Intraoperative arrhythmias and tissue damage during transmyocardial laser revascularization

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Intraoperative arrhythmias and tissue damage during transmyocardial laser revascularization

Kamuran A. Kadipasaoglu, PhD^a, Michele Sartori, MD^b, Takafumi Masai, MD^a, Hasan B. Cihan, MD^a, Fred J. Clubb, Jr, DVM, PhD^c, Jeff L. Conger, BS^a, O.H. Frazier, MD^d

^a Cullen Cardiovascular Research Laboratories, Texas Heart Institute/St. Luke’s Episcopal Hospital, Houston, Texas, USA
^b Department of Adult Cardiology, Texas Heart Institute/St. Luke’s Episcopal Hospital, Houston, Texas, USA
^c Department of Cardiovascular Pathology, Texas Heart Institute/St. Luke’s Episcopal Hospital, Houston, Texas, USA
^d Department of Cardiovascular Surgery, Texas Heart Institute, St. Luke’s Episcopal Hospital, Houston, Texas, USA

Accepted for publication June 30, 1998.

Address reprint requests to Dr Kadipasaoglu, Texas Heart Institute, MC 1-268, PO Box 20345, Houston, TX 77225-0345
e-mail: kkadison{at}biost1.thi.tmc.edu

Abstract

Top
Abstract
Introduction
Material and methods
Results
Comment
Acknowledgments
References

Background. Transmyocardial laser revascularization createstransmural channels to improve myocardial perfusion. Differentlaser sources and ablation modalities have been proposed fortransmyocardial laser revascularization. We investigated theincidence of cardiac arrhythmias and laser–tissue interactionsduring transmyocardial laser revascularization of normal porcinemyocardium with three different lasers.

Methods. We used a continuous-wave, chopped CO₂ laser (20 J/pulse,15 ms/pulse) synchronized with the R wave; a holmium:yttriumaluminum garnet (Ho:YAG) laser (2 J/pulse, 250 µs/pulse,5 Hz); and a xenon-chloride (excimer, Xe:Cl) laser (35 mJ/pulse,20 ns/pulse, 30 Hz). Each laser was used 30 times as the solemodality in four consecutive pigs, yielding 120 channels.

Results. The average number of pulses needed to create a channelwas 1, 11 ± 4, and 37 ± 8 for the CO₂, Ho:YAG,and Xe:Cl lasers, respectively. All Ho:YAG and Xe:Cl channelshad premature ventricular contractions. Ventricular tachycardiaoccurred in 70% of the Xe:Cl and 60% of the Ho:YAG channels.Only 36% of the CO₂ channels had premature ventricular contractions,and only 3% of the CO₂ channels had ventricular tachycardia(p < 0.001 versus Ho:YAG and Xe:Cl). Ho:YAG channels werehighly irregular: each had a 0.6-mm-wide central zone surroundedby a ring of coagulation necrosis (diameter, 1.84 ± 0.67mm) with effaced cellular architecture in a thin hemorrhagiczone. The Xe:Cl sections exhibited the same patterns on a smallerscale (diameter, 0.74 ± 0.18 mm). The CO₂ channels werestraight and well demarcated. The zone of structural and thermaldamage extended over half the channel’s diameter, measuring0.52 ± 0.25 mm.

Conclusions. During transmyocardial laser revascularization,the CO₂ laser synchronized with the R wave is significantlyless arrhythmogenic than the Ho:YAG and Xe:Cl lasers not synchronizedwith the R wave. In addition, the interaction of the CO₂ laserwith porcine cardiac tissue is significantly less traumaticthan that of the Ho:YAG and the Xe:Cl lasers.

Introduction

Top
Abstract
Introduction
Material and methods
Results
Comment
Acknowledgments
References

Transmyocardial laser revascularization (TMLR) is a relativelynew surgical technique in which transmural channels are createdto increase myocardial perfusion. The technique is undergoingclinical investigation for safety and long-term efficacy. Inpreliminary trials, TMLR with a high-energy carbon dioxide (CO₂)laser (Heart Laser, PLC Medical Systems, Franklin, MA) has beenused as sole therapy for patients with refractory angina. ByJuly 1998, more than 500 such patients had been enrolled inrandomized and nonrandomized protocols, with encouraging resultsof clinical and cardiac perfusional improvement [1].

