Sugammadex: A New Wheel Has Been Invented · prevent cholinergic crisis that can ... due to respiratory failure or myasthenic crisis. ... A systematic review of sugammadex vs neostigmine
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Sugammadex:
A New Wheel Has Been Invented
Ashlee A. Wheeler, BSN, RN, SRNA
Disclaimer Statement
Conflict of Interest: None
I have not received any compensation for this
presentation.
Objectives
The participant will be able to
Describe the mechanism of action for sugammadex.
List the indications and contraindications for the use of
sugammadex.
Explain when to utilize doses of 2 mg/kg, 4 mg/kg, and
16 mg/kg of sugammadex.
What is Sugammadex?
It is the first drug in a new class of medications called selective
relaxant binding agents
Brand name is Bridion
Received U.S. Food and Drug (FDA) approval on December
15th, 2015.
Is indicated for the reversal of neuromuscular blockade caused
by the aminosteroid non-depolarizing muscle relaxants
rocuronium bromide or vecuronium bromide
What's in a name…
• Su-in Sugammadex stands for sugar
• -gammadex stands for the structural molecule gamma-
cyclodextrin
• There are 3 naturally occurring cyclodextrins
• Alpha
• Beta
• Gamma
• Sugammadex is a modified γ-cyclodextrin
Encapsulating
• Intermolecular (van der Waals’)
forces
• Thermodynamic (hydrogen)
bonds
• Hydrophobic interactions
• The exterior of the structure is hydrophilic and the interior is lipophilic
• It is able to bind with rocuronium or vecuronium in a tight 1:1 ratio
• Sugammadex has a high association rate and very low dissociation
rate
• Estimated that for every 25 million rocuronium-sugammadex
complexes that form, only one dissociates
Sugammadex-How does it work?
When administered it binds with the free floating drug in the blood plasma
This causes a concentration gradient to form, moving rocuronium from the neuromuscular junction back into the blood plasma where it can continue to be encapsulated by sugammadex
Metabolism and Elimination
Neither sugammadex or the sugammadex-rocuronium
complex undergoes any metabolism and does not form
any metabolites within the body
Both sugammadex and the sugammadex-rocuronium
complex are cleared by the kidneys nearly 100%
Normal glomerular filtration rate:
70% excreted in 6 hours
over 90% within 24 hours
Indications
• Intravenous administration
• Reversal of neuromuscular
blockade induced by:
• Rocuronium bromide
• Vecuronium bromide
• Currently only approved for use in
adults
• In Europe it is also been approved
for the reversal of rocuronium in
children and adolescents
Contraindications
Absolute contraindication is:
known hypersensitivity to
sugammadex or any of its
components.
Considerations: Renal Impairment
Patients with renal impairment: currently only recommended in
patients who have a creatinine clearance greater than 30 mL/min
In patients with a creatinine clearance less than 30 mL/min it can
take 48 hours or more for the rocuronium-sugammadex molecule to
be eliminated
It is not known how long the complex will stay bound within the body
In a study by Cammu et al. (2012) it was found that the rocuronium-
sugammadex complex can be filtered by high-flux dialysis filters
but not low-flux
High-flux filters allow molecules that are 500-40,000 Da to pass
Sugammadex exceeds 2,000 Da
Considerations: Chemotherapy
Patients who are currently on prescribed chemotherapy
drug Toremifene
There could be a delay in reversal if Toremifene has been
given the same day as the surgery.
