Opposite effects of iv amiodarone on cardiovascular vagal and sympathetic efferent activities in rats

doi:10.1152/ajpregu.00608.2001

Opposite effects of iv amiodarone on cardiovascular vagal and sympathetic efferent activities in rats

Valdo Jose Dias Da Silva¹^,², Tomaso Gnecchi-Ruscone³, Barbara Lavelli¹, Valentina Bellina¹, Daniela Manzella¹^,⁴, Alberto Porta¹, Alberto Malliani¹, and Nicola Montano¹

¹ Dipartimento di Scienze Precliniche, L.I.T.A. di Vialba, Medicina Interna II, Ospedale L. Sacco, Universita' degli Studi di Milano, 20157 Milano, ³ Divisione di Cardiologia, Ospedale S L Mandic, 22055 Merate (LC), ⁴ Dipartimento di Geriatria e Malattie del Metabolismo, Universita' di Napoli II, Napoli, Italy; and ² Department of Biological Sciences, School of Medicine of the Triangulo Mineiro, 38015-050 Uberaba, Brazil

ABSTRACT

TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES

It is unknown whether amiodarone exerts a direct central action on the cardiovascular autonomic nervous system. This studywas designed to evaluate the effects of acute amiodarone administrationon vagal and sympathetic efferent nerve discharges. Experimentswere carried out in 25 decerebrate unanesthetized rats. In onegroup, vagal activity was recorded from preganglionic fibers isolatedfrom the cervical vagus nerve. In another group, sympathetic recordingswere obtained from fibers isolated from the cervical sympathetictrunk in intact conditions or after barodenervation. Recordingswere performed before and for 60 min after amiodarone (50 mg/kgiv) administration. In all groups, amiodarone induced bradycardiaand hypotension. Vagal activity increased immediately, reachinga significant difference after 20 min (260 ± 131% from 16.4 ±3.3 spikes/s) and was unmodified by the barodenervation. At difference,sympathetic activity after an initial and short-lasting increase(150 ± 83% from 24.8 ± 5.7 spikes/s) began to decrease significantlyafter 20 min (36 ± 17%) throughout the experiment. The initialincrease in sympathetic activity was not observed in barodenervatedanimals. These changes in vagal and sympathetic activity couldplay an important role in contributing to the antiarrhythmic actionofamiodarone.

arrhythmias; autonomic nervous system; baroreceptors; heart rate

	INTRODUCTION

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

SUDDEN DEATH represents the major cause of mortality in the Western countries. Sympathetic hyperactivity has been implicatedin triggering life-threatening arrhythmias, while, on the otherhand, vagal activation may partly play a protective role (18,21, 23). Thus a drug characterized by a mechanism of actionable to reduce sympathetic activity and increase vagal activitymight be of great benefit in preventing ventricular fibrillationand tachyarrhythmias. During the past decade, randomized clinicaltrials have investigated the ability of several antiarrhythmicdrugs to reduce sudden death in patients at high risk of arrhythmias(9, 24). Apart from $beta$ -blockers, no other agent has been conclusivelyfound to reduce mortality (25). However, a recent meta-analysis(1) indicated that amiodarone reduces the rate of arrhythmic/suddendeath in high-risk patients with myocardial infarction or congestiveheart failure. Amiodarone is a widely used antiarrhythmic drugthat lowers heart rate, reduces premature ventricular contractions,and prevents ventricular fibrillation (5, 14, 15). Thisaction is likely to occur through several antiarrhythmic mechanisms,such as a Na⁺ channel blockade, Ca²⁺ channel blockade, prolongation of cardiac repolarization andeffective refractory period (13), and a peripheral antiadrenergiceffect (8). However, no information is available on the possibledirect central effects on autonomic neuralmechanisms.

In this study we report that, in decerebrate unanesthetized, spontaneously breathing rats, intravenous amiodarone increasedvagal while reducing sympathetic preganglionic activity. The neuralchanges were associated with bradycardia and hypotension and werestill evident in the absence of baroreflex mechanisms, suggestinga direct effect of this drug on central neural structures. Thesecombined vagotonic and sympatholytic effects may contribute tothe powerful antiarrhythmic action ofamiodarone.

	METHODS

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Experimental Preparation

All experiments were performed according to the Guiding Principles for Research Involving Animals and Human Beings endorsedby the American PhysiologicalSociety.

Experiments were performed on 25 normotensive Sprague-Dawley rats (350-450 g). Rats were anesthetized with intraperitonealinjection of ketamine (80 mg/kg) and xylazine (10 mg/kg). A midlinecervical incision was performed, and both common carotid arterieswere isolated and occluded by ligature. Polyethylene catheters(PE-50) were inserted into the right common carotid artery andthe right femoral vein. The trachea was cannulated (PE-120) usinga T tube that was connected on one side to an end-tidal CO₂ analyzer(Capstar, Stoelting, Ardmore,PA).

