shown the presence of postjunctional $alpha$ ₂-adrenergic receptors on canine Purkinje fibers but not musclecells. Stimulation of these receptors results in prolongationof the action potential duration and the Purkinje relative refractoryperiod. We studied the effect of $alpha$ ₂-adrenergic agonists on inducibleischemic ventricular tachycardia (VT) of both Purkinje fiber andmyocardial origin. Open-chest dogs in whom VT was induced withextrastimuli after occlusion of the anterior descending coronaryartery were studied. A mapping system, incorporating Purkinjesignals, characterized the mechanisms of VT. The $alpha$ ₂-adrenergicagonists clonidine (0.5-4.0 µg/kg) or UK 14,304 (4-5 µg/kg) versussaline were given intravenously after reproducibility of induciblesustained monomorphic VT had been demonstrated. Eighteen dogswere given clonidine, eleven of which had focal Purkinje VT. Ofthese 11 dogs, clonidine blocked VT induction in 9 (81.9%) andrendered VT nonsustained in 1 (9.1%), and VT remained induciblein 1 dog (9.1%), although this was focal midmyocardial VT only.In the seven dogs with VT of myocardial origin, six (85.6%) remainedinducible with clonidine, whereas one dog (14.4%) had only nonsustainedVT after clonidine. Of the six dogs, UK 14,304 blocked VT inductionin four (66.6%) and rendered VT nonsustained in one (16.7%), andVT remained inducible in one dog (16.7%). In four dogs with VTof myocardial origin, VT remained inducible. In the eight controldogs that were given saline, focal Purkinje VT was repeatedlyinducible. Pharmacological stimulation of postjunctional $alpha$ ₂-adrenoceptorson Purkinje fibers may selectively prevent induction of VT ofPurkinje fiber origin in the ischemic canineventricle.

ischemia; mapping; autonomics

	INTRODUCTION

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

IN CONTRAST TO THE EFFECTS of $beta$ -adrenergic stimulation and blockade, the role of $alpha$ -adrenergic receptors in the heart is lesswell defined, and the postsynaptic $alpha$ -adrenergic receptors in theheart were thought to be primarily of the $alpha$ ₁-subtype (5, 8).However, recently published studies (4, 13, 14, 22, 23)have demonstrated the presence of postjunctional $alpha$ ₂-adrenergicreceptors in canine cardiac Purkinje fibers but not in the myocardium.Stimulation of these postjunctional $alpha$ ₂-adrenergic receptors resultsin prolongation of the Purkinje relative refractory period (PRRP)in the intact dog (4) and in prolongation of the action potentialduration (APD) in isolated canine Purkinje fibers in vitro (22).The presence of $alpha$ ₂-adrenergic receptors in canine Purkinje fibershas been confirmed by a radioligand binding and autoradiographicstudy (14). The electrophysiological effects of $alpha$ ₂-adrenergicstimulation in isolated Purkinje fibers are abolished after incubationwith pertussis toxin, implying that a pertussis toxin-sensitiveG protein is mediating these effects (22). In isolated Purkinjefibers, concomitant $alpha$ ₂- and $beta$ -adrenergic stimulation preventsthe induction of triggered activity previously inducible under $beta$ -adrenergic stimulation alone (22). These results suggest thatthe $alpha$ ₂-adrenergic effects are mediated through a G protein thatinhibits adenylate cyclase activity, thereby counteracting the $beta$ -adrenergic effects on cAMP production, which has been implicatedto be an important mediator of arrhythmias under conditions ofischemia and reperfusion (15).

The Purkinje system has been suspected of being a site of origin of ventricular arrhythmias occurring in the early ischemicperiod (10). We (1) recently reported that the Purkinje systemmay be importantly involved in the development of spontaneousventricular tachycardia (VT) during acute ischemia in a caninemodel.

This study tested the hypothesis that $alpha$ ₂-adrenergic agonists could prevent the induction of previously inducible VT of Purkinjefiber origin while not affecting VT originating from intramyocardialsites during the first 1-3 h after coronary artery occlusion inthedog.

	METHODS

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Healthy adult mongrel dogs of either gender weighing 18-24 kg were used for these studies. The protocol was approved by theUniversity of Iowa Animal Use and Care Committee and conformedto the guidelines of the American PhysiologicalSociety.