Despite the apparent clinical benefit of TMLR, some acute aspectsof the technique, pertaining to its application and biologictissue interaction, require further investigation. First, thearrhythmogenicity associated with irradiation of cardiac tissueat various intervals during the cardiac cycle has not been systematicallyinvestigated. Empirical observations during early animal experimentshave suggested that if the laser is activated during repolarizationof the myocardial cells (ie, during the T wave), the incidenceof arrhythmic disturbances is increased, leading to an adverseoutcome [2]. The arrhythmogenicity of the laser when fired duringthe T wave could be relevant to the choice of the laser sourceand the laser’s radiation pattern. Because the ablationspeed in cardiovascular tissue is directly proportional to thepulse energy [3, 4], a laser with a sufficiently high pulseenergy can create a channel with a single pulse. If this pulseis synchronized so as not to coincide with the T wave, arrhythmogenicitymay be circumvented. At lower pulse energies (lower ablationspeeds), however, delivery of multiple continuous pulse trainsbecomes necessary to create a TMLR channel. Because a numberof these pulses will coincide with the T wave, arrhythmogenicitycould become important. Thus, researchers need to determinewhether multiple-pulse TMLR without electrocardiographic synchronizationhas a harmful effect on the electrical activity of the ventricle.

Another aspect of TMLR involves the effect of laser-inducedacute tissue damage on the long-term patency of the channels.Early experiments in which channels were bored by means of needleacupuncture suggested that channel occlusion by scar tissuewas caused by an extensive fibrous reaction secondary to mechanicaldamage [5]. More recent research into basic laser–tissueinteractions has shown that the mechanical component, measuredas acoustic tissue damage, increases in direct proportion tothe peak power of the laser source [6]. The peak power of thelaser pulse, defined as the laser energy delivered per unittime, increases significantly with a decreasing pulse duration.Therefore, with short-pulse lasers, the duration of the laserpulse may be one of the major determinants of the degree ofinitial tissue trauma and, hence, of the long-term patency ofthe laser channels.

Thus, an analysis of the relative arrhythmogenicity and trauma-inducingpotential of various laser sources currently available for TMLRwould be important, because it could affect perioperative arrhythmiccomplications and increase long-term efficacy. In the presentstudy, we assessed the incidence of arrhythmias and the amountof tissue damage associated with three different lasers duringTMLR in normal porcine hearts: the high-energy, long-pulse CO₂laser and the low-energy, short-pulse holmium:yttrium aluminumgarnet (Ho:YAG) and xenon-chloride (excimer, Xe:Cl) lasers.

Material and methods

Top
Abstract
Introduction
Material and methods
Results
Comment
Acknowledgments
References

All animals at the Texas Heart Institute receive humane carein compliance with the Animal Welfare Act, the "Principles ofLaboratory Animal Care," formulated by the National Societyfor Medical Research, and the "Guide for the Care and Use ofLaboratory Animals" (NIH publication 85-23, revised 1996). Allprotocols related to this program were approved by our hospital’sinstitutional animal care and use committee before the studieswere initiated.

Animal preparation, surgery, and instrumentation
Domestic pigs weighing approximately 56.2 to 67.5 kg were acclimatizedand quarantined for at least 1 week before undergoing surgicalintervention. After the animals had fasted overnight, a preanestheticregimen was induced with acepromazine maleate (0.11 to 0.22mg/kg intramuscularly, not exceeding a total dose of 15 mg)and atropine sulfate (0.05 mg/kg intramuscularly, premixed inthe syringe). An ear vein was catheterized, and general anesthesiawith ketamine hydrochloride (20 mg/kg intravenously) was started10 minutes after the preanesthetic injection. The animals werethen intubated, and anesthesia was maintained throughout theoperation by means of an isoflurane and oxygen mixture.

