Open-access Postoperative residual paralysis

SPECIAL ARTICLE

Postoperative residual paralysis

Ligia Andrade da Silva Telles MathiasI; Ricardo Caio Gracco de BernardisII

IPhD, Faculdade de Medicina da Universidade de São Paulo (FM-USP); Adjunct Professor, Head of the Discipline of Anesthesiology, Faculdade Ciências Médicas da Santa Casa de São Paulo (FCMSCSP)

IIPhD, Surgery, FCMSCSP; Medical Director, Surgical Center, Irmandade da Santa Casa de Misericórdia de São Paulo

Correspondence to Correspondence to: Sociedade Brasileira de Anestesiologia Rua Professor Alfredo Gomes, 36 Botafogo 22251080 - Rio de Janeiro, RJ, Brazil E-mail: rba@sba.com.br

DESCRIPTION OF THE EVIDENCE COLLECTION METHOD

Multiple searches were carried out in the PubMed database to identify articles with better methodological design, followed by critical evaluation of their contents and classification according to the strength of evidence. According to the recommendations of the Oxford Centre for Evidence Based Medicine, literature systematic reviews and randomized clinical trials were preferred. Searches were carried out between January 2009 and July 2010. For the search in PubMed, different keywords combinations were used (random*; neuromuscular; postanesthesia; care; residual; paralysis; complications; blockade; curarization) as well as controlled vocabulary terms (Anesthesia, PerioperativeComplications [MeSH]; Residual Neuromuscular Blockade [MeSH]; Postanesthesia Care Unit [MeSH]; Monitoring Neuromuscular blockade [MeSH]; and Randomized Controlled Trial, Guidelines, Task force [Publication Type]). Were selected studies that evaluated the incidence, diagnostic tests, complications and prevention of postoperative residual paralysis in animals, conscious volunteers and patients submitted to surgical procedures, without distinction.

RECOMMENDANTIO DEGREE AND STRENGTH OF EVIDENCE

A: Experimental or observational studies of best consistency.

B: Experimental or observational studies of least consistency.

C: Case Reports (non-controlled studies).

D: Opinion without critical evaluation, based on consensuses, physiological studies or animal models.

OBJECTIVE

To evaluate incidence, diagnostic tests, complications and prevention of postoperative residual paralysis (PORP).

INTRODUCTION

Definition

Postoperative residual paralysis (PORP), also known as residual postoperative neuromuscular blockade, is defined as postoperative paralysis or muscle weakness due to incomplete or absent antagonism of nondepolarizing neuromuscular blockers (NMB)1(D). The T4/T1 ratio of 0.9 was assessed using the "train-of-four" stimuli (TOF). It is currently considered the gold standard of complete reversal of neuromuscular blockade1(D).

Incidence

PORP after the end of anesthesia has been reported in several studies, with an incidence ranging from 5% to 88%, considering PORP as T4/T1 ratio < 0.92(B),3(A),4(B),5(A).

What are the factors that alter the incidence of postoperative residual paralysis?

The great variability is due to different methods: use of T4/T1 ratio of 0.7, 0.8 or 0.9 as PORP criterion6,7(B); use of different NMB of short, intermediate and long-term duration3(A),6,7(B); use of single or repeated doses, or continuous infusion of NMB3(A),6,7,8(B); assessment method of the residual NMB1(D),9(A); with or without reversal of neuromuscular blockade at the end of anesthesia with anticholinesterase drugs, with dose and interval between the anticholinesterase drugs and degree assessment of neuromuscular blockade3(A),4,6-8(B); age10(B); presence of kidney, cardiac or neuromuscular dysfunction11(D); drug use that can alter the pharmacodynamics and/or pharmacokinetics of NMB (calcium channel blockers, magnesium, lithium, antibiotics, local anesthetics, inhaled anesthetics, opioids, benzodiazepines)11(D); and electrolyte abnormalities, metabolic or respiratory acidosis and hypothermia1,11,12(D).

The comparison of the PORP incidence and duration after multiple doses of cisatracurium and rocuronium showed that, at the end of surgery, the PORP incidence is significantly lower with rocuronium (44%) than with cisatracurium (57%). However, the time to achieve a T4/T1 ratio < 0.9 after the last dose of NMB is significantly higher with rocuronium2(B). The T4/T1 ratio measured 5 minutes after the end of the surgical procedure is significantly higher in the rocuronium group in comparison to cisatracurium, but at the end of 10 minutes there is no further significant difference between the T4/T1 ratio values for the two NMBs5(A).