Surgical preparation. Dogs were anesthetized with 500 mg of thiopental sodium and 100-200 mg/kg iv $alpha$ -chloralose as a bolus. Anesthesia was maintainedwith a continuous intravenous infusion of $alpha$ -chloralose dissolvedin polyethylene glycol at 8 mg · kg¹ · h¹. The animals were intubated and ventilated on a ventilator (HarvardApparatus) with settings adjusted to achieve a physiological arterialPCO₂ (25-35 Torr) and to maintain a normal PO₂ (80-150 Torr).NaHCO₃ was infused as necessary to maintain the pH within physiologicalrange (7.30-7.45). The serum electrolytes K⁺ (3.6-5.0 meq/l), Mg²⁺ (1.5-3.0 mg/dl), and Ca²⁺ (8.5-10.5 mg/dl) were periodically measured and were always withinnormal limits. Arterial pressure was continuously monitored viaa femoral arterial line, and the femoral vein was cannulated forinfusion of drugs andsaline.

The heart was exposed through a median sternotomy, and a snare was placed around the left anterior descending coronary arteryimmediately distal to the first septal perforator. After the experiment,the dogs were euthanized by induction of ventricularfibrillation.

Electrophysiological measurements. A bipolar electrode was used to pace the right atrium at two times diastolic threshold with pulses of 2-ms duration at a cyclelength (CL) of 300 ms. The region of the sinus node was permanentlyclamped to control the rate. Surface electrocardiographic leadsII and V5R were continuously monitored. All six limb leads (I,II, III, aVR, aVL, and aVF) and lead V5R were recorded. Ventricularpacing for VT induction was performed from the innermost poleof each of the 16-pole needles placed in three locations (apicalseptum, anterior base, and lateral midwall) outside of the riskzone of the coronary artery occlusion. Cathodal stimuli (2-msduration at 4 times diastolic current of threshold) were appliedto the pacing electrode while the anode was located in the abdominalsubcutaneous tissue. Twenty-one multipolar plunge needles wereinserted into and surrounding the risk zone of the left anteriordescending coronary artery occlusion as described previously indetail (1). Each needle recorded six bipolar electrograms fromcircumferential electrodes made from Teflon-insulated tungstenwires (1 mm apart), enabling recordings from a total of 126 sites.Details regarding the electrodes, including interelectrode andinterbipole spacing, were as recently described (1).

Electrograms were recorded simultaneously on two separate computers: one for the three endocardial-most bipoles, and the otherfor the three epicardial-most bipoles (1). Signals from thethree endocardial-most electrodes were amplified by a gain of100, band-pass filtered between 3 and 1,300 Hz, and sampled at3.2 kHz. The epicardial electrograms were sampled at frequencyof 1 kHz per channel and band-pass filtered at 30-300 Hz. Three-dimensionalactivation maps were constructed from multiplexed signals. Datafrom both acquisition systems were incorporated for the constructionof three-dimensional activation maps with a common surface electrocardiogram(lead V5R) recording pacing spikes, allowing for alignment ofsignals from bothcomputers.

Each needle had 16 unipoles, which were used to select the six optimal bipolar electrograms that were adjusted to maximizethe capability to record Purkinje signals on the endocardial-mostbipole. The adjustment was performed by sequential recordingson a storage oscilloscope for each bipole. A switching box wasutilized to connect the selected bipoles to each amplifier. Thelength of the needles (22 mm, with circumferential electrodescovering the proximal 16 mm of the needle shaft) traversed throughthe left ventricular wall into the left ventricular cavity. Theepicardial-most bipole recorded an electrogram from the epicardium,and subsequent bipoles recorded electrograms sequentially throughthe myocardial wall. The endocardial-most bipole was used to recordPurkinje potentials when they could be identified. Purkinje potentialswere identified at their endocardial location according to previouspublished criteria from this laboratory, including 0.5-mV spikeslasting 1-2 ms, preceding by 1-11 ms the larger and longer musclespike and the surface QRS on the lead recording the earliest activity(1, 3, 4). If a Purkinje potential was not identifiedfor a given electrode, no activation time was marked for the endocardial-mostelectrogram. Activation maps were constructed as described before(1).

Ventricular effective refractory period (VERP) was determined by delivering extrastimuli (Bloom stimulator) after eight pacedcomplexes, with the effective refractory period defined as thelongest interval between the drive pacing (S1) and the first extrastimulus(S2) that did not capture the ventricle. The drive CL was 300ms. VT induction utilized up to four premature stimuli as follows:the first premature stimulus (S2) was fixed at 4 ms longer thanthe VERP, and a second stimulus (S3) was employed at the samecoupling interval. The S3 was shortened in 10-ms decrements untileither VT induction or failure to capture occurred. If no VT wasinduced, the same procedure was followed for the third (S4) andfourth extrastimuli (S5) as required. There was a pause of 1 sbefore the next drive started. The PRRP was defined as the longestS1-S2 that produced a delay in the Purkinje activation but didnot produce a delay of the local muscle activation of the pacingelectrode (3). The PRRP were measured in subsets of five dogsfor each drugused.