Considerations: Oral Contraceptives
Women taking oral birth control with estrogen or
progestogen complexes:
Sugammadex will bind to the progestogen and block it,
therefore it is the equivalent of missing a dose
If given sugammadex, an alternative means of birth
control should be used for seven days post administration
Considerations: Pharmacology
Compatible delivery fluids:
Normal Saline
5% Dextrose
Ringer’s Lactate
Physically incompatible:
Verapamil
Ondansetron (Zofran)
Ranitidine (Zantac)
5% Dextrose in Normal Saline
2.5% Dextrose in 0.45% Normal
Saline
Safety Concerns
Application submitted to the FDA and the European Union
authorities in 2008
European Union authorities-approved
FDA-denied due to concerns about hypersensitivity reactions in
healthy volunteers who received high does
The incidence of hypersensitivity in all studies was less than 1%
Since its European approval in 2008 there have been over 9
million patient exposures-15 probable cases of sugammadex
anaphylaxis worldwide
Study by Godai et al, (2012) show 3 suspected cases of
sugammadex-induced hypersensitivity reactions over a 1
year period out of 1864 patient exposures-0.001609442%
“Sugammadex appears to be a safe and well-tolerated
agent”
No deaths have been related to the administration of
sugammadex
Side Effects
Hypotension
Coughing
Nausea
Vomiting
Dry Mouth
Sensation of a change in
temperature
Abnormal level of N-
Acetylglucosaminidase in the
urine
Most Frequent Adverse Effects:
Appear to be more frequent at higher clinical doses
Reactions are typically seen within 5 minutes of administration
Dosing Regimen
Dose range:
2 mg/kg if 2/4 twitches are present in response to train-of-four;
4 mg/kg if no TOF twitches are present but 1-2 post-tetanic counts are
seen
16 mg/kg within 3 minutes of 1.2 mg/kg rocuronium, in a cannot
intubate cannot ventilate situation
Delivered as a bolus within 10 seconds.
Onset: Less than 3 minutes
Dosing: Re-administration
Options for neuromuscular block after sugammadex 2-4 mg/kg
administration:
Succinylcholine
Benzylisoquinolinium agents
Cisatracurium or Atracurium
Rocuronium* or Vecuronium*
Dosing: Re-administration
Rocuronium* or Vecuronium*
Up to 4mg/kg of sugammadex
5 minutes
1.2 mg/kg rocuronium **
4 hours
0.6 mg/kg rocuronium
0.1 mg/kg vecuronium
16 mg/kg of sugammadex
24 hours
Rocuronium or Vecuronium
** Onset may be delayed up to
4 minutes
** Duration shortened up to 15
minutes
Dose
Train of Four
Reversal of 1.2 mg/kg Rocuronium
Compared to Neostigmine
This mechanism of action, as you can see, is
completely different from neostigmine
No parasympathetic effects. No anticholinergic
drugs required.
Speed of reversal has been found to be 3-8 times
faster than neostigmine
Figure1:Time(Minutes)fromAdministrationofBRIDIONorNeostigmineattheReappearanceofT2afterRocuroniumtotheT4/T1Rationto0.9
Figure2:Time(Minutes)fromAdministrationofBRIDIONorNeostigmineattheReappearanceofT2afterVecuroniumtoRecoveryoftheT4/T1Ratioto0.9
Cost
Drug Dose Price per vial $ to reverse a
100kg patient
Neostigmine 0.05 mg/kg (max
5mg)
$13.21/10 mL vial $39.39
Glycopyrrolate 200 mcg per 1 mg
of neostigmine
$13.09/2 mL vial
(2 vials, 800mcg)
$26.18
Sugammadex 2 mg/kg $88.28/2 mL vial $88.28
4 mg/kg $161.69/5 mL vial $161.69
16 mg/kg 3 x 5 mL vial =
$485.07
1 x 2 mL vial =
$88.28
$573.35
Prices from York Hospital – Reversal for 100kg patient
Drug Dose Price per vial $ to reverse a
100kg patient
Neostigmine 0.05 mg/kg (max
5mg)
$58.51/10 mL vial $89.65
Glycopyrrolate 200 mcg per 1 mg
of neostigmine
$31.14/5 mL vial
(1mg)
Sugammadex 2 mg/kg $88.59/2 mL vial $88.59
Cost
Prices from New Hanover Medical Group-Wilmington NC
J. Wheeler, personal communication, September 1,
2016
Can Sugammadex be cost-
effective?