When long-term NMB is used, the PORP incidence is significantly lower in patients being monitored, while there is no significant difference for those using short and mid-term NMB13(A).

The incidence of PORP upon entering the post-anesthetic care unit (PACU) also shows great variability4,14-16(B). The relationship between PORP and time in the PACU using mid-term NMB shows that age and T4/T1 ratio < 0.9 are independent variables associated to the length of stay in the PACU, but not to the type of NMB (vecuronium and cisatracurium) 15(B).

Recommendation: As PORP can occur after any general anesthesia that used NMB, neuromuscular blockade monitoring is recommended during and after general anesthesia and throughout post-anesthesia recovery.

Diagnostic tests

What are the diagnostic tests of Postoperative Residual Paralysis?

The diagnostic tests are clinical, qualitative and quantitative.

Clinical tests

Several clinical tests have been recommended to assess the reversal of neuromuscular blockade, such as: capacity to hold up the head for 5 seconds or to elevate an arm or a leg; eye opening when requested; protrusion or capacity to remove the tongue when held manually; maintenance of hand grip strength (measured with a dynamometer); maximal inspiratory pressure > 25 cm H2O, and vital capacity > 15 mL.kg-1 - all of them in conscious and cooperative patients2,6,8(B),17(D).

Qualitative or subjective tests

They consist in visual and/or tactile observation of the response evoked by electrical stimulation of the peripheral motor nerve. The number of responses and fatigue are assessed after TOF, or double burst stimulation (DB) of the ulnar nerve adductor pollicis muscle, or the presence of fatigue after tetanic stimulation (TS) at 50 Hz or 100 Hz, or post-tetanic count (PTC) that consists in the use of a continuous standard single stimulation 1 to 3 seconds after tetanic stimulation, counting the number of muscle contractions 17-19(D).

Quantitative or objective tests

These are tests in which a quantitative evaluation of TOF (T4/T1 ratio) is carried out using as standard the assessment of the ulnar nerve adductor pollicis muscle through acceleromyography, electromyography, kinemyography, phonomyography and mechanomyography.

The TOF and PTC monitoring allows the classification of neuromuscular blockade according to its depth: intense blockade is the period with no response of PTC (PTC = 0) and T4/T1 (0); deep blockade is the period with PTC > 1 and no response of the T4/T1 ratio (0); and moderate blockade occurs when the T4/T1 ratio is between T1 and T3. From T4 return to the normal pattern of T4/T1 ratio (> 0.9), the period is called recovery (Chart 1) 20(D).


Recommendation: Quantitative analysis is always better than the qualitative one for the PORP diagnosis.

What is the validity and correlation between the different PORP diagnostic tests?

Clinical tests have shown the following values of sensitivity, specificity, positive and negative predictive values19(D):

• Capacity to keep the head up for 5 seconds: 0.19; 0.88; 0.51; 0.64;

• Capacity to hold up the arm or the leg for 5 seconds: 0.25; 0.84; 0.50; 0.64;

• Protrusion or capacity to remove the tongue: 0.22; 0.88; 0.52; 0.64;

• Maintenance of hand grip strength: 0.18; 0.89; 0.51; 0.63.

None of the available clinical trials showed a positive correlation with the T4/T1 > 0.9, or ruled out the possibility of PORP7,8,19(B)21(C).

Qualitative tests were not superior to clinical trials19(D),22(A) and the use of DB did not eliminate the possibility of PC19(D),23(B).

There is no significant correlation between subjective and objective evaluation of the evoked response, considering T4/T1 > 0.9 as the standard for PORP absence24(B),25(C).

There is no consensus that quantitative tests of neuromuscular function are superior to qualitative ones. Regarding neuromuscular monitoring and PORP, there is also no consensus that the use of quantitative tests of neuromuscular function promote a reduction in PORP incidence9,13(A),17(D).

