1 Department of Anesthesiology and Surgical Intensive Care and 2 Department of Pediatric Dental Surgery, Pediatric and Physiology Hôpital Pontchaillou, 3 LTSI, INSERM 642 and 4 Groupe de Recherche Cardio-vasculaire (EA 3194), Université de Rennes 1, Rennes, France
* Corresponding author: Service d'Anesthésie-Réanimation Chirurgicale 2, Centre Hospitalier Regional et Universitaire, 2 rue Henri le Guilloux, 35033 Rennes Cedex 9, France. E-mail: eric.wodey{at}chu-rennes.fr
Accepted for publication August 12, 2004.
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Abstract |
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Methods. Forty children who required elective surgery received inhalational induction of anaesthesia using 8% sevoflurane. They were allocated randomly to receive either atropine, 20 µg kg1 (atropine group) or Ringer's lactate (control group) after 10 min of steady-state 1 MAC sevoflurane anaesthesia (baseline). Three minutes later (T0), all children received remifentanil 1 µg kg1 injected over a 60 s period, followed by an infusion of 0.25 µg kg1 min1 for 10 min then 0.5 µg kg1 min1 for 10 min. Haemodynamic variables and echocardiographic data were determined at baseline, T0, T5, T10, T15 and T20 min.
Results. Remifentanil caused a significant decrease in heart rate compared with the T0 value, which was greater at T20 than T10 in the two groups: however, the values at T10 and T20 were not significantly different from baseline in the atropine group. In comparison with T0, there was a significant fall in blood pressure in the two groups. Remifentanil caused a significant decrease in the cardiac index with or without atropine. Remifentanil did not cause variation in stroke volume (SV). In both groups, a significant increase in systemic vascular resistance occurred after administration of remifentanil. Contractility decreased significantly in the two groups, but this decrease remained moderate (between 2 and +2 SD).
Conclusion. Remifentanil produced a fall in blood pressure and cardiac index, mainly as a result of a fall in heart rate. Although atropine was able to reduce the fall in heart rate, it did not completely prevent the reduction in cardiac index.
Keywords: anaesthesia, paediatric ; anaesthetics i.v., remifentanil ; heart, myocardial contractility ; heart, myocardial function ; measurement techniques, echocardiography
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Introduction |
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Remifentanil is known to cause bradycardia and hypotension35 but the mechanisms are unclear. The potential for inducing these side-effects has been one of the reasons for the relatively infrequent use of remifentanil in children.
The aim of this study was to characterize the haemodynamic profile of remifentanil using non-invasive echocardiographic data67 during sevoflurane anaesthesia in children with and without atropine.
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Materials and methods |
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Anaesthesia was induced by inhalation of sevoflurane 8% in oxygen 100% through an open circuit in all patients. After placement of an i.v. line, the trachea was intubated and the lungs were ventilated to maintain normocapnia. Sevoflurane was then reduced to 1 MAC corrected for age for at least 10 min to achieve steady state. At this point (baseline), children were assigned randomly to receive i.v. (in 4 ml) either atropine 20 µg kg1 (atropine group) or Ringer's lactate (control group). Three minutes later (T0), all children received a bolus of remifentanil 1 µg kg1 injected over a 60 s period followed by an infusion of remifentanil 0.25 µg kg1 min1 for 10 min then 0.5 µg kg1 min1 for 10 min. At the end of the 20 min the study was finished and surgery could start. No neuromuscular blocking agents were administered.
