1Département dAnesthésie-réanimation, CHU de Nancy, Hôpital Central, 29 Avenue de Lattre de Tassigny, F-54035 Nancy Cedex, France. 2Laboratoire dExplorations Fonctionnelles Respiratoires et Allergologiques, CHU-Hopital Maison Blanche, F-51092 Reims, France*Corresponding author
Accepted for publication: June 6, 2001
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Abstract |
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Br J Anaesth 2001; 87: 54958
Keywords: allergy; neuromuscular block, allergy
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Introduction |
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The number of anaesthetic drugs is increasing, and active pharmacological surveillance of rare unexpected adverse effects of therapeutic agents is now regarded as essential.10 In addition, guidelines for the identification and/or management of high-risk groups have been proposed.11 12 Consequently, the confirmation and quantitative risk assessment of suspected rare serious adverse reactions require proper epidemiological studies.
Clinical symptoms and reaction severity do not allow one to distinguish between an immune-mediated anaphylactic reaction and an anaphylactoid reaction resulting from direct non-specific histamine release.2 13 Furthermore, no specific treatment has been shown to prevent the occurrence of anaphylactic reactions reliably.13 As a result, the only rational approach to a patient with perioperative symptoms consistent with either an anaphylactoid or an anaphylactic reaction is to assess precisely the type of reaction, to note the drugs responsible and eventual cross-reactivity with related drugs, and to avoid subsequent administration of incriminated drugs or agents. Diagnosis of type I allergy, mediated by specific IgE antibody, is usually confirmed by skin tests,9 14 15 supported whenever possible by specific IgE assays.16
In this paper we report the results of a 2-yr survey of the incidence of anaphylaxis during anaesthesia (19971998) conducted by the GERAP (Groupe dEtudes des Réactions Anaphylactoïdes Peranesthésiques), a network of 38 French allergo-anaesthesia outpatient clinics.
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Patients and methods |
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The protocol included a questionnaire about age at the time of reaction, sex, number of previous anaesthetic procedures, history of allergy (possible history of atopy, drug, food or latex intolerance), date of the reaction, and drugs used before the reaction. Details were obtained about the degree of reaction, which was graded from I to IV depending on increasing severity [grade I = presence of cutaneous signs; grade II = presence of measurable but not life-threatening symptoms, including cutaneous effects, arterial hypotension (defined as a decrease of more than 30% in arterial blood pressure associated with unexplained tachycardia), cough or difficulty in mechanical ventilation; grade III = presence of life-threatening reactions: cardiovascular collapse, tachycardia or bradycardia, arrhythmias, severe bronchospasm; grade IV = circulatory inefficacy, cardiac and/or respiratory arrest].
Information about allergy investigations was recorded systematically: date of incident, type of skin tests performed (skin prick-test and/or intradermal testing), dilution of the tested drug leading to a positive reaction, cross-reactivity in cases of adverse reaction to a neuromuscular blocking agent, results of histamine and tryptase monitoring during the adverse reaction, and of IgE-specific assays testing responses to quaternary ammonium or latex when available.
Skin tests were performed according to standardized procedures recommended by the Commission Tripartite en Allergologie.17 Prick and intradermal tests were accompanied by control tests carried out with negative (0.4% phenol in saline) and positive (9% codeine phosphate) controls to determine whether the skin was liable to release histamine and react to it.
Prick tests were performed on the anterior part of the forearm using a drop of undiluted drug in the cases of opioids, hypnotics, colloids and neuromuscular blocking agents, with the exception of atracurium, mivacurium and morphine, which were tested with a 1/10 dilution of the commercially available drug. Prick tests with latex were performed using a standardized commercial fresh natural rubber latex extract (Stallergenes, France). Skin tests were interpreted after 15 min. A prick test was considered positive when the diameter of the wheal was at least half of that produced by the codeine test and at least 3 mm greater than the negative control.
Intradermal tests with neuromuscular blocking agents were carried out after the results of prick tests had been obtained. However, in 12 centres, these were not performed when prick test results were strongly positive. Intradermal tests were performed by injection of 0.020.05 ml of drugs diluted in 0.4% phenol physiological solution. Injections were performed every 15 min, according to a dilution scale, beginning with a 104 dilution when the prick test was positive and a 103 dilution when the prick test was negative. Injection dilutions were increased progressively to 101 for aminosteroid neuromuscular blocking agents, as long as the results remained negative. For atracurium and mivacurium, a maximal dilution of 103 was used when tests were performed on the forearm and 102 when performed on the back. Intradermal tests were considered positive when the diameter of the wheal was at least 8 mm, with a surrounding flare. When the test was positive, cross-reactivity to other neuromuscular blocking agents was investigated.