Regarding the clinical and scientific use of acceleromyography compared to signals and/or symptoms of PORP and to pulmonary function, clinical or qualitative tests of neuromuscular function, one can concluded that accelerometry is the best test to diagnose PORP (Table I)26(B) and intraoperative monitoring with acceleromyography improves PORP detection, being as sensitive as mechanomyography. There is not sufficient evidence that when accelerometry is used uncorrected (without normalization), the value of the T4/T1 ratio should be increased above 0.9 to exclude clinically significant PORP9(A).

Recommendation: Acceleromyography is recommended for monitoring the NMB degree in intraoperative and post-anesthetic periods.

PORP Complications

PORP can lead to several complications.

There is association between T4/T1 ratio < 0.9 and the following complications:

• Impaired coordination between the lower pharyngeal constrictor muscle contraction and relaxation of the upper esophageal sphincter; difficulty in swallowing and delay on the start of swallowing reflex27,28(B); decreased tonus of the upper esophageal sphincter27,28(B); and increased risk of passive regurgitation27,29(B);

• Decreased volume of the upper airways; muscle dilating function impairment of the upper airways; decreased retropalatal and retroglossal inspiratory volume of upper airways; attenuation of the normal increase of posterior airway diameter during forced inspiration; and decreased activity of the genioglossus muscle during maximum voluntary tongue protrusion30(B);

• Decreased ventilator response to hypoxia in hypocapnia31-33(B);

• Decrease in forced inspiratory volume in one second and of the inspiratory flow, upper airway obstruction, and incapacity to keep the patent airways28(B);

• muscle weakness symptoms such as diplopia, difficulty to speak and drink, facial muscle weakness, incapacity to hold up the head for 5 seconds and generalized weakness2(B);

At the end of the anesthesia, either at the PACU or the Intensive Care Unit (ICU), it is known that:

• There is increased risk of postoperative hypoxemia3(A),34(B);

• There is an incidence increase of upper airway obstruction during transportation to PACU35(B);

• There are symptoms and signs of deep muscle weakness3(A);

• There is an incidence increase of critical respiratory events in the PACU34,35(B);

• There is delay in PACU discharge3(B);

• There is an increase in ventilator weaning and intubation time in patients undergoing cardiac surgical procedures 36 (A);

• There is an increased incidence of postoperative pulmonary complications (atelectasis and pneumonia)10(B).

PORP prevention

How can PORP be prevented?

The prevention of PORP is based on the complete reversal of the nondepolarizing NMB effects. It can be attained by waiting for the spontaneous termination of NMB effect, which is not predictable6(B) or by pharmacological reversal, ensuring the safety of the effect end11,37(D). The quantitative monitoring of neuromuscular blockade is the only sure way to evaluate its complete reversal28,38,39(B). Reversal may be accomplished through the use of anticholinesterase agents (ACAs), or a specific reversal agent for vecuronium and rocuronium11,37(D).

The ACAs used in anesthesia are neostigmine and edrophonium, administered intravenously at doses of 0.04 mg.kg-1 and 1.0 mg.kg-1, with peak action occurring at 7-11 minutes and 1-2 minutes, respectively11,37(D). Both have very variable latency to complete reversal of neuromuscular blockade11,37(D), reaching up to 80 minutes37(D), depending on the blockade degree.

ACAs have several limitations: they depend on the degree of neuromuscular blockade40(B); they have adverse effects on different organs and systems due to the antimuscarinic action; they have a ceiling effect41(D); they can lead to unpredictable reversal of neuromuscular blockade when used in patients with other comorbidities, or in situations such as hypothermia, or when using certain drugs such as calcium-channel blockers, aminoglycosides and magnesium sulphate37(D); and they can promote blockade by desensitization, with increased muscle weakness when used at high doses, or when used after complete recovery of neuromuscular blockade or without previous use of NMB43(C),42,44(D). They can also decrease the activity of the upper airway dilating muscles, if used after recovery of neuromuscular blockade induced by rocuronium45(B). When administered, ACAs should be associated with anticholinergic agents to reduce secondary muscarinic effects, with atropine being the most frequently used37(D),40(B).

The uncertainty regarding anticholinesterase drugs effectiveness in the neuromuscular blockade reversal, in addition to the incidence of their adverse effects has resulted in the use of sugammadex37(D). Due to its selectivity, sugammadex reverses the neuromuscular block induced by vecuronium and rocuronium and does not inhibit the effects of NMB belonging to the class of benzylisoquinoline alkaloids46(A),47,48(B),49(A).