For the experiment in which renal sympathetic nerve activity (RSNA) was recorded, the dog's flank was opened, and the hilumof the left kidney was dissected to expose the renal nerves. Thedistal nerve was cut and desheathed, and multifiber recordingswere made utilizing a platinum electrode. The nerve and sheathwere encased in silicone gel. Recordings were made with a high-impedanceprobe with signals filtered over 30 Hz-3 kHz with a HIPS 11J modelGrass instruments recorder (16). Nerve volleys were audiblethrough a loud speaker, and RSNA was quantified by the countingfrequency of action potentials that exceeded a selected voltageset above electrical noise using a nerve traffic analyzer (16).

Definitions. VT was defined as at least three or more premature ventricular complexes in a row. The CL of VTs was averaged over the first10 complexes. VT was considered sustained if it lasted longerthan 30 s or cardioversion was required because of hemodynamiccollapse. Only five VTs were cardioverted; four VTs were reproducedafter cardioversion, so the results were notaffected.

VT was designated to have a focal origin when no electrical activity could be recorded on all adjacent sites in three-dimensionsbetween the latest activation of one QRS complex and the earliestof the next QRS. Moreover, conduction from the site of earliestactivity to adjacent electrodes could not manifest a conductiondelay, which might account for a majority of the CL of theVT.

Purkinje origin of VT was defined as a focal endocardial mechanism with recording of a Purkinje potential before the QRS onthe lead recording the earliest activity to be considered mechanisticallyinvolved. Purkinje potentials had to be identified on electrogramsduring atrial pacing before and after coronary occlusion in additionto the VTrecording.

Mechanisms were defined as reentrant when the earliest activation site was located immediately adjacent to the site of thelatest activation from the previous complex and continuous diastolicactivation was recorded between complexes. Reentrant mechanismsalso demonstrated unidirectional and functional block to the subsequentearliest site ofactivation.

Ischemia was defined as a reduction in voltage of electrograms as described by Ruffy et al. (21) and previously used inthis model (1).

Experimental protocol. A total of 41 dogs were studied. After instrumentation of the risk zone with 21 multipolar plunge needles and before coronaryartery occlusion, induction of VT was attempted with extrastimulito exclude artifactual VT due to electrode instrumentation alone.None of the animals had inducible VT under these circumstances.The left anterior descending coronary artery was then occluded,and VT induction was attempted using serial induction protocolsduring the time period from 1 to 3 h after occlusion. Pacing wasfrom one of three additional electrodes placed outside the riskzone located in locations as described above. No spontaneous sustainedVT or ventricular fibrillation was observed during the periodof 1-3 h after coronary artery occlusion. Although the physiologicalconditions during 3 h of evolving ischemia were not constant,previous studies (2, 25) using this model have demonstratedthat VT is reproducibly inducible over the period of 1-3 h aftercoronaryocclusion.

When VT was induced with extrastimuli, repeat induction was attempted from the same site to ensure reproducibility. If thedogs had morphologically similar inducible VT on at least twoconsecutive attempts from the same pacing site, a drug or salinewas given (a schematic of the protocol is shown in Fig. 1). Theywere given an $alpha$ ₂-agonist, clonidine (0.5-4.0 µg/kg), or UK 14,304(4.0-5.0 µg/kg), as an intravenous infusion over 20 min or saline,and the induction protocol was repeated after 30 min. Five dogsalso had inferior vena caval occlusion to achieve similar changesin arterial pressure as produced by UK 14,304.

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Fig. 1. Schematic of study protocol. VT, ventricular tachycardia; CAO; coronary artery occlusion.

Pharmaceutical agents. Clonidine and $alpha$ -chloralose were purchased from Sigma (St. Louis, MO), and UK 14,304 was purchased from Research Biochemicals(Natick,MA).

Data analysis. All data are expressed as means ± SE. Fisher's exact test was used to test differences in inducibility with pharmacologicalintervention between groups receiving $alpha$ ₂-adrenergic agonists andthe control group. A Student's t-test was used for comparisonof mean arterial pressures (MAP) and refractory periods beforeand after drug administration and for comparison of drug doses.A P value of <0.05 was considered statisticallysignificant.

	RESULTS

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Of 41 dogs studied with reproducibly inducible sustained monomorphic VT, 18 were given clonidine, 10 were given UK 14,304,and 8 dogs were given saline and served as a control group forrepeated inducibility over the period of 1-3 h after coronaryartery occlusion. An additional five dogs served as controls forhypotensive effects of $alpha$ ₂-adrenergic agents. The mean CL of allVTs was 135 ± 3 ms; VT with Purkinje origin had a CL of 136 ±3 ms, and all other VTs had a mean CL of 132 ± 2 ms [P = not significant(NS)]. The mean number of Purkinje signals observed in the endocardial-mostlayer in all dogs was 9 ± 0.5 (range 4-15) of 21electrodes.