Each animal was positioned on its right side on an electrocoagulationelectrode and a warming blanket to maintain its body temperatureat 41°C. The body temperature was monitored nasally. Surfaceelectrocardiographic electrodes were applied, and the electrocardiographicwaveform during and after the laser procedure was recorded ona computerized data collection and analysis system (Dataflow;Crystal Biotech, Northborough, MA). Intravenous catheters wereplaced in the left jugular vein for further infusion of medicationsand in the carotid artery for monitoring the arterial pressure.A left thoracotomy was performed in the fourth intercostal space.The pericardium was exposed and cut in a T shape, and the heartwas isolated in a pericardial cradle. To prevent muscle spasms,pancuronium bromide (0.1 mg/kg intravenously) was given forone time only. After creation of the laser channels, the experimentwas terminated by injecting the unconscious animal intravenouslywith a euthanizing agent (Beuthanasia solution Delmarva LaboratoriesInc, Midlothian, VA).

Transmyocardial laser revascularization modalities
We used a high-energy CO₂ laser (Heart Laser; PLC Medical Systems,Inc), a Ho:YAG laser (Laser Photonics, Sunnyvale, CA), and anXe:Cl laser (Advanced Interventional Systems, Scottsdale, AZ).

Activation of the CO₂ laser was adjusted to coincide with theelectrocardiographic R wave, and pulses were delivered at 25J. Because this laser’s average output power is fixedat 800 W, this pulse energy setting corresponded to a pulseduration of 31 ms. The pulses were separated from each otherby at least 1 minute to achieve adequate hemostasis. In a separateset of experiments, CO₂ laser emission was set to coincide withthe T wave. The Ho:YAG laser was set to a pulse energy of 2J/pulse and a pulsing frequency of 5 Hz. The Xe:Cl laser wasset to an output energy of 0.035 J/pulse and a pulsing frequencyof 30 Hz. The pulse duration of the Ho:YAG and the Xe:Cl laserswas fixed at 250 x 10^-3 ms and 20 x 10^-9 ms, respectively. Thesesettings corresponded to peak powers of 8,000 W for the Ho:YAGlaser and 175 x 10³ W for the Xe:Cl laser. Both lasers werecoupled to a silica fiber (outer diameter, 600 µm), andlaser ablation was continued with gentle forward pressure untilthe full thickness of the myocardium was penetrated. In someadditional cases, the fiber was advanced without activatingthe laser, to assess the arrhythmogenicity of the fiber alone.In other cases, the laser was activated during both forwardmotion (toward the ventricular cavity) and backward motion ofthe fiber.

Histologic studies
Porcine hearts subjected to TMLR in vivo were flushed with 2L of 4°C physiologic saline (retrograde through the cannulatedthoracic aorta, at 40 mm Hg) and then with 1 L of 10% bufferedformalin. Each heart was removed and photographed, and transmuralsections of laser tracks were taken for microscopic evaluation.A minimum of four blocks from representative areas of each heartwere examined grossly and microscopically. Sections for microscopicstudies were processed using standard paraffin-embedding techniques.Five-micrometer paraffin-embedded sections were stained withhematoxylin and eosin. Slides were coded and examined. Afterall sections were evaluated, the descriptions were collatedby type of laser.

Experimental design and data analysis
The electrocardiographic and systemic arterial waveforms duringand after the lasing procedure were recorded on the data analysissystem. Each heart was treated with a single laser modality,so that 30 channels were created in the anterolateral aspectof the myocardium. To eliminate interanimal variability, thesame laser modality was used on 4 consecutive animals (total,120 channels for each laser modality). The experiments wereperformed in an acute setting.

The results of the experiments were evaluated separately foreach laser modality. Premature ventricular contractions (PVCs),ventricular tachycardia (VT), and other changes in cardiac rhythm,as recorded by continuous electrocardiography, were classifiedas events. Premature ventricular contractions were differentiatedfrom other changes by the accompanying compensatory pause. Runsof three or more PVCs in a row were classified as a VT episode.The number of events per channel was analyzed from analog anddigital tracings recorded during TMLR. Table 1 shows the totalnumber of events per channel and the classification of theseevents for each laser modality.

