1 Department of Anesthesiology and Intensive Care, St Anna Hospital Ferrara, Ferrara, Italy. 2 Department of Clinical and Experimental Medicine, Section of Pharmacology, University of Ferrara, Ferrara, Italy. 3 Department of Biomedical Sciences and Advanced Therapies, Section of Orthopedics and Traumatology, University of Ferrara, Ferrara, Italy. 4 Clinical Pharmacology, St Anna Hospital, University of Ferrara, Ferrara, Italy
*Corresponding author: Department of Clinical and Experimental Medicine, Section of Pharmacology, University of Ferrara, Via Fossato di Mortara 17-19, 44100, Ferrara, Italy. E-mail: ant@unife.it Declaration of interest. This work was supported by AstraZeneca, Basiglio, Milano, Italy. Presented in part at the Third European Congress of Orthopaedic Anaesthesia, 31 May2 June 2001, London, UK.
Accepted for publication: May 25, 2003
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Abstract |
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Methods. Thirty-seven patients undergoing elective hip/knee arthroplasties under spinal block were randomly assigned to two analgesia groups. Group M received continuous i.v. infusion of morphine plus ketorolac for 24 h. Then, a multi-hole 16 G catheter was placed subcutaneously and infusion of saline was maintained for 55 h. Group R received i.v. saline. Thereafter the wound was infiltrated with a solution of ropivacaine 0.5% 40 ml, then a multi-hole 16 G catheter was placed subcutaneously and an infusion of ropivacaine 0.2% 5 ml h1 was maintained for 55 h. Visual analogue scale scores were assessed at rest and on passive mobilization by nurses blinded to analgesic treatment. Total plasma ropivacaine concentration was measured.
Results. Group R showed a significant reduction in postoperative pain at rest and on mobilization, while rescue medication requirements were greater in Group M. Total ropivacaine plasma concentration remained below toxic concentrations and no adverse effects occurred. Length of hospital stay was shorter in Group R.
Conclusion. Infiltration and wound instillation with ropivacaine 0.2% is more effective in controlling postoperative pain than systemic analgesia after major joint replacement surgery.
Br J Anaesth 2003; 91: 8305
Keywords: anaesthetics local, ropivacaine; pain relief, postoperative; surgery, hip/knee arthroplasty
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Introduction |
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Thus, alternative strategies for postoperative pain relief have been studied. In particular, the treatment of postoperative pain by topical administration of local anaesthetics in the surgical area has recently proved effective in reducing postoperative pain after various surgical procedures.817 One of the most important limitations on the widespread use of this method is the potential toxicity of local anaesthetics18 resulting from their excessive plasma concentrations. Systemic absorption may be increased by large surgical incisions and soft-tissue dissection, which occur typically during major orthopaedic surgery.
Ropivacaine has vasoconstrictive properties19 and less cardiotoxicity compared with bupivacaine.20 21 These properties become particularly useful in the case of major surgical procedures. To the best of our knowledge, no studies have been performed concerning the pharmacokinetics and clinical effectiveness of large doses of ropivacaine infiltration and continuous perfusion in the surgical wound after major joint replacement surgery. The present randomized study was designed to evaluate the safety and effectiveness of continuous ropivacaine wound perfusion on postoperative pain levels compared with systemic analgesia in a sample of patients undergoing hip and knee arthroplasty.
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Patients and methods |
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All the patients received spinal anaesthesia using 0.5% plain bupivacaine (15 mg, 3 ml; Marcaina® 0.5; AstraZeneca, Basiglio, Italy) and fentanyl 15 µg at the L3L4 interspace with Whitacre 27 spinal needles. The same surgeon performed all the operations. A direct lateral approach was used for hip replacement and a median parapatellar approach for knee arthroplasties.