Mechanisms and origin of inducible VTs. Twenty-five of thirty-six (69.4%) VTs were of focal Purkinje origin (Table 1). An example of the focal Purkinje VT is shownon the electrogram in Fig. 2. A drive is followed by three extrastimuliand induction of VT. The VT complexes are preceded by Purkinjespikes, indicating that the earliest site of activity during theseis in the Purkinje system. Figure 3 shows an activation map forthe first VT complex. The earliest activity seen is in the Purkinjelayer, and subsequent activation proceeds away from this sitein all directions without any evidence of conduction delay, indicatinga focal origin of this complex. The other 11 VTs were of eitherfocal epicardial or reentrant mechanisms (Table 1 and Figs. 4and 5).

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Table 1. Mechanisms and sites of origin of VTs inducible at baseline

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Fig. 2. Electrograms showing induction of VT of focal Purkinje fiber origin. The last complex of a drive followed by 3 extrastimuli (downward arrows) result in induction of VT, of which the first 4 complexes are shown. Electrogram focus-endocardium (F-EN) was recorded from the site that was subsequently shown to be the focus of origin of this VT. Other electrograms are from sites immediately adjacent to the focus, with north-endocardium (N-EN) located towards the base of the heart and with others [east-endocardium (E-EN), extreme east-endocardium (EE-EN), south-endocardium (S-EN), southwest-endocardium (SW-EN), and northwest-endocardium (NW-EN)] located accordingly. Electrogram O-EN was recorded from the site immediately overlying the focus. Also shown (top of tracing) are surface electrograms II and V₃R. During the first VT complex, a Purkinje potential (upward arrows) precedes the onset of the surface QRS complex (vertical line), suggesting that the Purkinje fiber is the earliest site of electrical activity. The surrounding myocardium is activated subsequently. The same pattern is also seen in subsequent VT complexes.

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Fig. 3. Activation map of the first VT complex shown in Fig. 2. Each rectangle represents a layer in the anterior wall of the heart extending from epicardium (Epi) through to Purkinje (Purk) fiber. Activation is shown with 20-ms isochrones. Colors are indicative of different isochrones with yellow first and then red, green, and blue last. The earliest activity during this complex is seen in the Purkinje layer ( $-$ 14 m), consistent with the observations of the electrogram in Fig. 2. This indicates the onset of electrical activity in the Purkinje layer 14 ms before the onset of the surface QRS. The activation spreads out from this focus of origin to surrounding areas without evidence of a conduction delay, suggesting a focal origin. Activation then proceeds transmurally to the epicardium, where the last activity is seen (56 ms). S-Epi, subepicardium; Endo, endocardium; S-Endo, subendocardium.

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Fig. 4. This figure shows surface leads II and V₃R and epicardial bipolar (EP) electrograms from a remote (R) pacing site and northwest (NW), southwest (SW), north (N), south (S), east (E) sites and surrounding a focus (F) site and underling the focus (U) site. All intracardiac electrograms are at the same amplification. Similar to Fig. 2, extrastimuli produced VT with a focus (upward arrows).

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Fig. 5. Activation map of the first VT complex shown in Fig. 4. Orientation is similar to that of Fig. 3; earliest activity during this complex is seen in the epicardial layer ( $-$ 31 ms) with surrounding activation suggesting a focal origin in the epicardium. There is retrograde activation from epicardium to Purkinje fibers in nearly all sites. This pattern is exactly opposite of that of the activations shown in Fig. 2.

Effect of $alpha$ ₂-adrenergic agonists on inducible VTs. Of the 18 dogs given clonidine, 11 had focal Purkinje VT. VT induction was completely blocked in nine dogs (81.8%), whereasin one dog (9.1%) only nonsustained Purkinje VT was inducible(P < 0.0005 compared with control group). The mean dose of clonidinewas 1.9 ± 0.3 µg/kg. One dog (9.1%) continued to have inducibleVT after clonidine (2 µg/kg) administration but with a midmyocardialfocal origin only, whereas only Purkinje VT was inducible before,but not after, clonidine administration. Of the three dogs withintramyocardial macroreentrant VT, all continued to have inducibleVT after clonidine. Likewise, of the four dogs with epicardialfocal VT, all remained to have inducible VT on clonidine administration(mean dose 1.9 ± 0.6 µg/kg, P = NS compared with dose that preventedfocal Purkinje VT), although in one dog only nonsustained VT wasinduced after clonidine. After clonidine administration, MAP decreasedfrom 85 ± 4 to 80 ± 4 mmHg (P < 0.05), although the VERP (from137 ± 7 to 137 ± 4 ms) did not change (P = NS) (Table 2). ThePRRP in a subset of the dogs given clonidine (n = 5) prolongedfrom 179 ± 9 to 182 ± 6 ms (P < 0.05), indicating a specific effectof the drug on postjunctional $alpha$ ₂-adrenergic receptors on Purkinjefibers.

