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SEDATION AND PARALYSIS IN ICU
BY DR.ABHINOB ROY
SENIOR RESIDENT
CRITICAL CARE MEDICINE
ICU Triad
Pain
Agitation
Delirium
What do we know about agitation/discomfort?
•Prevelance
- 50% incidence in those with length of stay >24 hours
• Primary cause
• Unrelieved pain
• Delirium
• Anxiety
• Sleep deprivation
ICU Agitation/discomfort sequelae
Immediate
• Patient-ventilator
dyssynchrony
• Increased oxygen
consumption
• Self (and health care
provider) injury
• Family anxiety
Long term
• Chronic anxiety disorders
• Post-traumatic stress
disorder.
Goals of sedation in ICU
• Patient comfort
• Control of Pain
• Anxiolysis and amnesia
• Blunting adverse autonomic and hemodynamic responses
• Facilitate nursing management
• Facilitate mechanical ventilation
• Avoid self-extubation
• Reduce oxygen consumption
Characteristics of an ideal sedation agent for
the ICU
• Lack of respiratory depression
• Analgesia, especially for surgical patients.
• Rapid onset, titrable, with short elimination half-time
• Sedation with ease of orientation and arousability
• Anxiolytic
• Haemodynamic stability
• The optimal level of sedation for most patients is what offers comfort
while allowing for interaction with the environment
Validated sedation assessment tools
• Richmond Agitation-sedation Scale[RASS]
• Ramsay sedation scale [RSS]
• Riker sedation- agitation Scale [SAS]
• Observer assessment of Alertness/Sedation scale
[OAASS]
• Motor activity assessment scale [MAAS]
Riker sedation-agitation scale
Daily goal is arousable, comfortable
sedation
Sedation needs to be protocolised and
titrated to goal:
• Ideal sedation goal : patient to be awake and
comfortable with minimal to no distress (eg 0
on RASS scale
Effect of this strategy on outcomes:
• 15% reduction in overall mortality,
• 1.73-day reduction in ICU length of stay
• 3.55-day reduction in hospital length of stay
• 31% reduction in tracheostomy
Administration
• Current practice favours intermittent bolus dose, daily interruption or
dose minimization titrated to lighter levels of sedation (RASS -2 to 0)
of continuous infusion
Sedativeoptions
How to sedate?
• Benzodiazepines
• Propofol
• Alpha 2 agonists
Sedation options: Benzodiazepines
(Midazolam and Lorazepam)
Features Midazolam Lorazepam
Onset of action 2-5 minutes 15-20 minutes
Elimination half-time 1-4 hours (Reves Et al 1985) 10-20 hours
Duration of action (after bolus) 1-2 hours 6-10 hours
Metabolism In liver by P450 enzymes In liver by glucoronidation
Active metabolite 1 hydroxymidazolam None
Loading dose 0.01-0.05 mg/kg 0.02-0.04 mg/kg (</= 2 mg)
Continuous infusion 0.02-0.1 mg/kg/hr 0.01-0.1 mg/kg/hr (</= 10 mg/hr)
Benefits
• Anxiolytic
• Amnestic
• Sedating
• Anticonvulsant
Risks
• Delirium
• No analgesia
• Excessive sedation : especially after long term sustained use
• Propylene glycol toxicity after parentral lorezepam
• Unexplained metabolic acidosis during prolonged (> 24 hours) infusion
Sedation option : Propofol
• Mechanism of action- GABA agonist
• Pharmacokinetics/ pharmacodynamics-
• Onset- 1-2 minutes
• Duration of action- 10 minutes
• Context sensitive half-time for infusion lasitng upto 8 hrs : < 40 minutes.
( Hughes Et al 1992)
• Metabolism-Hepatic ( glucoronidation)
• Elimination – renal
• Dose -25-75 mcg/kg/min
• Benefits
• Rapid onset and offset and easily titrated
• Hypnotic and anti emetic
• Anticonvulsant action
• Risks
• No analgesia
• Hypotension
• Hypertriglyceridemia
• Respiratory depression
• Propofol infusion syndrome
• Prolonged high dose infusion >75mcg/kg/min for >24 hrs ( Badr Et al 2001)
• Rhobdomyolysis
• Severe metabolic acidosis
• Cardiac failure
Sedation option : Dexmedetomedine
• Mechanism of action – alpha 2 receptor agonist( alpha 2:alpha 1
selectivity :: 1620:1)
• Pharmacokinetics and pharmacodynamics-
• Onset of action -5-10 minutes
• Elimination half time- Approx. 2 hrs
• Metabolism- in liver ( glucuronidation,hydroxylation,n-methylation)
• Dose
• loading –1mcg/kg over 10 minutes
• Maintainance- 0.2-0.7 mcg/kg/hr
• Benefits
• Doesn’t cause respiratory depression
• Arousal is maintained despite deep levels of sedation
• Risks
• Life threatening bradycardia
Other modality for sedation
• AnaConDa system- Inhalational anesthesia system designed in
Sweden.