Patients were randomized with a computer-generated sequence and assigned to one of the following two postoperative options after opening a sealed envelope. (1) A loading dose of i.v. morphine 10 mg was given to both groups at the end of surgery. Group M (19 patients) then received a standard baseline i.v. infusion of morphine at 0.5 mg h1 plus ketorolac 3.6 mg h1 for 24 h through an elastomeric pump at a flow rate of 2 ml h1 (Infusor Baxter; 50 ml, 2 ml h1). (2) In Group R (18 patients) a normal saline solution was given i.v. at the same rate for 24 h. In Group R at the end of surgery, after the closure of the fascia, the surgeon infiltrated all surgical strata, in equal proportions for the whole length of the wound, with 40 ml of a solution of ropivacaine 0.5%, 200 mg (Naropine®; AstraZeneca). In both groups of patients, under direct visualization a multi-hole 16 G peridural catheter was placed between the muscle fascia and the subcutaneous tissues, with the catheter tip sited at the point that demarcated 50% of the length of the surgical wound. Thereafter, the catheter was stitched to the skin and the wound was closed in the usual way. A suction drain was usually placed near the arthroplasty and under the fascia at a distance from the indwelling catheter. The catheter was immediately connected to a bacterial filter through which an elastomeric infusion pump device (Infusor Baxter, Deezfield, IL, USA; 275 ml at 5 ml h1) delivered ropivacaine 0.2% at 5 ml h1 of (Group R) or saline solution (Group M) for the following 55 h. The catheter was removed at the end of infusion with an aseptic technique and the tip was subjected to microbiological analysis.
In Group R, peripheral venous blood samples (4 ml) were collected before the start of ropivacaine administration, 15, 30, 90, 180, 360 and 720 min after ropivacaine infiltration and on the first, second and third postoperative days. All plasma samples were frozen within 1 h after collection and stored at 20° C until assayed. Total plasma ropivacaine concentration was measured with a high-performance liquid chromatography method with ultraviolet detection at 210 nM.22 The system consisted of a solvent module pump (model 125; Beckman Coulter, Fullerton, CA, USA) connected to a Triathlon autoinjector and a UV detector (166 model). The column was a Lichrospher 5 µ (K5RPB12M; 125X4).
On regression of the sensory block, trained nurses, blinded to the analgesic technique used, instructed the patients on how to express their hip or knee pain at rest and on passive mobilization by kneehip flexion using a 100-mm visual analogue scale (VAS; 0 mm=no pain, 100 mm=worst imaginable pain). Pain assessments were made 2, 4, 8, 12, 24, 48 and 72 h after surgery.
During the entire postoperative period of observation, the nurses administered rescue analgesia according to this standard protocol: if VAS was <50 the patients was to receive i.m. diclofenac 75 mg; if the VAS score was 50 mm or if satisfactory pain relief was not achieved with diclofenac, an i.v. dose of 100 mg of tramadol was given (and repeated if necessary) until a pain score of <30 mm was recorded.
There were no restrictions on the frequency of drug administration or the overall daily dose in both groups. The amount of drugs needed for rescue analgesia was recorded and considered as a measure of ropivacaine efficacy. We recorded (i) local and systemic adverse events, such as postoperative bradycardia, hypotension, nausea, vomiting, headache, fever, agitation, drowsiness and confusion, (ii) liver and kidney function and (iii) the length of the wound incision. Other adverse events were recorded when observed by the physician or reported spontaneously by the patient. Patients were observed carefully for any symptoms of central nervous system toxicity, such as tinnitus, metallic taste, numbness of the tongue, dizziness or visual disturbances, muscular stiffness or twitching, dysarthria or haemodynamic changes, so that ropivacaine infusion could be stopped immediately.
After 72 h, we recorded patient satisfaction with the analgesia provided using a scale of poor, satisfactory and excellent. Length of hospital stay was also recorded. Discharge was decided by the surgeons, who were blinded to the randomization, according to the following discharge criteria: (i) satisfactory pain control for self-mobility; (ii) uncomplicated wound-healing process; (iii) uncomplicated clinical and radiographic outcome; (iv) no evidence of deep vein thrombosis; and (v) no impairments in haemoglobin or liverkidney function.
Statistical analysis
Data are expressed as mean (SEM) or mean and confidence interval. The results were analysed using the non-parametric MannWhitney test, Students t-test or the 2-test, as reported in the table and figure legends. A P-value of <0.05 was considered to be statistically significant.