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Table 1. Arrhythmias Associated With Channel Formation During TMLR

Statistical analysis
With each laser modality, the onset of arrhythmias associatedwith channel creation was considered the end point of the experiment.The nature of each arrhythmia, as well as the time of occurrenceof the arrhythmia (measured from the time of activation of thelaser), was also recorded. We adopted the worst-case value of0.5 for the standard deviation, ${sigma}$ [ ${sigma}$ = p (1 - p)], of the binomialdistribution of the outcomes (arrhythmia or no arrhythmia) witheach laser modality. For an acceptable standard error of 10%around the mean proportion, p, of occurrence of arrhythmiaswith each laser modality, the minimum number, n, of laser pulsesthat should be delivered with each laser modality was calculatedwith the following formula:

where 1.96is the Z value for a confidence limit of 95% ( ${alpha}$ = 0.05). Carryingon the calculation gives n = 96, which means that to detecta significant difference between the arrhythmic effects of eachlaser modality, at least 96 channels should be created witheach modality.

To preserve regional myocardial structural integrity, we refrainedfrom creating more than 30 channels per animal. Because eachlaser modality was used on 4 different animals to account forinteranimal variability, a total of 120 channels were createdwith each laser modality in a total of 4 animals. This arrangementgave us an additional margin of safety of 120/96 = 1.25, or25% above the minimum number of channels required for statisticalsignificance.

Results

Top
Abstract
Introduction
Material and methods
Results
Comment
Acknowledgments
References

No animals died of arrhythmia during the procedures. The averagenumber of pulses needed to create a single channel was 1 forthe CO₂, 11 ± 4 for the Ho:YAG, and 37 ± 8 forthe Xe:Cl. The specimens obtained from each animal’s heartwere preserved in paraffin blocks and subjected to histopathologicexamination.

Arrhythmia experiments
During creation of the 120 channels with the Ho:YAG laser, atotal of 431 events were recorded in 117 channels (98%), atan average rate of 3.68 events per channel (Table 1). All butone of the events were PVCs, occurring in 116 channels (97%).In 74 cases, distributed among 68 channels (60%), the PVCs occurredin runs of three or more, qualifying for classification as VT.The PVCs and VT episodes consistently occurred when the laserwas activated, regardless of the direction of motion of thecatheter, as long as the fiber was in contact with the myocardialtissue (Fig 1A). A brief pause in the generation of arrhythmiasoccurred when the fiber tip was fired into the blood withinthe ventricular cavity (Fig 1A). The laser fiber itself wasalso arrhythmogenic: by simply poking the transmural channelwithout firing the laser, we elicited arrhythmias in some cases(Fig 1B).

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Fig 1. Representative electrocardiographic and aortic pressure tracings obtained during transmyocardial laser revascularization. (A) Ho:YAG laser fiber firing toward, and away from, the ventricular cavity. Runs of three or more premature ventricular contractions in a row are interrupted when the fiber is not in direct contact with the myocardium. (B) Ho:YAG fiber penetrating the myocardium while not firing and while firing. The arrhythmias are more severe when the muscle is irradiated. (C) Xe:Cl laser irradiation of the heart. (D) CO₂ laser irradiation of the heart. Brief elevation of the R-wave amplitude coincides with laser activation. (E) CO₂ laser irradiation of the heart without electrical disturbance of the myocardium.

When the Xe:Cl laser was used, 426 events were recorded in 120channels, no channels being free of arrhythmic events (Table 1).Therefore, an average of 3.55 events occurred per channel.In all cases, the morphology was PVC-like (Fig 1C). A totalof 81 VT-type arrhythmias were observed in 80 channels (70%).The laser fiber itself was as arrhythmogenic as the Ho:YAG fiber.