Subsequently all rats were placed on a stereotaxic apparatus. A midsagittal incision was performed, and the skull was exposed.After removal of the parietal bones, a bilateral midcolliculartransection was performed and the forebrain was removed by suction.The accuracy of the transection was confirmed by postmortem examination.Decerebration allowed the rest of the experiment to be carriedout without the depressive influence of anesthesia on neuralstructures.

After a xifo-umbilical incision, the aorta and the inferior vena cava were isolated and pneumatic cuffs were placed aroundeach vessel to induce controlled increases (inflation of the aorticcuff) and decreases (inflation of the vena cava cuff) in arterialblood pressure(AP).

All animals were spontaneously breathing with a respiratory rate between 56 and 120 breaths/min and an end-tidal CO₂ between3.5 and 5.5%.

In all animals, electrocardiogram, AP, and endotracheal pressure were recorded. A bipolar electrode was used for neural recordings.All signals were acquired and stored on a personal computer equippedwith an analog-to-digital board at a sampling rate of 12kHz.

Neural Recordings

Vagal recording. The left cervical vagus nerve was isolated from the surrounding tissues and peripherally cut. The nerve sheath was removed,and the nerve was split to isolate vagal cardiovascular preganglionicfibers. Vagal cardioinhibitory fibers were characterized by adischarge synchronized with the expiratory phase of respirationand responsive to baroreflex mechanisms, namely reducing or increasingtheir discharge during, respectively, hypotension or hypertension(3). An example of vagal efferent recording is shown in Fig.1A.

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Fig. 1. A: raw vagal nerve activity (VNA), integrated VNA (int VNA), arterial pressure (AP), and R-R interval (RR) in baseline condition (Control), aortic constriction (AoC), and inferior vena cava constriction (IVCC) in a rat. Increase in AP induced by AoC was associated with increase in VNA and bradycardia. Conversely AP reduction induced by IVCC was associated with a decrease in VNA and tachycardia. B: raw sympathetic nerve activity (SNA) and integrated SNA (int SNA) in a rat. Increase in AP induced by AoC was associated with decrease in SNA and bradycardia. Conversely AP reduction induced by IVCC was associated with an increase in SNA and tachycardia.

Sympathetic recording. The left cervical sympathetic trunk was isolated from the surrounding tissues and peripherally cut. The nerve sheath was removed,and the nerve was split to isolate sympathetic cardiovascularpreganglionic fibers. Sympathetic cardiovascular fibers were characterizedby their response to baroreflex mechanisms, namely reducing orincreasing their discharge during, respectively, hypertensionor hypotension. An example of sympathetic efferent recording isshown in Fig. 1B.

Experimental Protocol

One hour after nerve filament isolation, recordings were continuously performed from 10 min before to 1 h after an intravenousdose of 50 mg/kg (dissolved in 1 ml/kg of vehicle) of amiodarone.Vagal fibers were recorded in rats with intact baroreflex (n =7). In four of seven animals recordings were also performed afterbarodenervation at the end of the experiment. Sympathetic fiberswere recorded in two groups: one with intact baroreflex (n = 8)and the other with barodenervation (n = 5). Barodenervation wasperformed by bilateral section of the aortic depressor nerve andwas confirmed by the absence of reflex changes in autonomic nerveactivities and heart rate after increases or decreases inAP.

Effects of Atropine

To quantify the role of vagal nerve activity in inducing bradycardia, in a separate group of animals (n = 5), atropine (5mg/kg iv) was given 20 min after intravenous administration ofamiodarone. These animals underwent a surgical procedure and experimentalprotocol similar to the one followed in the other groups, includingleft cervical vagus nerve section but no nerve recordings wereperformed.

Data Analysis

The neural signal was fed into a preamplifier (Grass RPS 107, Quincy, MA) and filtered using a 30- to 3,000-Hz bandwidth.A counted neural activity signal was obtained by calculating thenumber of spikes over a temporal basis of 10 ms using an automaticdigital program based on a threshold detection. The thresholdlevel was set to avoid the background noise. This stepwise signalwas filtered at 2 Hz. This procedure does not affect the meanvalue of neural activity but allows us to obtain values per secondadjusted for the heart rate changes. R-R interval, mean AP (MAP),and vagal or sympathetic neural activity were measured at 1 minbefore and 1, 5, 10, 20, 30, 40, 50, and 60 min after intravenousamiodaroneadministration.

Statistical Analysis

Data are expressed as means ± SE. To evaluate the effects of the treatment on repeated measurements of all data, a one-wayANOVA for repeated measures followed by a Tukey's multiple comparisontest was performed using the software SPSS 7.5 for Windows (SPSS,Chicago, IL). Differences were considered significant when P <0.05.