Sample size calculation was based on an expected difference of 20 mm in the VAS measurement for pain between group means, based on a reported value of minimal clinically important differences in acute pain,23 on a standard deviation of 16, obtained from previous studies, with P=0.90 and =0.05. A sample size of 14 patients per group was obtained. For the same variables, an expected difference in patient satisfaction of 50% between the two groups generated a similar sample size. A conservative sample size of at least 18 patients/group was then chosen to ensure that the calculated number would be maintained for the final analysis.
Microsoft Excel for Windows and SAS for Windows were used for data entry and analysis.
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Results |
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A significant difference in postoperative pain intensity (VAS) was found in Group R vs Group M both at rest and on mobilization, beginning at 8 h and continuing to 72 h after operation (Fig. 2). These differences increased with time after surgery and became maximal during the following 1248 h. Before that period (2 and 4 h after surgery) no significant differences between groups were observed.
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The mean amount of narcotic and non-narcotic rescue medication was significantly lower in Group R than in Group M (Fig. 3). Furthermore, in Group R a significant reduction in the length of hospital stay compared with group M was observed (6.34 (0.67) and 8.79 (1.39) days respectively; P<0.05).
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Discussion |
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In this randomized clinical study we evaluated the safety and effectiveness of wound infiltration with ropivacaine 0.5% and continuous wound perfusion for 55 h with ropivacaine 0.2% into the surgical area after major joint replacement. Symptoms of systemic toxicity did not occur in the present study and no patient experienced adverse events that may have been related to ropivacaine administration. Accordingly, the total plasma concentration of ropivacaine consistently remained below the central nervous system toxicity threshold. The highest total plasma concentrations (Cmax) were between 0.30 and 1.28 µg ml1, with a mean value of 0.71 (0.17) µg ml1. A possible criticism of this evaluation is that venous rather than arterial plasma ropivacaine concentrations were measured, which may have underestimated the risk of ropivacaine toxicity. However, it is worth noting that the ropivacaine concentrations observed in this study were far below the established toxic threshold. Although previous studies24 25 reported mild central nervous system symptoms at venous plasma ropivacaine concentrations ranging from 1 to 2 µg ml1 after i.v. administration of the drug in non-premedicated volunteers, Wiedermann et al.26 observed that, during long-term epidural infusion of ropivacaine, the total plasma concentration of the anaesthetic increased steadily during infusion from 2.39 to 6.08 µg ml1 without symptoms of systemic toxicity. In addition, by evaluating the pharmocokinetics of different concentrations of ropivacaine after iliohypogastric block, other authors27 reported a Cmax of 3.70 µg ml1 with no adverse reactions. In addition, during 72 h of epidural ropivacaine infusion no signs of systemic toxicity, even at a very high total plasma ropivacaine concentration (7.1 µg ml1), have been reported.28 Finally, after wound infiltration of ropivacaine (0.75%, 375 mg) for hernia repair surgery, the highest individual maximum plasma concentration was 3.0 µg ml1, with no evidence of systemic adverse events.10
Recently, it has been found that patient-controlled wound instillation with ropivacaine decreased post-Caesarean delivery pain and opioid requirements, and good pain relief was found after patient-controlled wound instillation with ropivacaine even in the first hour after cesarean delivery.8 In our study, the poor pain control 4 h after surgery could be explained by the inability of ropivacaine to reach periosteum nociceptors under the fascia, which are the main receptors involved in early postoperative pain, while different nociceptive mechanisms cause visceral pain. However, in the following 2448 h, when postoperative pain is usually considered by the patients to be at its worst, Group R reported significantly better pain relief and fewer differences in pain intensity, both at rest and on mobilization. Interestingly, 72 h after surgery the pain was still reduced in Group R in spite of discontinuation of ropivacaine infusion. This could be explained by a vasoconstrictor action of ropivacaine that reduces its local absorption in relation to the presence of the drug in the plasma, even on the third postoperative day.