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Table 2. Effects of $alpha$ ₂-adrenergic agonists on MAP, VERP, and PRRP

Of the 10 dogs given the $alpha$ ₂-adrenergic agonist UK 14,304, 6 had inducible focal Purkinje VT before receiving the drug. VTinduction was prevented in four (66.6%) of these and renderednonsustained in one dog (16.7%) (P < 0.005 compared with controlgroup) after UK 14,304 (mean dose 4.4 ± 0.9 µg/kg) administration.VT originating in the Purkinje fibers was inducible in only onedog (16.7%) after UK 14304 administration (4 µg/kg). In two offour dogs in which induction of Purkinje VT was prevented by UK14,304, VTs with focal midwall origin were inducible only afterUK 14,304 was given. In four dogs with VT of epicardial origin(3 reentrant and 1 focal), UK 14,304 (mean dose 4.5 ± 1.0 µg/kg,P = NS compared with dose that prevented focal Purkinje VT) didnot affect VT inducibility. After UK 14,304 administration, MAPdecreased from 104 ± 10 to 65 ± 11 mmHg (P < 0.05), and VERP wasunchanged (141 ± 5 to 142 ± 5 ms, P = NS), but PRRP increasedfrom 175 ± 6 to 181 ± 4 ms (P < 0.05), indicating an $alpha$ ₂ -adrenergicreceptor effect in Purkinje fibers (Table 2).

When the results of the effects of both $alpha$ ₂-agonists on inducible VT are combined, they were effective in preventing focalPurkinje VT in 13 of 17 dogs (76.4%), partially effective (sustainedto nonsustained VT) in 2 dogs (11.8%), and not effective in 2dogs (11.8%). VTs with epicardial focal or reentrant mechanismswere not affected by the $alpha$ ₂-adrenergic agonists in 10 of 11 dogs(90.1%), and in 1 of 11 dogs (9.9%) nonsustained VT was inducibleafter the $alpha$ ₂-adrenergic agonist was given. These combined resultsprovide further support that the $alpha$ ₂-adrenergic agonists may preferentiallymodulate only VTs of Purkinje fiber origin. Neither clonidine(54 ± 4% to 56 ± 3%, P = NS) nor UK 14,304 (61 ± 4 to 62 ± 4%,P = NS) had an effect on the size of the ischemic zone, expressedas the percentage of electrodes exhibiting voltage changes consistentwithischemia.

Observations from an experiment with RSNA recordings during the use of clonidine in doses from 0.5-8.0 µg/kg is shown in Fig.6. With the doses of clonidine used for arrhythmia preventionin this study, no reduction in RSNA was seen. On the other hand,an increase in RSNA was seen with doses of 0.5 and 2.0 µg/kg.Only a mild decrease was seen in MAP with a dose increase from0.5 to 2.0 µg/kg. With a dose of 8.0 µg/kg, a decrease in MAPwas seen and a lesser increase in the RSNA occurred, which maybe consistent with the initiation of a central sympathoinhibitoryeffect of clonidine at that dose. This suggests that the dosesused in this study may not have caused significant central inhibitionof sympathetic tone.

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Fig. 6. Effect of escalating doses of clonidine (0.5-8.0 µg/kg iv) on renal sympathetic nerve activity (SNA). With the doses used for prevention of VT in this study, the renal SNA increased slightly, consistent with a lack of decrease in central sympathetic outflow. Only at 8 µg/kg is there a lesser increase in renal SNA than seen with the increase in dosage from 0.5 to 2.0 µg/kg, suggesting that at 8 µg/kg clonidine began to have an inhibitory effect on sympathetic outflow from the central nervous system.

Five dogs had inferior vena caval occlusion, which dropped MAP from 114 ± 9 to 78 ± 2 mmHg, (P < 0.05), similar to the changein pressure produced by UK 14,304. However, Purkinje VT was stillinduced in each, and the CL of VT was unchanged from 151 ± 14to 154 ± 16 ms (P = NS). VERP was also unchanged from 145 ± 6to 146 ± 6 ms (P = NS). Thus mechanical alterations of fillingand arterial pressure produced no change in Purkinje VT, suggestingthat receptor-specific effects of $alpha$ ₂-agonists on Purkinje tissuewere responsible for alterations in inducibility of VT by UK 14,304.