• For use with ventlators in ICU.
• Better pharmacokinetic profile than than many i.v sedatives.
Significance of ICU delirium
• Prevelance –
The prevalence of delirium reported in medical and surgical ICU cohort
studies has varied from 20% to 80%, depending upon severity of illness
observed and diagnostic methods used. (Thomason JW Et al, 2008)
• Definition –
Disturbance of consciousness (ie, reduced clarity of awareness of the
environment) occurs, with reduced ability to focus, sustain, or shift attention.
(DSM-5 diagnostic criteria for delirium)
Types of delirium
• decreased responsiveness
• withdrawal
• apathy
Hypoactive
delirium
• agitation
• restlessness
• emotional lability
hyperactive
delirium
Validated tools for delirium assessment
•CAM ICU (Confusion Assessment method for the
intensive care unit)
•ICDSC (Intensive Care delirium screening
Checklist)
CAM -ICU
Content of consciousness is assessed (delirium is diagnosed) using the Confusion Assessment Method for the ICU
(CAM-ICU) [50,53]. When three of four diagnostic features are present (either features 1, 2, and 3, or features 1, 2,
and 4), delirium is diagnosed .
Pharmacological intervention : Haloperidol
• Mechanism of action : Dopamine receptor blocker
• Onset of action : 10-20 minutes
• Duration of action : 10-20 minutes
• Dose
• Mild anxiety 0.5 -2 mg
• Moderate anxiety 5-10 mg
• Severe anxiety 10-20 mg
• REDUCE trial conducted across 21 ICU in Netherland showed Prophylactic
treatment with 2 mg Haloperidol 8 hourly did not prevent the onset of
delirium (33% 2 mg Haloperidol vs. 33% Placebo, difference 0.4%, 95% CI,
−4.6% to 5.4%) and did not alter delirium/coma-free days (median
difference, 0 days, IQR 0 to 0 days)
BENEFITS
• Hemodynamic neutrality
• No respiratory depression
Adverse effects
• QTc prolongation and torsades pointes
• Extrapyramidal side effects : less common when given intravenously
Atypical antipsychotics : Quetiapine,
Olanzepine,Risperidone, Ziprasidone
One prospective randomized study showing equal efficacy of
olanzapine to haloperidol with less extra pyramidal symptoms.
2018 Pain ,Agitaion/sedation, Delirium, Immobility
and Sleep disruption (PADIS) guideline
-SCCM
• Focus – on improving post- ICU outcomes.
• Investigating –
sedation delivery paradigm ( light vs deep)
specific sedative medications
Sedation delivery paradigm
- light vs deep sedation
•Evidence – 8 RCTs and 3 Observational studies
• 90 days mortality ( 2RCTs, 324 patients)
• Not significant. RR 1.01 (95%CI, 0.80 to 1.27; low quality)
• Self extubation (4 RCTs, 546pts)
• Not significant RR 1.29 (95% CI , 0.58 to 2.88;low quality)
• Light sedation was not associated with reduction in
• PTSD (2 RCTs, 62 pts) RR 0.67 (95% CI, 0.12 to3.79)
• Depression (2 RCTs, 128 pts) , RR 0.76 (95% CI ,0.10 to 5.58)
• Delirium ( 2 RCTs , 140 pts) RR 0.96 ( (%% CI, 0.80 to 1.16)
• Tracheostomy rate (1 RCT & 1 Observational , 452 pts)
• Reduced RR 0.57 (95 % CI , 0.41 to 0.80)
• Time to extubation ( 3 RCTs 453 pts ;low quality)
• Associated with shorter time , MD – 0.77 days ( 95% CI , -0.24to 0.50)
• Time to extubation ( 3 observation, 1524 pts ; low quality)
• Associated with shorter time MD- 3.46 days (95% CL, -5.70 to -1.23)
Recommendation
• Light sedation ( vs deep sedation ) is recommended in critically ill ,
mechanically ventilated adults ( low quality of evidence)..