	RESULTS

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Vagal Recordings

Results are summarized in Fig. 2, left. In baseline conditions, the average values of vagal nerve activity, R-R interval,and MAP were, respectively, 16.4 ± 3.3 spikes/s, 150 ± 13 ms,and 113 ± 8 mmHg. Vagal activity was already increased 1 min afteramiodarone administration, reaching a significant difference after20 min (260 ± 131%; P < 0.01) up to the end of the observationperiod. R-R interval underwent an increase that became significantafter 5 min (112 ± 42%; P < 0.01) up to the end of the recordingsession. MAP decreased significantly after the first minute afteramiodarone administration (21 ± 9%; P < 0.01) and remained significantlylower during the rest of the experiment.

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Fig. 2. Left: time course of VNA, R-R interval, and mean arterial pressure (MAP) before and after intravenous amiodarone (indicated by the broken line) recorded in the group of 7 rats. Right: time course of SNA, R-R, interval and MAP before and after intravenous amiodarone recorded in the group of 8 rats. The values are expressed as means ± SE. The marked bradycardia and hypotension induced by amiodarone were associated with a progressive increase of VNA after drug administration that became significant after 20 min. SNA showed an abrupt but transitory increase in SNA followed by a significantly reduction after 20 min. * P < 0.01 vs. baseline.

In four animals in which a barodenervation was performed 60 min after amiodarone administration, vagal activity remained significantlyhigher compared with baseline conditions (325 ± 107%; P < 0.01).

Sympathetic Recordings

Results are summarized in Fig. 2, right. Before amiodarone, the average values of sympathetic nerve activity, R-R interval,and MAP were, respectively, 24.8 ± 5.7 spikes/s, 190 ± 17 ms,and 115 ± 4mmHg.

A short-lasting increase in sympathetic activity was detectable during the first minute after amiodarone administration (158± 83%; P < 0.01) but was soon replaced by a progressive decreasereaching statistical significance at 20 min (36 ± 17%; P < 0.01)and for the rest of the observation period. Despite the increasein sympathetic activity 1 min after amiodarone, the R-R intervalincreased and became significant at 5 min (+61 ± 10%; P < 0.01)up to the end of the experiment. MAP was already significantlydecreased ( $-$ 32 ± 7%; P < 0.01) 1 min after amiodarone administrationand remained significantly lower for the wholeexperiment.

In the group of animals in which barodenervation was performed at the beginning of the experiment (Fig. 3), the initial increasein sympathetic activity was not observed, whereas a decrease innerve activity was similarly present throughout the whole experiment,reaching statistical significance after 20 min (41.1 ± 12%; P< 0.01). The barodenervated group showed no differences at baselinefor MAP while having a higher SNA and R-R interval.

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Fig. 3. Time course of SNA, R-R interval, and MAP before and after intravenous amiodarone recorded in the group of 5 barodenervated animals ( $open circle$ ) compared with the 8 intact animals (

). The values are expressed as means ± SE. The marked bradycardia and hypotension induced by amiodarone were associated with a progressive reduction of SNA that became significant after 20 min. Note the absence of the transitory increase of SNA in barodenervated animals compared with the intact ones. * P < 0.05 vs. baseline. # P < 0.05 barodenervated vs. intact.

Effect of Atropine

In the group of animals in which muscarinic blockade was performed 20 min after amiodarone administration, the drug-inducedbradycardia was reduced by 33 ± 9% (P < 0.05), whereas MAP wasnot significantlyaffected.

	DISCUSSION

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Our study provides the first evidence that amiodarone increases the discharge of vagal efferent fibers while reducing thesympathetic outflow discharge. These autonomic changes were accompaniedby a significant decrease in heart rate and AP and were preservedafter barodenervation, suggesting a central effect of thedrug.

Vagal and sympathetic nerve filaments were likely to include an efferent activity largely participating in cardiovascularneural regulation, according to functional criteria largely acceptedin various human and animal experimental conditions (19).

These data are consistent with previous observations in conscious rats (7) in which, after acute administration of amiodarone,bradycardia and hypotension were associated with a significantincrease in markers of cardiac vagal modulation detected by meansof spectral analysis of heart ratevariability.

The vagal excitation is likely to be due to a direct action of amiodarone on the central autonomic structures rather thanto peripheral reflex mechanisms such as the baroreflex. Indeed,the increase in vagal efferent activity was present despite theconcomitant hypotension, a condition usually associated with areduction in vagal outflow. Moreover, vagal excitation was unaffectedby the barodenervation performed at the end of the experiment.Conversely, a baroreflex mechanism seems involved in the abruptincrease in sympathetic activity in concomitance to AP decreaseobserved 1 min after amiodarone administration, because it wasabolished by the barodenervation procedure. Therefore, this increasein cardiac vagal activity may participate in determining the reductionin heart rate induced by the drug. However, although it has beenreported that amiodarone crosses the blood-brain barrier (22),to our knowledge, no data are available regarding a possible specificsite of action at the central nervous systemlevel.