The present findings are consistent with previous studies demonstrating that the addition of local infiltration in patients having spinal anaesthesia significantly improves postoperative pain relief.29 It may be suggested that the combination of spinal anaesthesia and local infiltration could prevent central sensitization through an additive or synergistic effect. Unlike the repeated single shot, wound instillation maintains continuous inhibition of the peripheral painful stimulus.
Early mobilization of patients after major joint replacement surgery is one of the most important surgical outcomes for hospital discharge. The optimal mobilization pain control during 4872 h after surgery in Group R allowed a significant reduction in length of hospital stay with earlier patient rehabilitation, thus improving the patients quality of life and health-care while reducing hospitalization costs. The higher degree of patient satisfaction compared with systemic analgesia is further evidence in favour of the use of this technique for postoperative pain management.
A possible concern about this technique may be the potential risk of delayed wound healing and infection. Our study revealed no signs of local inflammation in any of the patients. Furthermore, it is worth noting that local anaesthetics have been reported to possess bacteriostatic and antimicrobial effects.30 Although another possible criticism of the present study is that both hip and knee joint replacement patients were included, the fact that both groups had a clear majority of hip replacement patients and an equal number of knee joint replacements should be taken into consideration. We therefore believe that the large and highly statistically significant reduction in rescue analgesia required by Group R constitutes a clinically important finding.
In conclusion, the present data suggest that wound infiltration with ropivacaine 0.5% and wound instillation with ropivacaine 0.2% could be a useful, practical and safe method as a part of a multimodal analgesic regime for the management of postoperative pain after major joint replacement surgery. Further studies in different surgical groups, including evaluation in the long-term rehabilitation setting, may be necessary to confirm the efficacy of this new pain management strategy.
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References |
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2 Bonica JJ. Postoperative pain. In: Bonica JJ, ed. The Management of Pain, Vol. 1, 2nd edn. Philadelphia: Lea and Febiger, 1990; 46180
3 Laitinen J, Nuutinen L. Intravenous diclofenac coupled with PCA fentanyl for pain relief after hip replacement. Anesthesiology 1992; 76: 1948[ISI][Medline]
4 Kostamovaara PA, Laitinen J, Nuutinen L, Koivuranta MK. Intravenous ketoprofen for pain relief after total hip or knee replacement. Acta Anaesthesiol Scand 1996; 40: 697703[ISI][Medline]
5 Ready LB, Brown CR, Stahlgren LH, et al. Evaluation of intravenous ketorolac administered by bolus or infusion for treatment of postoperative pain. Anesthesiology 1994; 80: 127786[ISI][Medline]
6 Souter AJ, Fredman B, Wite PF. Controversies in the perioperative use of nonsteroidal antiinflammatory drugs. Anesth Analg 1994;79: 117890[ISI][Medline]
7 Mei-Ling Ho, Je-Ken Chang, Gwo-Jaw Wang. Antiinflammatory drug effects on bone repair and remodeling in rabbits. Clin Orthop 1995; 313: 2708[Medline]
8 Fredman B, Shapiro A, Zohar E, et al. The analgesic efficacy of patient-controlled ropivacaine instillation after cesarean delivery. Anesth Analg 2000; 91: 143640
9 Horn EP, Schroeder F, Wilhelm S, et al. Infiltration and drain lavage with ropivacaine after major shoulder surgery. Anesth Analg 1999; 89: 14616