• In a study by Carron et al. (2016) they looked at the clinical outcomes and the cost-effectiveness of sugammadex
• Cost savings were shown by decreasing the recovery time from neuromuscular blockage in the OR
• Additional savings:
• Reducing rate of postoperative residual curarization
• Time spent in the recovery room
• Decreased the rate of unexpected ICU admissions
Patient Populations
Children: Not currently FDA approved for the use in patients ≤ 17 years of age
Elderly: >65 years old. No difference in dose recommendations as long as kidney function is normal, recovery time may be prolonged from < 2 minutes to < 4 minutes
Obesity: Dose based on actual body weight
Pregnancy and breast feeding:
Animal studies showed no signs of direct or indirect negative side effects
Unknown if it is excreted in breast milk; animal studies do show a degree of excretion
Oral absorption of sugammadex is low and no effects on infants are expected
Myasthenia Gravis
Autoimmune disease resulting in a decrease in the number of postsynaptic acetylcholine receptors
Patients are treated with anticholinesterase medications such as pyridostigmine
Typically neuromuscular blocking agents are avoided in these patients
These patients are resistant to succinylcholine requiring higher doses to achieve paralysis
They can show sensitivity to nondepolarizing neuromuscular blockers requiring ½ of the ED95 dose to achieve paralysis
Reversing nondepolarizing neuromuscular blockers is avoided to prevent cholinergic crisis that can occur since patients are currently on these medications for their illness
Myasthenia Gravis-Continued
Sugammadex may change the anesthetic treatment for these patients.
Study by Ulke et al. (2013) enrolled 10 patients with myasthenia gravis who were scheduled for a video-assisted thoracoscopic extended thymectomy (VATET)
All patients received 0.3 mg/kg of rocuronium for intubation and supplemental doses if required; total dose of rocuronium was 48 mg (±16 mg)
At the end of the case all patients received 2 mg/kg of sugammadex
All patient’s achieved a train of four ratio of >0.9. All were extubated in the operating room and none required mechanical ventilation due to respiratory failure or myasthenic crisis
Case Study- Rocuronium Anaphylaxis
33-year-old, 77 kg, female laparoscopic procedure for the investigation of infertility
30 seconds after receiving 30 mg of rocuronium Tachycardia 122 beats per minute
Cough
Difficult mask ventilation
After intubation-visual confirmation of tube placement No carbon dioxide detected on capnography
Airway pressures were elevated
SpO2 decreased to 80%
No carotid pulse detected CPR started
IV fluids administered
Increasing doses of epinephrine, initial 200 mcg, 800 mcg, 1 mg
Case Study-Continued
19 minutes into resuscitation
4 mg of epinephrine
2000 mL of Lactated Ringer’s
1500 mL of colloid
500 mg of sugammadex (6.5 mg/kg) administered during chest compressions
45 seconds after administration during chest compressions, patient opened her eyes and reached for the endotracheal tube
Blood pressure 111/56
Heart rate 126 beats minute
SpO2 97%
Patient was transferred to an off site intensive care unit
Within 30 minutes of arrival to the ICU patient was extubated and no vasopressor support was required
Patient was discharged 48 hours after the event with no additional complications and no recollection of the event
Questions??
References
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Cammu, G., Van Vlem, B., van den Heuvel, M., Stet, L., el Galta, R., Eloot, S., & Demeyer, I. (2012). Dialysability of sugammadex and its complex with rocuronium in intensive care patients with severe renal impairment. British journal of anaesthesia, 109(3), 382-390.
Carron, M., Baratto, F., Zarantonello, F., & Ori, C. (2016). Sugammadex for reversal of neuromuscular blockade: a retrospective analysis of clinical outcomes and cost-effectiveness in a single center. ClinicoEconomics and outcomes research: CEOR, 8, 43.
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References
Naguib, M. (2007). Sugammadex: Another milestone in clinical neuromuscular pharmacology. Anesthesia & Analgesia, 104(3), 575-581.
Peeters, P. A., van den Heuvel, M. W., van Heumen, E., Passier, P. C., Smeets, J. M., van Iersel, T., & Zwiers, A. (2010). Safety, tolerability and pharmacokinetics of sugammadex using single high doses (up to 96 mg/kg) in healthy adult subjects. Clinical drug investigation, 30(12), 867-874.
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