When the CO₂ laser was synchronized with the R wave, 164 arrhythmicevents were recorded in 70 channels (60%), for an average of2.34 events per channel (p < 0.01 versus the Ho:YAG and Xe:Cllasers, Table 1). Of the 164 events, 87 (53%) were associatedwith changes that did not involve a PVC-type morphology, butrather, consisted of a transient, minimal elevation of the signalvoltage or duration (Fig 1D); 77 events (47%) involved a PVC-typemorphology. In four instances, the PVCs progressed to a nonsustainedepisode of VT. The 77 PVCs occurred in 43 channels (36%), andthe four VT episodes occurred in four channels (3%) (p <0.001 versus the Ho:YAG and Xe:Cl lasers). The remaining 50channels (42%) were arrhythmia-free (Fig 1E). When the CO₂ laserwas fired during the T wave, 332 events were recorded. Of the120 channels, 103 (86%) were associated with at least one event,and the average number of events per channel was 3.22 (p <0.001 versus the CO₂ laser fired during the R wave). Of the332 events, 325 (98%), occurring in 97 channels (81%), involvedPVC-type morphology (p < 0.01 versus the CO₂ fired duringthe R wave). A total of 26 VT episodes were observed in 18 channels(15%). This was significantly less compared with the Ho:YAG-and Xe:Cl-induced VT episodes (p < 0.01).

In Figure 2, the results of the arrhythmia experiments arepresented in graphic form with respect to the number of eventsper channel (Fig 2A) and the percentage of channels that hadan event (Fig 2B).

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Fig 2. Incidence of arrhythmias during transmyocardial laser revascularization with three laser modalities. (A) Number of arrhythmic events per channel. (B) Percentage of channels with an arrhythmic event. (CO₂-R = CO₂ laser synchronized to fire on the R wave; CO₂-T = CO₂ laser synchronized to fire on the T wave; Ho:YAG = holmium:yttrium aluminum garnet laser; PVC = premature ventricular contraction; VTach = ventricular tachycardia; Xe:Cl = xenon-chloride laser.)

Gross examination of tissue
On their epicardial surface, the Ho:YAG-treated hearts exhibitedfocal spots (diameter, 0.7 to 1.0 mm) of darkened, coagulatedblood that marked the laser fiber’s entry point. The darkcentral spots were surrounded by a concentric circular zone,which was characterized by blanching because of the thermaleffects of laser irradiation. The central spots were also demarcatedby a thin circle of hemorrhage. Transmural sections showed irregularlyshaped tracks, which were continuous with the epicardial circlesand were marked by extensive discoloration. The tracks measuredup to 2 mm in width (Fig 3A). The endocardial exit pointsof these tracks appeared similar to the entry points on theepicardial surface.

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Fig 3. Gross and histologic appearance of myocardial tissue after treatment with a Ho:YAG laser operated at a pulse energy of 2 J, pulse duration of 250 x 10^-3 s, and pulse frequency of 10 s^-1. (A) Transmural appearance of the track in a longitudinal section, showing the zigzag nature of the track. (B) Photomicrograph of a midmural section. Open arrows show laser channels, closed arrows show the borders of the zone of irreversible coagulation damage, and arrowheads show the zone of reversible damage, with an admixture of changes (see Results for details; hematoxylin and eosin stain; original magnification, x40.)

The hearts treated with the Xe:Cl laser exhibited a similarpattern of changes but on a smaller scale: the laser fiber’sepicardial entry points were smaller in diameter, and the epicardialsurface of the hearts was, in general, less invaded by grosshemorrhage. Laser tracks in the transmural sections were equallyirregular, reflecting the results of multiple pulsations ona moving heart, but the width of the tracks was much narrowerthan in the Ho:YAG-treated hearts (Fig 4A).

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Fig 4. Gross and histologic appearance of myocardial tissue after treatment with an Xe:Cl laser operated at a pulse energy of 0.035 J, pulse duration of 20 x 10^-9 s, and pulse frequency of 30 s^-1. (A) Transmural cross-section of an irregular channel. (B) Photomicrograph of a subepicardial section. Open arrows show laser channels, closed arrows show the borders of the zone of irreversible coagulation damage, and arrowheads show the zone of reversible damage with an admixture of changes (see Results for details; hematoxylin and eosin stain; original magnification, x40.)