The sugammadex-rocuronium complex is eliminated by the kidney50(B). However, the comparative use between patients with chronic renal failure and with normal renal function, associated with rocuronium, shows that the time to reach T4/T1 of 0.9 is similar in both groups and there is absence of recurarization or of adverse effects50(B).

Sugammadex has a higher reversal rate of rocuronium-induced neuromuscular blockade when compared with neostigmine in situations of moderate or deep blockade51-54,56(A)55(B). The same situation occurs in the reversal of neuromuscular blockade induced by vecuronium57(A).

After rocuronium or vecuronium use, sugammadex at a dose of 2 mg.kg-1 completely reverses (T4/T1 ratio > 0.9) the moderate neuromuscular blockade and at a dose of 4 mg.kg-1 it reverses deep neuromuscular blockade58(A),59,60(B). The use of sugammadex at doses < 2 mg.kg-1 is related to transient return of the neuromuscular blockade61(D).

In "no ventilation, no intubation" situations, which often occur shortly after anesthetic induction and failed tracheal intubation attempt, sugammadex at a dose of 16 mg.kg-1 promotes immediate reversal of the neuromuscular blockade induced by rocuronium at a dose 1.0 to 1.2 mg.kg-158(A),60(B). In this situation, the reversal time of neuromuscular blockade with the association rocuronium 1.2 mg.kg-1 and sugammadex 16 mg.kg-1 (3 minutes after the NMB) is lower than of succinylcholine 1 mg.kg-1 62(A).

Sugammadex was successfully used in children between 2 and 11 years old at a dose of 2 mg.kg-1, without adverse events63(A), as well as in patients with heart disease (coronary ischemic disease, arrhythmia and congestive heart failure) to be submitted to noncardiac procedures64(A), in patients with history of pulmonary disease11,37(D), in pregnant women who underwent a C-section65(C), and in obese patients with body mass index (BMI) > 30 kg.m-237(D). In elderly patients (age > 64 years), the use of sugammadex at a dose of 2 mg.kg-1 results in reversion of the neuromuscular blockade within a shorter time than in young adult individuals (difference of 42 seconds)66,67(B).

The sugammadex interaction has been experimentally demonstrated with flucoxacillin, fusidic acid and toremifene, with a delay in the reversal time of neuromuscular blockade. However, the interaction with flucoxacillin has not been proven clinically and no drug has been shown to promote recurarization or reversal of neuromuscular blockade68(C).

Adverse events due to sugammadex use are rare, including nausea, vomiting, headache, neck pain, back pain, coughing, dysgeusia, constipation, and pyrexia, most likely related to drugs used during anesthesia46 (A). Movements can also be observed before the end of the anesthesia, due to superficial anesthesia11(D),49(A). The onset of spontaneous evolution of allergic reaction following the use of sugammadex has been reported in only six patients37,11(D),46(A).

Recommendation: PORP prevention after nondepolarizing NMB can be attained by using anticholinesterase agents associated with anticholinergics, or sugammadex if vecuronium or rocuronium are administered. Sugammadex is recommended whenever rocuronium or vecuronium is used, as it is the only specific reverser.

FINAL RECOMMENDATIONS

The PORP shows high incidence and may lead to adverse events with increased postoperative morbidity and mortality. Monitoring of the neuromuscular blockade is recommended by quantitative tests such as acceleromyography. The use of cholinesterase inhibitors for pharmacological reversal of neuromuscular blockade is not free of adverse effects. Therefore, we recommend the use of sugammadex for reversal of neuromuscular blockade induced by rocuronium or vecuronium.

REFERENCES

Received from the Brazilian Society of Anesthesiology, Brazil.