The presence of specific IgE against muscle relaxants was investigated using radioimmunoassay (RIA) based on coupling of a choline analogue to Sepharose (QAS RIA, positive threshold 1.5%) or p-aminophenylphosphoryl choline to agarose (PAPPC RIA, positive threshold 1%), as described elsewhere.18 19 The specificity of antibodies against the suspected neuromuscular blocking agent was confirmed by an inhibition step performed with the drug (inhibition required >15%).
In vitro testing for latex-specific IgE was carried out using RAST (Cap System; Pharmacia, France) according to the manufacturers instructions. Values of allergen-specific IgE above 0.35 kU l1 were considered positive. Plasma concentrations of histamine (RIA Histamine; Immunotech) and tryptase (UniCAP Tryptase, Pharmacia & Upjohn, France) were determined with commercially available RIA kits. Values above 9 nmol l1 for histamine and 12 µg l1 for tryptase were considered to be positive.
Anaphylaxis was diagnosed on the basis of skin test and/or IgE assay results consistent with the clinical history of the adverse reaction and the anaesthetic protocol. To reduce further the risk of false positives when intradermal skin test positivity for aminosteroid neuromuscular blocking agents was observed only at 1/10 dilution, the presence of specific IgE on RIA assay was required to confirm sensitization to the neuromuscular blocking agent administered at the time of the reaction.
To compare the incidences of anaphylaxis to available neuromuscular blocking agents, the number of vials of each agent sold in France in 1997 and 1998 was obtained from the pharmaceutical companies that marketed these drugs (Glaxo Wellcome, Organon Teknika, Pharmacia & Upjohn, Rhône Poulenc Rorer). The number of vials effectively used in anaesthesia was then estimated on the basis of data obtained from a market survey in France, which provided an estimate of the consumption of each neuromuscular blocking agent and its respective use during anaesthesia in intensive care units and in emergency settings in a representative sample of 100 French hospitals (data obtained from Le Panel Hospitalier, MAPI, Lyon, Edition Domaine Medical, 1998). To estimate the number of patients effectively exposed to each compound, a correction factor was applied. This factor took the average number of vials of a specific neuromuscular blocking agent used during a standard anaesthetic procedure into account. It depended on the commercially available presentation of the neuromuscular blocking agent, and was established in accordance with Glaxo Wellcome and Organon Teknika for the products they sold.
Statistical analysis
StatView IV software (Abacus Concepts, Berkeley, CA, USA) was used. Results are expressed as mean (SEM). Comparisons were performed using the 2 test or analysis of variance when appropriate. P
0.05 was considered statistically significant.
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Results |
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History of atopy, allergy, asthma or a previous adverse reaction during anaesthesia
Atopy was present in 121 cases (25.4%), and asthma in 41 cases (8.6%). A history of drug intolerance was reported in 76 cases (15.9%) and food allergy was present in 14 cases (2.9%). When latex and neuromuscular blocking agents were compared, atopy appeared to be significantly more frequent in the case of latex allergy (39 vs 24.8%, P<0.01).
In five patients, careful assessment of the medical history revealed the onset of an adverse reaction during a previous anaesthetic. In three cases, no allergic investigations had been performed after the initial incident. In the two remaining cases, diagnosis of sensitization to a neuromuscular blocking agent had been made after the initial incident.
Clinical features
Most adverse reactions were grade II (22.9%) or grade III (62.6%); only 10.1% were grade I and 4.4% grade IV. Cutaneous symptoms were present in 69.6% of cases (n=332), angio-oedema in 11.7% (n=56), bronchospasm in 44.2% (n=211), arterial hypotension in 17.8% (n=85), cardiovascular collapse in 53.7% (n=256), bradycardia in 2.1% (n=10) and cardiac arrest in 4% (n=19) (Table 2). Cardiovascular collapse was the sole feature in 40 cases, hypotension in 10 cases, bronchospasm in 15 cases and cutaneous symptoms in 37 cases. Angio-oedema never occurred in isolation.