The bradycardia observed after intravenous amiodarone (14) has been attributed to different mechanisms, including directNa⁺ and Ca²⁺ channel blocking properties that depress the automaticity ofsinus node (10, 13), non-competitive $beta$ -adrenergic blockade,and reserpine-like sympatholytic action (2, 8, 13). Controversialevidence is present in the literature regarding a possible effectof amiodarone on cardiac vagal modulation. Indeed, in vivo studieson muscarinic blockade reported that amiodarone does not affect(2) or slightly reduces (11) vagal modulation, whereas invitro studies indicated that this drug might possess a vagolyticeffect because it is able to block cardiac muscarinic receptors(20) and inhibit the acetylcholine-dependent K⁺ current in atrial cells (4). However, our data seem to demonstratea direct excitatory effect of amiodarone on vagal efferent dischargethat may importantly contribute to the induced bradycardia. Indeed,sinus node muscarinic blockade with atropine was able to increaseheart rate by >30%.

Amiodarone-induced hypotension may be due to a variety of mechanisms such as a vascular sympatholytic effect, probably viaa reserpine-like action (15) or an $alpha$ -adrenergic blocking action(7). In addition, a direct effect on vascular smooth musclecells due to the Ca²⁺ channel blocking properties of the drug (1) should be takeninto account. Moreover, the vehicle per se, containing polysorbate-80,could exert a hypotensive effect (10). However, studies fromour laboratory were not able to show any hypotensive effect ofvehicle containing polysorbate-80 in conscious rats (7).

Study Limitations

A major limitation of our study is that we did not evaluate a dose-response relationship for amiodarone. However, we selecteda dose that has been commonly used in rats to evaluate its cardiovasculareffects (15, 16, 22). Interestingly, in these studies, plasmaticdosing of amiodarone after intravenous injection ranges from ~45µg/ml at the early time to 5 µg/ml at 60 min (22), which isvery similar to that found in humans after an acute dose of intravenousamiodarone (27).

Although we hypothesized a central effect to explain the observed changes in autonomic efferent activities, we did not measureamiodarone brain concentration and distribution. However, amiodaronehas been shown to be detectable in the rat brain and to reachthe highest concentration 20-30 min after intravenous administration(22). Therefore, the timing of brain distribution of amiodaroneseems consistent with the observed modifications in vagal andsympathetic nerve discharges that became significant after 20min of drugadministration.

Clinical Implications

Acute sympathetic excitation acting on a dysfunctional ventricular myocardium has been implicated as a trigger for life-threateningcardiac arrhythmias in patients with coronary artery disease,heart failure, and hypertension (18, 21, 23). Accordingly,increased vagal modulation and enhanced baroreflex sensitivityhave been associated with a reduced risk of life-threatening arrhythmiasand sudden death (21). Pharmacological interventions aimed toreduce the cardiac effect of sympathetic activation and/or toincrease cardiac vagal modulation might have beneficial effectsin preventing cardiac arrhythmias (1, 3, 21). It has beenreported that while vagally mediated paroxysmal atrial fibrillationis preferentially observed in the absence of detectable heartdisease, sympathetically mediated atrial fibrillation is observedin the presence of any heart disease, inducing a vagal withdrawal(26). Lombardi et al. (17) recently described that patientswith early atrial fibrillation recurrences are characterized byan enhanced sympathetic and reduced vagal modulation to the sinusnode, suggesting that an alteration in the sympathovagal balancemay contribute to the electrical remodeling involved in the genesisand maintaining of atrial fibrillation. Within this latter scenario,amiodarone would be a candidate drug to exert beneficial autonomiceffects on theheart.

In conclusion, our data indicate that amiodarone possesses vagotonic and sympatholytic properties. We suggest that these effectsmay contribute to the powerful antiarrhythmic action of acuteamiodaroneadministration.

	ACKNOWLEDGEMENTS

This study was supported by the Ministero dell'Universita' e della Ricerca Scientifica e Tecnologica, COFIN-2000 Grant (toN. Montano and A. Malliani), University of Milan FIRST-2000 Grant(to N. Montano), and Italian Space Agency Grant ASI 336/2000 (toA. Malliani). V. J. Dias da Silva was supported by a postdoctoraltraining grant from Conselho Nacional de Desenvolvimento Cientificoe Technologico-Brazil.

	FOOTNOTES

Address for reprint requests and other correspondence: N. Montano, DiSP LITA di Vialba, Ospedale L. Sacco, via GB Grassi,74, 20157 Milano, Italy (E-mail: Nicola.Montano{at}unimi.it).

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.

May 6, 2002;10.1152/ajpregu.00608.2001

Received 10 October 2001; accepted in final form 24 April 2002.

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