References

  • 1. Murphy GS, Brull SJ - Residual neuromuscular block: lessons unlearned. Part I: definitions, incidence, and adverse physiologic effects of residual neuromuscular block. Anesth Analg, 2010;111:120-128. (D)
  • 2. Kopman AF, Yee PS, Neuman GG - Relationship of the train-of-four fade ratio to clinical signs and symptoms of residual paralysis in awake volunteers. Anesthesiology, 1997;86:765-771. (B)
  • 3. Murphy GS, Szokol JW, Franklin M, Marymont JH, Avram MJ, Vender JS - Postanesthesia care unit recovery times and neuromuscular blocking drugs: A prospective study of orthopedic surgical patients randomized to receive pancuronium or rocuronium. Anesth Analg, 2004;98:193-200. (A)
  • 4. Baillard C, Clec'h C, Catineau J et al. - Postoperative residual neuromuscular block: a survey of management. Br J Anaesth, 2005;95:622-626. (B)
  • 5. Maybauer DM, Geldner G, Blobner M et al. - Incidence and duration of residual paralysis at the end of surgery after multiple administrations of cisatracurium and rocuronium. Anaesthesia, 2007;62:12-17. (A)
  • 6. Hayes AH, Mirakhur RK, Breslin DS, Reid JE, McCourt KC - Postoperative residual block after intermediate-acting neuromuscular blocking drugs. Anaesthesia, 2001;56:312-318. (B)
  • 7. Debaene B, Plaud B, Dilly MP, Donati F - Residual paralysis in the PACU after a single intubating dose of nondepolarizing muscle relaxant with an intermediate duration of action. Anesthesiology, 2003;98:1042-1048. (B)
  • 8. Murphy GS, Szokol JW, Marymont JH, Franklin M, Avram MJ, Vender JS - Residual paralysis at the time of tracheal extubation. Anesth Analg, 2005;100:1840-1845. (B)
  • 9. Claudius C, Viby-Mogensen J - Acceleromyography for use in scientific and clinical practice: a systematic review of the evidence. Anesthesiology, 2008;108:1117-1140. (A)
  • 10. Berg H, Roed J, Viby-Mogensen J et al. - Residual neuromuscular block is a risk factor for postoperative pulmonary complications. A prospective, randomised, and blinded study of postoperative pulmonary complications after atracurium, vecuronium and pancuronium. Acta Anaesthesiol Scand, 1997;41:1095-1103. (B)
  • 11. Srivastava A, Hunter JM - Reversal of neuromuscular block. Br J Anaesth, 2009;103:115-129. (D)
  • 12. Eriksson LI - The Effects of Residual Neuromuscular Blockade and Volatile Anesthetics on the Control of Ventilation. Anesth Analg, 1999;89:243-251. (D)
  • 13. Naguib M, Kopman AF, Ensor JE - Neuromuscular monitoring and postoperative residual curarisation: a meta-analysis. Br J Anaesth, 2007;98:302-316. (A)
  • 14. Morais BS, Castro CHV, Teixeira VC, Pinto AS - Bloqueio Neuromuscular Residual após o Uso de Rocurônio ou Cisatracúrio. Rev Bras Anestesiol, 2005;55:622-630. (B)
  • 15. Butterly A, Bittner EA, George E, Sandberg WS, Eikermann M, Schmidt U - Postoperative residual curarization from intermediate-acting neuromuscular blocking agents delays recovery room discharge. Br J Anaesth, 2010;105:304-349. (B)
  • 16. Yip PC, Hannam JA, Cameron AJ, Campbell D - Incidence of residual neuromuscular blockade in a post-anaesthetic care unit. Anaesth Intensive Care, 2010;38:91-95. (B)
  • 17. Plaud B, Debaene B, Donati F, Marty J - Residual paralysis after emergence from anesthesia. Anesthesiology, 2010;112:1013-1022. (D)
  • 18. Fuchs-Buder T, Schreiber JU, Meistelman - Monitoring neuromuscular block: an update. Anaesthesia, 2009;64(suppl 1):82-89. (D)
  • 19. Brull SJ, Murphy GS - Residual neuromuscular block: lessons unlearned. Part II: methods to reduce the risk of residual weakness. Anesth Analg, 2010;111:129-140. (D)
  • 20. Fuchs-Buder T, Claudius C, Skovgaard LT, Eriksson LI, Mirakhur RK, Viby-Mogensen J - Good clinical research practice in pharmacodynamic studies of neuromuscular blocking agents II: the Stockholm revision. Acta Anaesthesiol Scand, 2007;51:789-808.(D)