On gross examination, the CO₂ laser channels appeared to besurrounded by a 1-mm-diameter concentric circle of hemorrhagictissue on the epicardial surface. On longitudinal sections,this circle was continuous with a straight line that crossedthe myocardium radially (Fig 5A); the circle exhibited a zoneof collateral damage or hemorrhage similar to that seen on theepicardial surface. From the endocardial viewpoint, the channelsalso appeared similar to those on the epicardium, forming acircle that measured up to 1 mm in diameter.

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Fig 5. Gross and histologic appearance of myocardial tissue after treatment with a CO₂ laser operated at a pulse energy of 20 J and pulse duration of 19 x 10^-3 s. (A) Transmural cross-section. (B) Photomicrograph of a midmural section. Open arrows show laser channels, closed arrows show the borders of the zone of coagulation damage, and arrowheads show the zone of reversible damage with an admixture of changes (see Results for details; hematoxylin and eosin stain; original magnification, x40.)

Light microscopic examination
On light microscopic examination, all the laser-treated tissueswere characterized by a central zone, which showed a track thatwas primarily open space filled with wispy strands of fibrin,enmeshed erythrocytes, and necrotic debris (Figs 3B, 4B, 5B).This track was surrounded by a zone of thermal damage or coagulationnecrosis in the immediate periphery of the channels. The cardiacmyocyte morphology in this region was primarily dense, exhibitingan eosinophilic cytoplasm, with hypercontraction bands in manymyocytes, and pyknotic to absent nuclei. The coagulated tissuethen gave way to a zone of structural changes, in which scatteredmyocytes exhibited coagulation necrosis, vacuolar changes, contractionband changes, or wavy fiber changes. This perimeter zone wasfurther accentuated by extravasated erythrocytes in the interstitialspace that corresponded to the hemorrhagic outer circles inthe gross sections. The zone of structural damage blended intothe histologically normal tissue.

The extent of damage in each zone varied according to the laserused. Table 2 shows the cumulative width of the various laserzones observed on light microscopy. Volumetric damage to thetissues was calculated from the single-dimensional measurements,assuming the presence of cylindrical channels in a 20-mm-thickmyocardium.

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Table 2. Histologic Damage in Cardiovascular Tissue During TMLR With Three Laser Modalities

	Comment

Top Abstract Introduction Material and methods Results Comment Acknowledgments References

Using three different laser instruments, we assessed the arrhythmogenicityand acute trauma-inducing potential of TMLR in the normal pigheart. We chose the pig as our experimental model because thecardiovascular anatomy of this species is remarkably similarto that of humans with respect to cardiac mass to body weightratio [7], coronary anatomy [8], and collateral formation [9].Moreover, our previous experience with this model suggestedthat it is highly susceptible to the induction of arrhythmias,even under conditions of normal perfusion. In our earlier porcineexperiments, we had observed that attempts to create regionalischemia by ligating the left anterior descending coronary arterywere incompatible with survival in most cases unless prophylacticantiarrhythmic therapy was instituted. Such therapy, however,would have interfered with the experimental design of the presentstudy, because it would have affected the primary dependentvariable, ie, the number of arrhythmic events observed per channel.The typical clinical scenario would have best been representedby an ischemic model, particularly that of a chronically hibernatingmyocardium as described by Bolukoglu and coworkers [10]. Nevertheless,the present study was conducted on porcine hearts under conditionsof normal coronary artery blood flow. We believe that this modelwas appropriate for assessing the arrhythmogenicity and trauma-inducingpotential of TMLR, which was the specific purpose of our study.