Control group. Eight dogs with focal Purkinje VT were not given an $alpha$ ₂-adrenergic agonist but served as controls for repeated inducibilityover the time course of the study. All eight dogs had reproducibleinducible VT with the same origin over time. In these dogs, bothMAP [from 109 ± 8 to 115 ± 9 mmHg (P = NS)] and VERP [from 146± 6 to 143 ± 7 ms (P = NS)] were stable over the time course ofrepeatedinducibility.

	DISCUSSION

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

The results of this study indicate that inducible ischemic VT of Purkinje fiber origin appears to be susceptible to selectivemodulation by pharmaceutical agents that stimulate the postjunctional $alpha$ ₂-adrenergic receptor on Purkinje tissue. The $alpha$ ₂-adrenergticagonists clonidine and UK 14,304 were both effective in preventinginduction of previously inducible VT of Purkinje fiber originonly while most of the inducible VT originating in the ventricularmyocardium was not affected by $alpha$ ₂-adrenergic agonists. In addition,PRRP was increased, but no change was noted in the VERP, and adecrease in RSNA was not seen with the doses of clonidine usedfor VT modulation. Finally, mechanically induced reduction ofarterial pressure similar to that produced by an $alpha$ ₂-agonist producedno effect on Purkinje VT. These novel findings suggest an functionallyimportant role for the postjunctional $alpha$ ₂-adrenergic receptorsrecently described on canine Purkinjefibers.

$alpha$ ₂-Adrenergic receptors on Purkinje fibers. The existence of postjunctional $alpha$ ₂-adrenergic receptors was first suggested in a report by Mugelli et al. (19), who demonstratedthat changes in automaticity in sheep Purkinje fibers exposedto norepinephrine under conditions of hypoxia were blocked byyohimbine but not $alpha$ ₁- or $beta$ -adrenergic blockers. Earlier, Rosenet al. (20) reported that clonidine decreased automaticity inisolated dog Purkinje fibers but, because these effects were notblocked by yohimbine, they were attributed to direct effects.Cable et al. (4) later showed in an intact dog model that $alpha$ ₂-adrenergicstimulation prolonged the PRRP selectively without any effecton the VERP and that these effects were attenuated by yohimbine.A subsequent study (22) utilizing standard microelectrode techniquesin isolated superfused Purkinje fibers showed that $alpha$ ₂-adrenergicstimulation, both with norepinephrine in the presence of propranololand prazosin and UK 14,304, prolonged the APD. These effects werealso reversed by yohimbine, suggesting $alpha$ ₂-adrenergic receptorspecificity. Further studies have shown that the effects of $alpha$ ₂-adrenergicagonist on APD were intact in the presence of blockers of theion channels of inward rectifying and slow rectifying K⁺ currents, Cl current, and Ca²⁺ currents but were abolished in the presence of 4-aminopyridine,a blocker of transient outward K⁺ current (I_to). These results are suggestive of I_to being a majormediator of modulation of the APD of $alpha$ ₂-adrenoceptor agonists(13).

The APD of Purkinje fibers that had been incubated with pertussis toxin was not prolonged with $alpha$ ₂-adrenergic agonists, indicatingthat the $alpha$ ₂-adrenergic effects in Purkinje fibers are mediatedthrough a pertussis toxin-sensitive G protein, likely G_i (22).The $alpha$ ₂-adrenergic receptor coupling to G_i, which inhibits adenylatecyclase and cAMP production, could therefore potentially counteractsome of the arrhythmogenic effects of excess $beta$ -adrenergic stimulation.Sustained triggered activity, which was inducible in isolatedPurkinje fibers under conditions of elevated extracellular calciumand unopposed $beta$ -adrenergic stimulation, could be suppressed inthe presence of concomitant $beta$ - and $alpha$ ₂-adrenergic stimulation (22).

This constitutes the basis of the hypothesis that $alpha$ ₂-adrenergic effects may have an antiarrhythmic effect on those arrhythmiasthat originate from the His-Purkinje system and are induced duringthe setting of enhanced sympathetic tone, such as in acute ischemia/infarction.

Effects of $alpha$ ₂-adrenergic agents on inducible VT. The results of this study strongly suggest that $alpha$ ₂-adrenergic agents selectively modulate VT of focal Purkinje fiber origin,whereas focal and macroreentrant VT with origin in the myocardiumwere not affected. In addition to the postjunctional receptormediated $alpha$ ₂-adrenergic stimulation, clonidine is known to haveother pharmacological effects, including stimulation of the centralnervous system (CNS) imidazoline receptors (26) and all $alpha$ ₂-adrenergicagonists have an effect on central or prejunctional $alpha$ ₂-adrenergicreceptors and, through these, may modulate the sympathetic nervoussystem output from the CNS, resulting in decreased peripheralsympathetic tone. Presynaptically, clonidine may inhibit norepinephrinerelease from nerve terminals (26). We performed an experimentin which RSNA was recorded during infusion of clonidine in dosesfrom 0.5 to 8.0 µg/kg. No decrease in RSNA was seen, indicatinga lack of inhibition of central sympathetic outflow by clonidinein the doses used in this study. Hence, the modulation of VT inductionby clonidine and UK 14,304 can be attributed to their effectson postjunctional $alpha$ ₂-adrenergic receptors in cardiac Purkinjetissue.