  • 21. Beemer GH, Rozental P - Postoperative neuromuscular function. Anaesth Intensive Care, 1986;14:41-45. (B)
  • 22. Pedersen T, Viby-Mogensen J, Bang U, Olsen NV, Jensen E, Engboek J - Does perioperative tactile evaluation of the train-of-four response influence the frequency of postoperative residual neuromuscular blockade? Anesthesiology, 1990;73:835-839. (A)
  • 23. Fruergaard K, Viby-Mogensen J, Berg H, el-Mahdy AM - Tactile evaluation of the response to double burst stimulation decreases, but does not eliminate, the problem of postoperative residual paralysis. Acta Anaesthesiol Scand, 1998;42:1168-1174. (B)
  • 24. Baurain MJ, Hennart DA, Godschalx A et al. - Visual evaluation of residual curarization in anesthetized patients using one hundred-hertz, five-second tetanic stimulation at the adductor pollicis muscle. Anesth Analg, 1998;87:185-189. (B)
  • 25. Viby-Mogensen J, Jensen NH, Engbaek J, Ording H, Skovgaard LT, Chraemmer-Jorgensen B - Tactile and Visual Evaluation of the Response to Train-of-four Nerve Stimulation. Anesthesiology, 1985;63:440-442. (C)
  • 26. Samet A, Capron F, Alla F, Meistelman C, Fuchs-Buder T - Single acceleromyographic train-of-four, 100-Hertz tetanus or double-burst stimulation: which test performs better to detect residual paralysis? Anesthesiology, 2005;102:51-56. (B)
  • 27. Eriksson LI, Sundman E, Olsson R et al. - Functional assessment of the pharynx at rest and during swallowing in partially paralysed humans. Anesthesiology, 1997;87:1035-1043. (B)
  • 28. Eikermann M, Groeben H, Hüsing J, Peters J - Accelerometry of Adductor Pollicis Muscle Predicts Recovery of Respiratory Function from Neuromuscular Blockade. Anesthesiology, 2003;98:1333-1337. (B)
  • 29. Sundman E, Witt H, Olsson R, Ekberg O, Kuylenstierna R, Eriksson LI - The incidence and mechanism of pharyngeal and upper esophageal dysfunction in partially paralyzed humans Anesthesiology, 2000;92:977-984. (B)
  • 30. Eikermann M, Vogt FM, Herbstreit F et al. - The predisposition to inspiratory upper airway collapse during partial neuromuscular blockade. Am J Respir Crit Care Med, 2007;175:9-15. (B)
  • 31. Eriksson LI, Lennmarken C, Wyon N, Johnson A - Attenuated ventilatory response to hypoxaemia at vecuronium-induced partial neuromuscular block. Acta Anaesthesiol Scand, 1992;36:710-715. (B)
  • 32. Eriksson LI, Sato M, Severinghaus JW - Effect of a vecuronium-induced partial neuromuscular block on hypoxic ventilatory response. Anesthesiology, 1993;78:693-699. (B)
  • 33. Eriksson LI - Reduced hypoxic chemosensitivity in partially paralysed man. A new property of muscle relaxants? Acta Anaesthesiol Scand, 1996;40:520-523. (B)
  • 34. Murphy GS, Szokol JW, Marymont JH, Greenberg SB, Avram MJ, Vender JS - Residual neuromuscular blockade and critical respiratory events in the postanesthesia care unit. Anesth Analg, 2008;107:130-137. (B)
  • 35. Murphy GS, Szokol JW, Marymont JH et al. - Intraoperative acceleromyographic monitoring reduces the risk of residual neuromuscular blockade and adverse respiratory events in the postanesthesia care unit. Anesthesiology, 2008;109:389-398. (B)
  • 36. Murphy GS, Szokol JW, Marymont JH et al. - Recovery of neuromuscular function after cardiac surgery: pancuronium versus rocuronium. Anesth Analg, 2003;96:1301-1307. (A)
  • 37. Hogg RM, Mirakhur RK - Reversal of neuromuscular blockade: current concepts & future developments. J Anaesth Clin Pharmacol, 2009;25:403-412. (D)
  • 38. Mortensen CR, Berg H, El-Mahdy A, Viby-Mogensen J - Perioperative monitoring of neuromuscular transmission using acceleromyography prevents residual neuromuscular block following pancuronium. Acta Anaesthesiol Scand, 1995;39:797-801. (B)