During the study the heart rate, peripheral oxygen saturation () and end-tidal carbon dioxide (
) were monitored continuously. Non-invasive blood pressure (mm Hg) was measured every minute using an automated blood pressure cuff with an appropriate cuff size in relation to the size of the child's arm. Bradycardia was defined as greater than 20% decrease in heart rate. The following haemodynamic variables were recorded at baseline, T0, T5, T10, T15 and T20 min: heart rate, mean blood pressure (MBP), continuous Doppler, and 2D transthoracic echocardiographic data (Sonos 1000; Hewlett-Packard, Andover, MA, SA). The echocardiographic data obtained in each patient included aortic diameter and shortening fraction (SF). In the long-axis view of the left ventricular outflow tract (using the 2D mode), the end-systolic internal aortic diameter (Dao) was measured, at the annulus, and the aortic sectional area (SaAo) was calculated as (SaAo=
(Dao)2/4). The SF was measured by M mode from the parasternal long-axis view of the left ventricle at the junction of mitral valve leaflets and the papillary muscle. The left ventricular end-diastolic diameter (LVDD) was measured at the point of maximum diameter, and the left ventricular end-systolic diameter (LVSD) was measured at the point of peak upward deflection of the posterior wall. The posterior wall thickness (Pwes) was measured at end-systole. The SF was calculated as (LVDDLVSD)/LVDD and expressed as a percentage. The rate-corrected velocity of circumferential fibre shortening (VCFc) was calculated using the formula VCFc=SF/rate-corrected ejection time. The rate-corrected ejection time was ejection time divided by the square root of the RR interval (to correct to a heart rate of 60 beats min1). The left ventricular end-systolic wall stress (ESWS) was calculated using the formula: ESWS=(1.35xMBPxLVSD)/[(1+Pwes/LVSD)x(Pwes)x4].8
Continuous Doppler readings were used to measure the flow in the ascending aorta from the suprasternal view of the heart. The audio signal intensity was used to confirm positioning for maximal aortic blood flow velocities. Because the angle between the estimated direction of blood flow and the Doppler beam was 15° or less, no angle correction of the Doppler signal was made. The mean aortic flow velocity (Vao) was calculated using the software of the ultrasound system as average velocity multiplied by flow period. The average of three consecutive flow velocity integrals was taken. The cardiac index (CI) was calculated from the volumetric equation: CI (ml kg1 min1)=Vao (cm/s)xSaAo (cm2)x60/body weight (kg). The systemic vascular resistance (SVR) was evaluated as the quotient of the mean blood pressure and CI without measurement of right atrial pressure.
The VCFcESWS relation or SFESWS relation can be used to determine contractility independently of loading conditions. However, SF, VCFc and ESWS were age- and body surface area-dependent. As described by Colan and colleagues, the Z score rather than the absolute value was used to normalize these calculations, with age- and growth-related means taken from values established for healthy children or infants.9 The stressvelocity index for each child was determined relative to the distribution of this index in children at the steady state with sevoflurane without remifentanil and calculated as a normal deviate (Z score). The stress velocity index was calculated as (X1M)/SD, where X1 is the measured VCFc, M is mean VCFc calculated for the measured ESWS, and SD is the standard deviation of the regression group stressvelocity index. The stressshortening index (SSI) was correspondingly quantified as the normal deviate of fractional shortening for the given ESWS, obtained in a manner analogous to that described for the stressvelocity index. The normal value of the Z score was between 2 and +2.
All echo measurements were obtained by the same observer, who was not aware of the study hypothesis or the design details.
Statistical analysis was done using non-parametric tests. The analysis of the overall evolution of the variables between the two groups was carried out with Friedman's test. Comparisons between groups were made with the MannWhitney test and comparisons within groups with the Wilcoxon matched test. A probability value less than 0.05 was considered significant. Values are expressed as median (range).
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Results |
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Administration of atropine did not change the stressvelocity index or the SSI. However, after administration of remifentanil the stressvelocity index and the SSI decreased significantly in both groups compared with baseline and T0, with no significant difference between the two groups: this decrease remained, however, between 2 and +2 SD of the baseline values (Fig. 3).
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Discussion |
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Many authors have shown that remifentanil can induce a decrease in heart rate in adult as well as in paediatric patients.5 1017 Indeed, Klemola and colleagues reported a significant fall of 69% in heart rate when remifentanil was administered at induction of anaesthesia to children who had been pretreated with atropine before induction.14 The cardiovascular side-effects of remifentanil appear to be similar to those of other opioids (such as fentanyl and alfentanil), although the degree of bradycardia with remifentanil seems greater than with the other opioids. In our study, remifentanil caused a progressive decrease in heart rate during the first level of infusion (0.25 µg kg1 min1) and then a further reduction during the second level of infusion (0.5 µg kg1 min1), suggesting a dose-dependent effect of remifentanil on heart rate. In a similar way, Wee and colleagues found a higher incidence of bradycardia and hypotension when remifentanil was given to infants with a 1 µg kg1 min1 loading dose compared with an initial infusion of 0.25 µg kg1 min1.10 These results could explain the high proportion of children with bradycardia in our study who had not received atropine pretreatment.