Administration of both $alpha$ ₂-adrenergic agonists used in this study resulted in a decrease in MAP. MAP fell modestly in responseto clonidine and substantially in response to UK 14,304. The effectsof UK 14,304 in vivo have not been well characterized. It is aselective $alpha$ ₂-adrenergic agonist and has predominately been usedas a tool in experimental pharmacology. In a previous study (9)involving a similar model in our laboratory, a decrease in MAPof up to 50 mmHg did not affect the inducibility of VT, althoughtransmural activation times and the rate of VT were affected.In the present study, a similar decrease in MAP, produced by inferiorvena caval ligation, had no effect on VT inducibility. Kabellet al. (11), however, reported that blood pressure may affectfocal arrhythmias arising in ischemically injured hearts, albeit>24 h later. It cannot be completely ruled out that some degreeof modulation of central sympathetic outflow may have occurredwith administration of the $alpha$ ₂-adrenergic agonists because a direct $alpha$ ₂-adrenergic effect on vascular smooth muscle results in vasoconstriction.However, if inhibition of central sympathetic outflow was a significantmechanism in suppressing inducible VT in this study, both VT fromintramyocardial sites and VT originating from Purkinje fiberswould have been expected to be affected approximately equally,which was not the case. Our results, showing that induction ofPurkinje VT was selectively inhibited, whereas VT from intramyocardialsites were not suppressed by UK 14,304, further indicate a lackof effect in the ventricular myocardium. VERP was not affectedby either $alpha$ ₂-adrenergic agonist, indicating minimal or no prejunctionaleffect at the doses given, because prejunctional $alpha$ ₂-adrenergicstimulation would be expected to increase the VERP by inhibitingnorepinephrine release (18). Both clonidine and UK 14,304 increasedthe PRRP in a nonselected subgroup of animals, consistent witha direct postjunctional effect on $alpha$ ₂-adrenoceptors on Purkinjefibers.

On the basis of the results of this study, we speculate that a major function of the postjunctional $alpha$ ₂-adrenergic receptorson Purkinje fibers is to counterbalance the effects of $beta$ -adrenergicstimulation by inhibition of cAMP production, which may be animportant mediator of arrhythmogenesis duringischemia.

VT of Purkinje fiber origin. Previous studies (1, 17) from this laboratory have shown that the Purkinje system may be involved in the genesis of bothspontaneous and inducible VT during acute ischemia. In the presentstudy, we examined the effects of $alpha$ ₂-adrenergic modulation oninducible VT because reproducibility was important to assess theeffects of the pharmacologicalintervention.

Recording of Purkinje signals in this model is facilitated by long needles traversing the myocardium into the ventricularcavity, circumferential electrodes and the electrograms were carefullyanalyzed for Purkinjespikes.

The underlying mechanism of the inducible focal VTs in this study is not entirely clear, and the methodology does not allowfor delineation of the exact mechanism of focal VTs. Given thespacing between needles of ~10 mm, the possibility of microreentryas a mechanism of some of the focal VTs cannot be totally ruledout. However, no significant conduction delay was seen surroundingthe earliest site of origin of the focal VTs in this study, anda group of dogs studied later demonstrated lack of typical entrainmentfor inducible focal Purkinje VT, further suggesting alternativemechanisms than reentry (17). Abnormal automaticity can be ruledout as an etiological factor in this study because this arrhythmiais not inducible by programmed extra stimulation. Triggered activitydue to delayed afterdepolarizations is a possible mechanism, whereasearly afterdepolarizations are less likely to play a role, becausetheir occurrence is bradycardia dependent and, in the presentexperiments, VT was induced during ventricular pacing at a pacedCL of 300ms.

VT of Purkinje fiber origin has been implicated to occur in some tachycardias in humans. Both idiopathic left ventriculartachycardia and bundle branch macroreentrant VT may importantlyinvolve the Purkinje system (6, 12). While a role for Purkinjetissue has not been proven in VT associated with ischemia in humans,it is certainly possible that Purkinje tissue may be involvedin the development of ischemic ventricular arrhythmias as hasbeen suggested in experimental animal models (1, 10).