  • 39. Gätke MR, Viby-Mogensen J, Rosenstock C, Jensen FS, Skovgaard LT - Postoperative muscle paralysis after rocuronium: less residual block when acceleromyography is used. Acta Anaesthesiol Scand, 2002;46:207-213. (B)
  • 40. Magorian TT, Lynam DP, Caldew JE, Miller RD - Can early administration of neostigmine, in single or repeated doses, alter the course of neuromuscular recovery from a vecuronium-induced neuromuscular blockade? Anesthesiology, 1990;73:410-414. (B)
  • 41. Bartkowski RR - Incomplete reversal of pancuronium neuromuscular blockade by neostigmine, pyridostigmine, and edrophonium. Anesth Analg, 1987;66:594-598. (D)
  • 42. Paine JP, Hughes r, Al Azawi S - Neuromuscular block by neostigmina in anaesthetized man. Br J Anaesth, 1980;52:69-76. (B)
  • 43. Goldhill Dr, Wainwright AP, Stuart CS, Flynn PJ - Neostigmine after spontaneous recovery from neuromuscular blockade. Effect on depth of blockade monitored with train-of-four and titanic stimuli. Anaesthesia, 1989;44:293-299. (B)
  • 44. Yost CS, Maestrone E - Clinical concentrations of edrophonium enhance desensitization of the nicotinic acetylcholine receptor. Anesth Analg, 1994;78:520-526. (D)
  • 45. Eikermann M, Zaremba S, Malhotra A, Jordan AS, Rosow C, Chamberlin NL - Neostigmine but not sugamadex impairs upper airway dilator muscle activity and breathing. Br J Anaesth, 2008;101:344-349. (B)
  • 46. Chambers D, Paulden M, Paton F et al. - Sugammadex for the reversal of muscle relaxation in general anaesthesia: a systematic review and economic assessment. Health Technol Assess, 2010;14:1-211. (A)
  • 47. Epemolu O, Bom A, Hope F, Mason R - Reversal of neuromuscular blockade and simultaneous increase in plasma rocuronium concentration after the intravenous infusion of the novel reversal agent Org 25969. Anesthesiology, 2003;99:632-637. (B)
  • 48. Gijsenbergh F, Ramael S, Houwing N, van Iersel T - First human exposure of Org 25969, a novel agent to reverse the action of rocuronium bromide. Anesthesiology, 2005;103:695-703. (B)
  • 49. Sorgenfrei IF, Norrild K, Larsen PB et al. - Reversal of rocuronium-induced neuromuscular block by the selective relaxant binding agent sugammadex: a dose-finding and safety study. Anesthesiology, 2006;104:667-674. (A)
  • 50. Staals LM, Snoeck MM, Driessen JJ, Flockton EA, Heeringa M, Hunter JM - Multicentre, parallel-group, comparative trial evaluating the efficacy and safety of sugammadex in patients with end-stage renal failure or normal renal function. Br J Anaesth, 2008;101:492-497. (B)
  • 51. Sacan O, White PF, Tufanogullari B, Klein K - Sugammadex reversal of rocuronium-induced neuromuscular blockade: a comparison with neostigmine-glycopyrrolate and edrophonium-atropine. Anesth Analg, 2007;104:569-574. (A)
  • 52. Flockton EA, Mastronardi P, Hunter JM et al. - Reversal of rocuronium-induced neuromuscular block with sugammadex is faster than reversal of cisatracurium-induced block with neostigmine. Br J Anaesth, 2008;100:622-630. (A)
  • 53. Jones RK, Caldwell JE, Brull SJ, Soto RG - Reversal of profound rocuronium-induced blockade with sugammadex: a randomized comparison with neostigmine. Anesthesiology, 2008;109:816-824. (A)
  • 54. Blobner M, Eriksson LI, Scholz J, Motsch J, Della Rocca G, Prins ME - Reversal of rocurium induced nm blockade with sugammadex compared with neostigmine during sevoflurane anaesthesia: results of a randomised, controlled trial. Eur J Anaesthesiol, 2010;27:874-881. (A)
  • 55. Illman HL, Laurila P, Antila H, Meretoja AO, Alahuhta S, Olkkola KT - The duration of residual neuromuscular block after administrationm of neostigmine or sugammadex at two visible twitches during train-of-four monitoring. Anesth Analg, 2011;112:63-68. (A)