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Severe complications, such as transient renal failure (n=2), coma (n=4), persistent vegetative state (n=1), hemiplegia (n=1) and neurological sequelae in the newborn of a pregnant patient n=1, were observed.
No differences in symptom severity were observed with respect to sex, history of atopy, asthma or food and drug intolerance. In eight cases, long-term treatment with ß-blockers was noted. Seven of these cases were of grade III severity and one was of grade IV with cardiac arrest.
A significant association between the onset of bronchospasm and a history of atopy or asthma was observed (P<0.005).
Specific considerations for neuromuscular blocking agents and latex allergy
Neuromuscular blocking agents
The respective contribution of each neuromuscular blocking drug is shown in Table 1. Three hundred and thirty-six cases of anaphylaxis involved a neuromuscular blocking agent. Although succinylcholine (n=78) remains a major causal agent, rocuronium (n=98) was the drug incriminated most frequently over the 2 yr (19971998) study period. Atracurium (n=71) and vecuronium (n=59) were also involved frequently, whereas reactions to pancuronium (n=20), mivacurium (n=9) and cisatracurium (n=1) were less common. When considering these results, the actual clinical use of these drugs in France should be taken into account. This can be estimated on the basis of the results of the survey of the market share of neuromuscular blocking agents. The percentages of vials of each drug used in operating rooms and in intensive care units were also considered (Table 3). A correction factor based on the average number of vials used during anaesthesia in one patient, defined with and accepted by the principal manufacturers of neuromuscular blocking agents (Glaxo Wellcome and Organon Teknika) was also used to estimate the number of anaesthetized patients exposed to each compound. A significant difference was observed when percentage of anaphylactic reactions to each drug was compared with the estimated percentage of patients who received these drugs over the same time period (P<0.0001). Succinylcholine and rocuronium appeared to be involved most frequently, followed by vecuronium and pancuronium, and atracurium was involved least frequently.
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Early plasma histamine and tryptase determinations were performed in 90 and 97 cases respectively. They were considered to be positive in 81 and 94 cases respectively. When both tests were performed in a patient, they were both negative in only two cases. This corresponded to a positive intradermal reaction to atracurium at a dilution of 103.
The numbers of positive intradermal test results according to the dilution threshold and the different agents involved are summarized in Table 4. Skin tests were performed in 331 out of 336 patients. They were negative in four cases. In each of these four cases, the severity grade of the reaction was III or IV, and specific IgE against a neuromuscular blocking agent was detected. Moreover, tryptase determination was positive in three of them.
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Specific IgE assay was performed in 234 patients. Results for the various agents studied are summarized in Table 5. They were positive in 202 cases (86.3%). Negative results for both IgE and skin tests were never observed. In the four cases of life-threatening reaction and negative skin tests, the IgE assay was positive, with a high percentage of specific IgE binding in the presence of the offending molecule.
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Reactions to latex were less severe than those observed with neuromuscular blocking drugs (P<0.0001) (Fig. 3). On four occasions, these reactions occurred during gynaecological procedures, after injection of oxytocin, and in one case after removal of a tourniquet.
A history of previous anaesthesia was found in 51 of the 59 cases of latex allergy (86.4%). No detailed information was available about the number of previous anaesthetics or the patients occupational status. A history evocative of latex sensitization, such as fruit allergy or intolerance to materials containing rubber latex, was noted retrospectively in 14 cases (23.7%). Atopy was present in 23 cases (39%) and asthma in seven (11.9%).
Skin prick tests were performed in 58 out of 59 cases and were positive in 57 patients (98.3%). In the patient with a negative skin test and the patient not investigated using the prick-test, IgE latex-specific assay was positive. Specific latex IgE assay was performed in 41 of these patients. It was positive in 38 cases (92.7%).