Ross and colleagues showed a 17% incidence of remifentanil-related hypotension in a paediatric study in which atropine was given at the discretion of the anaesthetist.3 Similarly, Klemola and colleagues reported a decrease in MBP of 1113% after anaesthetic induction with remifentanil.14 Our results are consistent with these.
In our study, the fall in MBP resulted from a dose-dependent fall in CI. Although the fall in CI was greater in the control group, this was offset by a greater increase in SVR compared with the atropine group, so that the fall in MBP was similar in the two groups. In the control group, and in contrast to studies in adults,1112 remifentanil had no effect on the stroke volume, while the reduction in SV in the atropine group was apparent before the administration of remifentanil. In the control patients, therefore, the reduction in heart rate can largely explain the reduced CI caused by remifentanil. Administration of atropine had no significant effect on CI before remifentanil was given because the increased heart rate was offset by a fall in SV. The addition of remifentanil reversed the tachycardia but had no effect on the SV, thereby reducing the CI. Thus, irrespective of pretreatment with atropine, remifentanil reduces the CI below baseline values by causing a reduction in the absolute (rather than relative to baseline) value of the heart rate.
We have not been able to find any previous reports of atropine causing a reduction in SV in children. The reduction in SV could be due to a loading defect secondary to tachycardia. However, at T20 in the atropine group the SV remained impaired, whereas the heart rate had returned to baseline. As atropine did not significantly change the SVR at T0 in the atropine group, the effect of atropine on SV could be attributed to a preload decrease, i.e. a vasodilator effect. This finding could explain the smaller increase in SVR in the atropine group during the remifentanil infusion.
Myocardial contractility is difficult to quantify in clinical practice. Using echocardiographic measurements, Colan and colleagues reported the possibility of determining an estimate of myocardial contractility in a non-invasive manner and independently of loading conditions in children as well as in adults.9 This method has already been used successfully in paediatric anaesthesia to compare the effects of different anaesthetics.1820 In the present study, the myocardial contractility index represented by SSI and the stressvelocity index appeared to be moderately reduced in the two groups, remaining between 2 and +2 SD. This allows us to establish that the effect of remifentanil on myocardial contractility is probably moderate in healthy children.
No severe adverse effects occurred in our study with remifentanil. We intentionally used high infusion rates of remifentanil to allow us to analyse the haemodynamic effects and safety of remifentanil in children. The same infusion doses have already been used safely in adults.21 Taking into account the doses of remifentanil used, only half of the children in the control group experienced a 20% drop of CI, compared with 10% in the atropine group. All episodes of hypotension (decrease from baseline >20%) and bradycardia resolved spontaneously without pharmacological intervention when the rate of remifentanil infusion was decreased.
Thus, during sevoflurane anaesthesia in children, remifentanil decreased mean blood pressure and CI mainly because of a decrease in heart rate. Although pretreatment with atropine was able to limit the effect of remifentanil on heart rate, its potential beneficial effects on blood pressure and CI appeared to be less. The specific effect of atropine on SV in children during sevoflurane anaesthesia requires further investigation.