  • 56. Schaller SJ, Fink H, Ulm K, Blobner M - Sugammadex and neostigmine dose-finding study for reversal of shallow residual neuromuscular block. Anesthesiology, 2010; 113:1-7. (A)
  • 57. Khuenl-Brady KS, Wattwil M, Vanacker BF, Lora-Tamayo JI, Rietbergen H, Alvarez-Gómez JA - Sugammadex provides faster reversal of vecuronium-induced neuromuscular blockade compared with neostigmine: a multicenter, randomized, controlled trial. Anesth Analg, 2010;110:64-73. (A)
  • 58. de Boer HD, Driessen JJ, Marcus MA, Kerkkamp H, Heeringa M, Klimek M - Reversal of rocuronium-induced (1.2 mg/kg) profound neuromuscular block by sugammadex: a multicenter, dose-finding and safety study. Anesthesiology, 2007;107:239-244. (A)
  • 59. Suy K, Morias K, Cammu G, Hans P et al. - Effective reversal of moderate rocuronium or vecuronium-induced neuromuscular block with sugammadex: a selective relaxant binding agent. Anesthesiology, 2007;106:283-288. (B)
  • 60. Pühringer FK, Rex C, Sielenkämper AW et al. - Reversal of profound, high-dose rocuronium-induced neuromuscular blockade by sugammadex at two different time points: an international, multicenter, randomized, dose-finding, safety assessor-blinded, phase II trial. Anesthesiology, 2008;109:188-197. (A)
  • 61. Eleveld DJ, Kuizenga K, Proost JH, Wierda JM - A temporary decrease in twitch response during reversal of rocuronium-induced muscle relaxation with a small dose of sugammadex. Anesth Analg, 2007;104:582-584. (D)
  • 62. Lee C, Jahr JS, Candiotti KA, Warriner B, Zornow MH, Naguib M - Reversal of profound neuromuscular block by sugammadex administered three minutes after rocuronium: a comparison with spontaneous recovery from succinylcholine. Anesthesiology, 2009;110:1020-1025. (A)
  • 63. Plaud B, Meretoja O, Hofmockel R et al. - Reversal of rocuronium-induced neuromuscular blockade with sugamadex in pediatric and adult surgical patients. Anesthesiology, 2009;110:284-294. (A)
  • 64. Dahl V, Pendeville PE, Hollmann MW, Heier T, Abels EA, Blobner M - Safety and efficacy of sugammadex for the reversal of rocuronium-induced neuromuscular blockade in cardiac patients undergoing noncardiac surgery. Eur J Anaesthesiol, 2009;26:874-884. (A)
  • 65. Pühringer FK, Kristen P, Rex C - Sugammadex reversal of rocuronium-induced neuromuscular block in Caesarean section patients: a series of seven cases. Br J Anaesth, 2010;105:657-660. (C)
  • 66. Suzuki T, Kitajima O, Ueda K, Kondo Y, Kato J, Ogawa S - Reversibility of rocuronium-induced profound neuromuscular block with sugammadex in younger and older patients. Br J Anaesth, 2011;106:823-826 (B)
  • 67. McDonagh DL, Benedict PE, Kovac AL et al. - Efficacy, safety, and pharmacokinetics of sugammadex for the reversal of rocuronium-induced neuromuscular blockade in elderly patients. Anesthesiology, 2011;114:318-329. (B)
  • 68. Zwiers A, van den Heuvel M, Smeets J, Rutherford S - Assessment of the potential for displacement interactions with sugammadex - a pharmacokinetic-pharmacodynamic modelling approach. Clin Drug Investig, 2011;31:101-111. (C)
  • Correspondence to:
    Sociedade Brasileira de Anestesiologia
    Rua Professor Alfredo Gomes, 36 Botafogo
    22251080 - Rio de Janeiro, RJ, Brazil
    E-mail:
  • Publication Dates

    • Publication in this collection
      05 June 2012
    • Date of issue
      June 2012
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    Sociedade Brasileira de Anestesiologia R. Professor Alfredo Gomes, 36, 22251-080 Botafogo RJ Brasil, Tel: +55 21 2537-8100, Fax: +55 21 2537-8188 - Campinas - SP - Brazil
    E-mail: bjan@sbahq.org
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