10 Pettersson N, Emanuelsson BM, Reventlid H, Hahn RG. High-dose ropivacaine wound infiltration for pain relief after inguinal hernia repair: a clinical and pharmacokinetic evaluation. Reg Anesth Pain Med 1998; 23: 18996[ISI][Medline]
11 Rawal N, Axelsson K, Hylander J, et al. Postoperative patient-controlled local anesthetic administration at home. Anesth Analg 1998; 86: 869[ISI][Medline]
12 Oakley MJ, Smith JS, Anderson JR, Fenton-Lee D. Randomized placebo-controlled trial of local anesthetic infusion in day-case inguinal hernia repair. Br J Surg 1998; 85: 7979[CrossRef][ISI][Medline]
13 Rawal N. Postoperative pain management in day surgery. Anesthesiology 1998; 53: 502
14 Bourget JL, Clark J, Joy N. Comparing preincisional with postincisional bupivacaine infiltration in the management of postoperative pain. Arch Surg 1997; 132: 7669[Abstract]
15 Karsten A, Galatius H, Hansen A, et al. Preoperative wound infiltration with bupivacaine reduces early and late opioid requirement after hysterectomy. Anesth Analg 1996; 83: 37681[Abstract]
16 Gozal Y, Shapira C, Gozal D, Magora F. Bupivacaine wound infiltration in thyroid surgery reduces postoperative pain and opioid demand. Acta Anaesthesiol Scand 1994; 38: 81315[ISI][Medline]
17 Partridge BL, Stabile BE. The effect of incisional bupivacaine on postoperative narcotic requirements, oxygen saturation and length of stay in the post-anesthesia care unit. Acta Anaesthiol Scand 1990; 34: 48691[ISI][Medline]
18 Dahl JB, Moiniche S, Kehlet H. Wound infiltration with local anaesthetics for postoperative pain relief. Acta Anaesthesiol Scand 1994; 38: 714[ISI][Medline]
19 Kopacz DJ, Carpenter RL, Mackey DC. Effect of ropivacaine on cutaneous capillary blood flow in pigs. Anesthesiology 1989; 71: 6974[ISI][Medline]
20 Scott DB, Lee A, Fagan D, et al. Acute toxicity of ropivacaine compared with that of bupivacaine. Anesth Analg 1989; 69: 5639[Abstract]
21 Sztark F, Malgat M, Dabadie P, Mazat JP. Comparison of the effects of bupivacaine and ropivacaine on heart cell mitochondrial bioenergetics. Anesthesiology 1998; 88: 13409[ISI][Medline]
22 Reif S, Le Corre P, Dollo G, et al. High-performance liquid chromatographic determination of ropivacaine, 3-hydroxy-ropivacaine, 4-hydroxy-ropivacaine and 2',6-pipecoloxylidide in plasma. J Chromatogr B Biomed Sci Appl 1998; 719: 23944[CrossRef][Medline]
23 De Loack LJ, Higgins MS, Caplan AB, Stiff JL. The Visual Analog Scale in the immediate postoperative period: intrasubject variability and correlation with a numeric scale. Anesth Analg 1998; 86: 1026[Abstract]
24 Scott DA, Emanuelsson BM, Mooney PH, et al. Pharmacokinetic and efficacy of long term epidural ropivacaine infusion for postoperative analgesia. Anesth Analg 1997; 85: 132230[Abstract]
25 Knudsen K, Beckman Suurkula M, Blomberg S, et al. Central nervous and cardiovascular effects of i.v. infusion of ropivacaine, bupivacaine and placebo in volunteers. Br J Anaesth 1997; 78: 50714
26 Wiedermann D, Muhlnickel B, Staroske E, Neumann Rose W. Ropivacaine plasma concentration during 120-hours epidural infusion. Br J Anaesth 2000; 85: 8305
27 Wulf H, Worthmann F, Behnke H, Bohle A S. Pharmacokinetics and pharmacodynamics of ropivacaine 2 mg/ml, 5 mg/ml, or 7.5 mg/ml after ileoinguinal blockade for ileoinguinal hernia repair in adults. Anesth Analg 1999; 89: 14714
28 Burm AGL, Stienstra R, Browwer R, et al. Epidural infusion of ropivacaine for postoperative analgesia after major orthopaedic surgery. Anesthesiology 2000; 93: 395403[CrossRef][ISI][Medline]
29 Clifford JW, Mun-Seng C. Preemptive analgesia treating postoperative pain by preventing the establishment of central sensitization. Anesth Analg 1993; 77: 36269[ISI][Medline]
30 Hollmann MW, Gross A, Jelacin N, Durieux ME. Local anesthetic effects on priming and activation of human neutrophils. Anesthesiology 2001; 95: 11322[CrossRef][ISI][Medline]