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References |
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2 Prys-Roberts C, Lerman J, Murat I, et al. Comparison of remifentanil versus regional anaesthesia in children anaesthetised with isoflurane/nitrous oxide. International Remifentanil Paediatric Anaesthesia Study group. Anaesthesia 2000; 55: 8706[CrossRef][ISI][Medline]
3 Ross AK, Davis PJ, Dear Gd GL, et al. Pharmacokinetics of remifentanil in anesthetized pediatric patients undergoing elective surgery or diagnostic procedures. Anesth Analg 2001; 93: 1393401
4 Hogue CW Jr, Bowdle TA, O'Leary C, et al. A multicenter evaluation of total intravenous anesthesia with remifentanil and propofol for elective inpatient surgery. Anesth Analg 1996; 83: 27985[Abstract]
5 DeSouza G, Lewis MC, TerRiet MF. Severe bradycardia after remifentanil. Anesthesiology 1997; 87: 101920[CrossRef][ISI][Medline]
6 Gardin JM, Dabestani A, Matin K, Allfie A, Russell D. Reproducibility of Doppler aortic blood flow measurements: studies on intraobserver, interobserver and day-to-day variability in normal subjects. Am J Cardiol 1984; 54: 10928[ISI][Medline]
7 Hanseus K, Bjorkhem G, Lundstrom NR. Cardiac function in healthy infants and children: Doppler echocardiographic evaluation. Pediatr Cardiol 1994; 15: 2118[ISI][Medline]
8 Rowland DG, Gutgesell HP. Use of mean arterial pressure for noninvasive determination of left ventricular end-systolic wall stress in infants and children. Am J Cardiol 1994; 74: 989[ISI][Medline]
9 Colan SD, Parness IA, Spevak PJ, Sanders SP. Developmental modulation of myocardial mechanics: age- and growth-related alterations in afterload and contractility. J Am Coll Cardiol 1992; 19: 61929[ISI][Medline]
10 Wee LH, Moriarty A, Cranston A, Bagshaw O. Remifentanil infusion for major abdominal surgery in small infants. Paediatr Anaesth 1999; 9: 4158[CrossRef][ISI][Medline]
11 Elliott P, O'Hare R, Bill KM, Phillips AS, Gibson FM, Mirakhur RK. Severe cardiovascular depression with remifentanil. Anesth Analg 2000; 91: 5861
12 Kazmaier S, Hanekop GG, Buhre W, et al. Myocardial consequences of remifentanil in patients with coronary artery disease. Br J Anaesth 2000; 84: 57883[Abstract]
13 Stevens JB, Wheatley L. Tracheal intubation in ambulatory surgery patients: using remifentanil and propofol without muscle relaxants. Anesth Analg 1998; 86: 459[Abstract]
14 Klemola UM, Hiller A. Tracheal intubation after induction of anesthesia in children with propofolremifentanil or propofolrocuronium. Can J Anaesth 2000; 47: 8549
15 Friesen RH, Veit AS, Archibald DJ, Campanini RS. A comparison of remifentanil and fentanyl for fast track paediatric cardiac anaesthesia. Paediatr Anaesth 2003; 13: 1225[CrossRef][ISI][Medline]
16 Davis PJ, Lerman J, Suresh S, et al. A randomized multicenter study of remifentanil compared with alfentanil, isoflurane, or propofol in anesthetized pediatric patients undergoing elective strabismus surgery. Anesth Analg 1997; 84: 9829[Abstract]
17 Roulleau P, Gall O, Desjeux L, Dagher C, Murat I. Remifentanil infusion for cleft palate surgery in young infants. Paediatr Anaesth 2003; 13: 7017[CrossRef][ISI][Medline]
18 Holzman RS, Van der Velde ME, Kaus SJ, et al. Sevoflurane depresses myocardial contractility less than halothane during induction of anesthesia in children. Anesthesiology 1996; 85: 12607[ISI][Medline]
19 Wodey E, Pladys P, Copin C, et al. Comparative hemodynamic depression of sevoflurane versus halothane in infants: an echocardiographic study. Anesthesiology 1997; 87: 795800[CrossRef][ISI][Medline]
20 Wodey E, Chonow L, Beneux X, Azzis O, Bansard JY, Ecoffey C. Haemodynamic effects of propofol vs thiopental in infants: an echocardiographic study. Br J Anaesth 1999; 82: 51620
21 Dershwitz M, Randel GI, Rosow CE, et al. Initial clinical experience with remifentanil, a new opioid metabolized by esterases. Anesth Analg 1995; 81: 61923.[Abstract]