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Discussion |
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Our results confirm the large female predominance (2.7 female/1 male) of anaphylactic reactions, although it is less marked than that reported in other studies, where it ranges from 8 females/1 male22 to 3.5 females/1 male.9 It should be noted that this difference persists even when the sex ratio of anaesthetized patients established by the French survey of anaesthesia (1.1 female/1 male) is taken into account.20
Atopy and the presence of drug or food intolerance were assessed by history. Immunological assessment by skin testing or immunoassay was not performed systematically. The presence of atopy was reported in 25.4% of our patients. This rate is similar to that observed in our previous survey2 and that observed in normal subjects.23 However, as reported previously,2 24 the presence of atopy was significantly more frequent in cases of latex allergy than in allergy to neuromuscular blocking agents (39 vs 24.8%, P<0.01). A history of drug allergy was present in 15.9% of our patients, a rate that approaches that reported in normal subjects (15%).25 In most cases, clinical reactions were severe (90% of cases were at least grade II) and often life-threatening (67% were grade III or IV). These results confirm the severity of immune-mediated adverse reactions. This contrasts with reports of anaphylactoid reactions of a non-immune type, 49% of which were of grade I.2 In addition, it should be noted that, because of the design of the present study, severe reactions resulting in death or major clinical sequelae impeding patient follow-up remained unaccounted for. Clinical observations in which tryptase was determined post-mortem26 or specific muscle relaxant IgE was detected in blood samples taken during a fatal anaesthetic anaphylactic event3 have been reported.
The most common features in this study were cardiovascular manifestations, present in 71.47%, followed by cutaneous symptoms (69.6%) and bronchospasm (44.2%). Cardiovascular symptoms were the sole feature in 10.5% of cases and in 10 cases were limited to hypotension. Similarly, bronchospasm was the only sign in 15 cases. These results concur with previous data2 16 27 and may explain why the reaction can be attributed to causes other than anaphylaxis. As in previously reports, asthmatic patients with anaphylaxis often presented with bronchospasm.16 27 Reaction severity was more pronounced in cases of sensitization to neuromuscular blocking agents than in cases of latex sensitization.2
The overall distribution of the various causal agents was similar to those reported previously.2 27 Anaphylactic reactions to local anaesthetics appear to be uncommon.16 Adverse reactions to colloids were less frequent than in some previous studies27. This probably reflects the decreased use of gelatins as volume expanders in France. Latex sensitization was involved in 12.1% of cases. These results differ significantly from previous reports from a time when latex allergy was poorly recognized.9 The relative decrease in the number of cases diagnosed is encouraging; in our last published survey latex allergy was involved in 16.6% of cases.2 Increasing awareness of the risk of latex sensitization in spina bifida children28 or health-care workers,29 combined with the efficacy of surgical procedures in a latex-free environment,30 could be responsible for the decrease in the incidence of latex anaphylaxis we observed.
Although succinylcholine (n=78) remains a major causal agent, there are differences in this report, compared with our last survey, in the involvement of other neuromuscular blocking agents.2 Rocuronium (n=98) appears to be the agent involved most frequently. As can be seen in Table 3, when account is taken of differences in the anaesthesia market share and the number of patients exposed, there are significant differences among the drugs that have been incriminated. These observations rely on the estimation of the number of patients exposed and should therefore be considered with circumspection. In addition, anaesthetists might have paid more attention to the effects of the drugs that have become available more recently, especially in cases of mild reactions. However, the increasing awareness of adverse reactions to rocuronium and the incidence of anaphylaxis (82 cases) is noteworthy.2 27 3138
In our study, positive diagnosis was mainly based on clinical history and skin test results, often corroborated by specific IgE assay. Although skin tests have been used extensively for more than two decades, there has been controversy recently concerning their use in the diagnosis of sensitization to rocuronium.39 According to Levy and colleagues,39 rocuronium prepared as a solution of 10 mg ml1 requires dilution to 102 to avoid false-positive intradermal test results. This differs from the 101 dilution recommended by the Commission Tripartite en Allergologie, which was the highest test concentration used by our participating centres.17 However, in the report of Levy and colleagues, intradermal testing was performed on the anterior face of the forearm rather than on the patients back. The latter approach is favoured in France because the skin of the forearm is more likely to release histamine non-specifically.15 Moreover, an unexpected mean weal diameter of almost 6 mm with a negative control injection of saline was reported by Levy and colleagues. According to the Commission Tripartite en Allergologie recommendations, such a result would have invalidated the test. Among the 98 cases of sensitization to rocuronium we observed, intradermal testing was considered positive at a dilution of 101 in only six cases. These observations corresponded to three grade II and three grade III reactions, and in all of these cases the specific IgE assay against rocuronium was positive.