We have been using the CO₂ laser in clinical trials since June1993. We therefore had access to it for experimental studies.However, despite our requests, we were not able to obtain theHo:YAG or the Xe:Cl laser hardware directly from the manufacturerof a clinically used model. Therefore, we substituted alternativecommercial models for these laser modalities. Our understandingwas that the nature of the laser–tissue interactions wouldnot be affected so long as the clinically important variables,ie, the respective wavelengths (308 nm and 2,010 nm), deliverysystems (600-µm optical silica fibers), and settings forpulse energy and repetition rate (see Methods) were kept identicalto current clinical specifications. It should be noted, however,that there is at least one manufactured Ho:YAG modality thatis undergoing clinical evaluation and that is gated to the Rwave. Therefore, the conclusions drawn from the present resultsmay not apply to this modality.

The first factor of interest in this study was the rate of generationof complex arrhythmias associated with the creation of a singlechannel using the three different laser modalities. When theCO₂, Ho:YAG, and Xe:Cl lasers were fired during the cardiacrepolarization period (ie, during the T wave), all three laserscaused a high incidence of PVC arrhythmias (98%, 100%, and 100%,respectively). The incidence of VT, however, was significantlyhigher with the Ho:YAG (60%) and Xe:Cl (70%) instruments thanwith the CO₂ laser (15%). This finding suggests that complexventricular arrhythmias may be influenced by the type of laserwhen firing of the laser is not synchronized to occur away fromthe T wave. The incidence of VT with the CO₂ laser was furtherreduced when that laser was fired during the depolarizationperiod (R wave). This fact supports our initial hypothesis thatarrhythmias during ablation are influenced by the time of lasingwith respect to the cardiac cycle.

The hearts of patients undergoing TMLR are vulnerable to arrhythmias[11]. The presence of scar tissue or periinfarct ischemia isa well-known risk factor for reentrant ventricular tachyarrhythmias[12]. Because extracorporeal cardiopulmonary support is notused, the duration of TMLR is shortened; nevertheless, left-sidevolume overload and circumferential ventricular stress, whichoften accompany ischemic cardiomyopathy, predispose these patientsto ventricular and supraventricular arrhythmias.

In the initial 35-patient series treated at our hospital (whichreflects our early experience in using TMLR with a CO₂ laser[13, 14] either as sole therapy or as an adjunct to coronaryartery bypass grafting between July 1993 and July 1995), 28patients had a history of major arrhythmias such as frequentPVCs and runs of VT, pacemaker-dependent syncope, or cardiacarrest at baseline. After TMLR, 17 (61%) of these patients hadone or more arrhythmic sequelae, 7 of which proved fatal despitethe aggressive use of various antiarrhythmic agents. Only 3(11%) of the 28 patients had no arrhythmias postoperatively.In 9 (32%) of the 28 patients with a history of major arrhythmias,the postoperative arrhythmias were similar to those seen atbaseline. The 7 patients without a history of arrhythmias atbaseline had no postoperative complications. The increased perioperativeincidence of arrhythmic complications in patients predisposedto arrhythmia suggests that TMLR exacerbates the electricalvulnerability of the myocardium, even when the operation isperformed with the least arrhythmogenic modality (the CO₂ lasersynchronized with the R wave). Thus, the threat of arrhythmiasis a major limitation to the more widespread application ofTMLR. Use of optimal laser ablation parameters and synchronizationwith the cardiac cycle are highly important. In light of ourfindings, TMLR should be done with extreme caution when thenonsynchronized laser modalities are used. In the current randomizedphase of the clinical TMLR trials, patients with a history ofmajor arrhythmias are excluded.

The second factor of interest in our study was the relativeextent of the tissue damage caused by the currently availableTMLR laser modalities. The thermal and acoustic damage thatsurrounded the transmyocardial channel was significantly greaterwith the Ho:YAG and Xe:Cl lasers than with the CO₂ laser. Itis important to note that we did not test to determine whetherthe difference in arrhythmogenic effect with the three laserswas causally related to the different amount of tissue damagethat each laser created in our heart model. However, as discussedbelow, the trauma-inducing capacity may arguably govern thelong-term patency of the laser channels. The damage impartedto the target tissue was considerably less with the CO₂ laserthan with the other two laser modalities. The damage was predominantlythermal in the immediate vicinity of the channels and structuralin the outlying layers. The gross appearance of the channelsclosely reflected the geometry of channels created in tissuephantoms observed under fast video cinegrams [15]. The extentof the damage was also in agreement with the acute effects thatFisher and associates [16] observed in CO₂- and Ho:YAG-treatedcardiac tissue.