Limitations. A major limitation to these observations is that the drugs used in this study, UK 14,304 and especially clonidine, both havea variety of effects, although common to both are $alpha$ ₂-adrenergicagonist effects. Effects on sites outside of Purkinje fibers likelyoccurred during this study as seen by the effects of the decreasein MAP. Both drugs can cross the blood-brain barrier and influence $alpha$ ₂-adrenergic receptors in the CNS. Clonidine can also stimulateimidazoline receptors in the CNS. Ideally, a study like this presentone would be performed using an $alpha$ ₂-adrenergic agonist that doesnot cross the blood-brain barrier. We are, however, not awareof an $alpha$ ₂-adrenergic agonist with such properties. The selectiveeffects on Purkinje VT and increase in the PRRP seen along withlack of effect on VERP are consistent with a drug effect directlyon the $alpha$ ₂-adrenergic receptors on Purkinje fibers. An experimentwhere RSNA was recorded with doses of clonidine used in this studyrevealed no decrease in central sympathetic outflow with the dosesused in thisstudy.

Alternatively, eliminating the involvement of the autonomic nervous system might have been helpful because this would havenegated any reflex-dependent increase in sympathetic input tothe heart. However, we (7) observed in this model that thissignificantly alters VT inducibility and, therefore, denervationwas notundertaken.

The model used for these studies involves open-chest dogs with myocardial ischemia/infarction. This model is generally stablefor up to 3 h after coronary artery occlusion. Thereafter, deteriorationin the animal and alterations in arrhythmia inducibility may occur.This somewhat limits the time frame of the study and makes thepossibility of administrating selective $alpha$ ₂-adrenergic antagoniststo confirm $alpha$ ₂-adrenergic selectivity of the actions of clonidineand UK 14,304, after giving and testing for VT with an $alpha$ ₂-adrenergicagonist, moredifficult.

The mechanisms of the actions of the $alpha$ ₂-adrenergic agonists were not studied. However, previous studies from this group havesuggested a possible mechanism. Samson et al. (22) suggestedthat the $alpha$ ₂-adrenoceptors on Purkinje fibers are coupled to apertussis toxin-sensitive G protein. Another recent study (23)investigated the effects of $beta$ - and $alpha$ ₂-adrenergic stimulation onPurkinje fiber contraction. The strength of Purkinje fiber contractionwas enhanced by isoproterenol, forskolin, and 8-bromo-cAMP. $alpha$ ₂-Adrenergicstimulation with UK 14,304 reversed the effects of isoproterenoland forskolin but not 8-bromo-cAMP, further suggesting that $alpha$ ₂-adrenoceptorson Purkinje fibers are coupled to a pertussis toxin-sensitiveG-protein, likely G_i.

As discussed previously, it is unknown whether VT of Purkinje fiber origin occurs during acute ischemia in humans. It is alsounclear at present whether $alpha$ ₂-adrenoceptors exist on human Purkinjefibers as they appear to on canine Purkinje fibers. This awaitsfurther examination. Thus although the results of this study areintriguing and suggest a potential antiarrhythmic role for $alpha$ ₂-adrenoceptorsin canine Purkinje fibers, these results should not presentlybe extrapolated tohumans.

In conclusion, the results of this study suggest that pharmacological stimulation of $alpha$ ₂-adrenoceptors on Purkinje fibers mayselectively prevent induction of VT originating in this tissueunder ischemic conditions in a canine model. This may indicatean important role for these $alpha$ ₂-adrenoceptors recently describedin canine Purkinjefibers.

	ACKNOWLEDGEMENTS

The authors thank Dr. Mark Chapleau for technical assistance and Linda Bang for expert secretarialassistance.

	FOOTNOTES

This work was supported by grants from the American Heart Association, Iowa Affiliate, and the Veterans Administration MedicalCenter. Dr. Arnar was supported by a Fellowship Award from theAmerican Heart Association, IowaAffiliate.

Address for reprint requests and other correspondence: J. B. Martins, Div. of Cardiovascular Diseases, Dept. of Internal Medicine,Univ. of Iowa College of Medicine, 200 Hawkins Dr., Iowa City,IA 52242 (E-mail: james-martins{at}uiowa.edu).

The costs of publication of this article were defrayed in part by the payment of page charges. The article must thereforebe hereby marked "advertisement" in accordance with 18 U.S.C.Section 1734 solely to indicate thisfact.

Received 19 July 1999; accepted in final form 25 October 2000.

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Am J Physiol Heart Circ Physiol 280(3):H1182-H1190

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Prevention of ischemic ventricular tachycardia of Purkinje origin: role for 2-adrenoceptors in Purkinje?

Prevention of ischemic ventricular tachycardia of Purkinje origin: role for $alpha$ ₂-adrenoceptors in Purkinje?