Nevertheless, the differences observed in the relative frequencies of sensitization to the various commercially available neuromuscular blocking agents remain to be explained. Indeed, one of the mechanisms of anaphylaxis to these drugs involves the presence of quaternary ammonium ions,40 but other factors, such as the distance between the quaternary ammonium ions and the flexibility of the entire molecule, may also be important.41 The differences observed in cross-sensitization between different agents in this study have also been noted in previous reports; cross-sensitization appears to be more frequent with aminosteroid neuromuscular blocking agents than with benzylisoquinoline-derived neuromuscular blocking agents.42 43
The need for early as well as delayed laboratory investigations to confirm the occurrence of anaphylaxis should be stressed. In this series, early histamine and tryptase determinations were performed in 90 and 97 cases of anaphylaxis due to a neuromuscular blocking agent, and were found to be positive in 81 and 94 cases respectively. Moreover, when both tests were performed in the same patient, they were both negative in only two patients. This is consistent with previous reports concerning the value of these tests in the diagnosis of anaphylaxis to anaesthetic drugs.44 45
Similarly, determination of specific muscle relaxant IgE, when performed, was positive in 86.3% of cases. These results were obtained with RIAs based on coupling an analogue of choline to Sepharose (QAS-RIA)18 or p-aminophenylphosphorylcholine to agarose (PAPPC-RIA).19 These RIA methods offer greater sensitivity (QAS-RIA, 87.5%; PAPPC-RIA, 97%) and specificity (QAS-RIA, 100%; PAPPC-RIA, 97%) than classic commercially available RIA kits, such as the RAST-succinylcholine test (sensitivity 66%).18 In addition, when performed, specific latex IgE assays were positive in 92.7% of cases, confirming the quality of this RIA. These results support the widespread use of the specific IgE assay in suspected cases of adverse reactions to anaesthetics. Moreover, serum samples can be drawn at the time of the adverse reaction and stored for testing later. This can facilitate further investigation of fatal anaphylactic reactions.3
In conclusion, our study confirms the predominance of sensitization to neuromuscular blocking agents and latex in anaphylactic reactions during anaesthesia. The differences observed over time concerning the relative contributions of the various neuromuscular blocking agents strengthen the need for post-marketing risk detection for new drugs. In addition, our results underline the need for wider use of specific IgE assays combined with skin testing in the diagnosis of sensitization to neuromuscular blocking agents and latex, even in cases of minor adverse reactions. As suggested by the reduced incidence of anaphylaxis to latex, which is a probable consequence of generalized identification and preventative measures, an active policy to identify at-risk patients through the establishment of allergo-anaesthesia centres should be promoted.
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Acknowledgements |
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Groupe d'Etudes des Réactions Anaphylactoïdes Peranesthésiques. Amiens: B. Benabes, C. Quequet. Angers: C. Cottineau, M. Drouet. Besançon: M. Neidhardt, P. Girardin, M. Vigan. BordeauxPellegrin Tripode: S. Guez. Pessac: M. Tunon de Lara. Brest: J. C. Rakatoseheno. Caen: D. Laroche, M. C. Vergnault. Dijon: E. Collet, N. Louvier. Dreux: J. B. Duffin. Grenoble: C. Jacquot, P. Zambelli, D. Coperan. Lille: A. Facon. Limoges: I. Orsel. Lorient: F. Le Pabic. Lyon: Y. Benoît, J. Motin, L. Guilloux. Marseille: J. Birnbaum, D. Vervloet. Montpellier: M. C. Bonnet, T. Ryckwaert. Nancy: M. C. Laxenaire, C. Mouton, D. A. Moneret-Vautrin, S. Widmer, J. L. Guéant, I. Gastin. Nantes: F. Wessel. Nice: G. Occelli, J. Amédéo. Nîmes: M. Joncourt. Paris-Pitié: A. M. Korinek. Paris-Necker: D. Brunet-Langot, J. Labbez. Paris-Broussais: B. Fontaine. Paris-Tenon: F. Leynadier. Poitiers: K. Breuil. Reims: A. Gallet, F. Lavaud. Rennes: M. M. Lucas, Y. Delaval. Saint-Etienne: C. Dzviga. Strasbourg: J. Valfrey. Suresnes: M. T. Guinnepain. Tarbes: J. Gayraud. Toulouse-Purpan: D. Giamarchi, M. Migueres, H. Perelroizen. Toulouse-Rangueil: A. Didier. Tours: P. Carré.
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