Ablation of cardiovascular tissue with laser energy is governednot only by the thermal- and light-distribution characteristicsof the tissue but also by the nonadjustable settings of thelaser pulse. The important parameters of the laser pulse areits energy, duration, and frequency. For a given amount of energydelivered per laser pulse, the peak power (energy over time)will increase with a decrease in the pulse duration. Therefore,with ultrashort pulses, the peak power will be very high, evenat a relatively low pulse energy. The higher the peak power,the faster the rate at which the pulse energy is delivered tothe tissue. Any excess energy not used for active ablation isused to heat the tissue, and that heat should eventually dissipateby means of conductive processes. If a high pulse frequency,however, causes heat to build up within a confined tissue spacefaster than it can be dissipated, water vapor bubbles will form.The explosive collapse of these bubbles will send shock wavesthrough the adjacent tissue layers. As this acoustic effectradiates from the ablation site in all directions, it will ripthe tissue apart and superimpose a considerable structural componenton the already existing thermal damage [6].

On histomorphometric analysis of our CO₂ laser-treated tissues,the combined thermal and structural components of the laser-induceddamage extended through a zone of 0.52 ± 0.25 mm on eachside of the channel in planar cross-sections (Table 2). Assumingthat the laser channels had a cylindrical geometry in a 20-mm-thickporcine myocardium, the volume of damaged myocardium was calculatedas 1.49 ± 1.03 cm³, excluding the channel volume itself.The total volume of damaged tissue was calculated as 1.87 ±0.72 cm³ for the Xe:Cl laser and 8.46 ± 5.35 cm³ forthe Ho:YAG laser. Therefore, these two lasers respectively produced25% and 568% more volumetric damage than did the CO₂ laser.If the intensity of the fibrous repair process is indeed proportionalto the extent of the damage, the tissue reaction to Ho:YAG andXe:Cl laser ablation will be that much greater than the reactionto CO₂ laser ablation. Therefore, unlike TMLR with the CO₂ laser[17], TMLR with the Ho:YAG and Xe:Cl lasers may not be compatiblewith long-term channel patency; according to one untested theory,however, it may enhance angiogenesis [18].

In conclusion, compared with the high-energy CO₂ laser, thelower energy Ho:YAG and Xe:Cl lasers that were not synchronizedto the subject’s electrocardiogram were more arrhythmogenicowing to the necessity of delivering multiple pulses per TMLRchannel. Also, the Ho:YAG and Xe:Cl lasers, which have a shorterpulse duration than the CO₂ device, were more traumatic to cardiovasculartissue, possibly owing to the development of high peak powers.One way to minimize these adverse reactions may be to synchronizeactivation of the Ho:YAG and Xe:Cl lasers with the subject’selectrocardiographic waveform. Whether the comparative effectsobserved in our animal model can be extrapolated to the clinicalsetting is a question that should be evaluated in controlled,multicenter, clinical trials.

Acknowledgments

Top
Abstract
Introduction
Material and methods
Results
Comment
Acknowledgments
References

We thank Ms. Virginia Fairchild, senior medical editor and writer,for her assistance in editing the manuscript. We also appreciatethe technical help of Daniel Tamez in conducting some of theexperiments and Sheila Moore in reducing the data.

This work was partially supported by PLC Systems, Inc., Franklin,MA.

References

Top
Abstract
Introduction
Material and methods
Results
Comment
Acknowledgments
References

Horvath K.A., Cohn L.H., Cooley D.A., et al. Transmyocardial laser revascularization: results of a multicenter trial with transmyocardial laser revascularization used as sole therapy for end-stage coronary artery disease. J Thorac Cardiovasc Surg 1997;113:645-654.[Abstract/Free Full Text]
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