Choice of sedative: medical and surgical
patients ( non cardiac surgery)
• For sedation in critically ill and mechanically ventilated adults
comparison of the following drugs have been done-
Propofol vs benzodiazepines
Dexmed vs benzodiazepines
Dexmed vs propofol
• Propofol vs benzodiazepines
• Time to extubation ( 10 RCTs, 423 pts )
• Reduced by 11.6 hr ( 95%CI , -15.6 to 7.6 ; low quality)
• Time to light sedation (10 RCTs, 357 pts)
• Reduced by 7.2 hr ( 95 % CI , -8.9to -5.5 ;low quality )
• Dexmed vs Benzodiazepines
• No significant benefit of Dexmed ovr BZD infusion for-
• Duration of mechanical ventilation
• ICU length of stay
• Risk of delirium
• Dexmed vs Propofol
• No significant difference in time to extubation (3 RCTs , 850 pts)
Recommendation
• Either Profopol or Dexmed is suggested over benzodiazepines for
sedation in critically ill, mechanically ventilated adults
In the existing studies for this recommendation –
Bzodiazepines mostly given as infusion rather than bolus.
Recommendation
•Routinely using Haloperidol and antipsychotic to
treat delirium not suggested (low quality
evidence)
Neuromuscular Blockade (NMB) (Paralytics) in the
Adult ICU
• Used most often acutely (single dose) to facilitate intubation or
selected procedures
• Issues
NO ANALGESIC or SEDATIVE properties
If administering for prolonged period (> 6 - 12 hours), use an objective monitor
to assess degree of paralysis.
Indications
• Facilitate mechanical ventilation, especially with abdominal
compartment syndrome, high airway pressures, and dyssynchrony
• Assist in control of elevated intracranial pressures
• Reduce oxygen consumption
• Prevent muscle spasm in neuroleptic malignant syndrome, tetanus, etc.
Two classes of NMBS
Depolarizers
-Succhinylcholine
- Prolonged binding to acetylcholine receptor to produce
depolarization (fasciculations) and subsequent desensitization so that the
motor endplate cannot respond to further stimulation right away
Nondepolarizers
- Blocks acetylcholine from postsynaptic receptor competitively
- Benzylisoquinoliniums - Curare, atracurium, cisatracurium, mivacurium,
doxacuronium
- - Aminosteroids - Pancuronium, vecuronium, rococuronium
Quick Onset Muscle Relaxants for Intubation
Patients with aspiration risk need rapid onset paralysis for intubation.
• Rocuronium
Duration 60 minutes
Dose is 1.2 mg/kg to have intubating conditions in 45 seconds
Succinylcholine
Duration - 10 minutes
Dose is 1 - 2 mg/kg to have intubating conditions in 30 seconds
Potential Contraindications of Succinylcholine
• Increases serum potassium by 0.5 to 1 meq/liter in all patients
• Can cause bradycardia, anaphylaxis, and muscle pain
• Potentially increases intragastric, intraocular, and intracranial pressure
• Severely elevates potassium due to proliferation of extrajunctional
receptors in patients with denervation injury, stroke, trauma, or burns
of more than 24 hours
Nondepolarizing muscle relaxants
Pancuronium, vecuronium,atra/cisatracurium
All rapid onset (2 - 3 minutes)
• Differ in duration (pancuronium >50 minutes, vecuronium,atra/
cisatracurium 20 to 50 minutes)
• Differ in route of elimination (pancuronium = renal/liver, vecuronium
= renal/bile, atra/cisatracurium = Hoffman degradation)
Infusion doses
• Pancuronium 0.048 - 0.1 mg/kg/h (Greenberg 2013)
• Vecuronium 0.048 - 0.72 mg/kg/h
• Atracurium 0.24 – 1.2 mg/kg/h (Murray 2002)
• Cisatracurium 0.06- 0.18 mg/kg/hr (Greenberg 2013)
Other distinguishing features
• Pancuronium causes tachycardia
• Vecuronium has neutral effects on hemodynamics but has several renally
excreted active metabolites
• Elimination of atra/cisatracurium is not affected by organ dysfunction
Monitoring NMBAs
• Goal - To prevent prolonged weakness associated with excessive NMBA
administration.
• Methods
Peripheral nerve stimulation
• Train of four response consists of four stimulae of 2 Hz, 0.2 msec in duration,
and 500 msec apart.
• 4 twitches seen 0-75% receptors are blocked
• 3 twitches seen at least 75% receptors are blocked
• 2 twitches seen 80% of receptors are blocked
• 1 twitch 90% receptors are blocked
For monitoring sedation during paralysis BIS (Bispectral index) is used.
THANK YOU

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ICU Sedation and Paralysis Guide

  • 1. SEDATION AND PARALYSIS IN ICU BY DR.ABHINOB ROY SENIOR RESIDENT CRITICAL CARE MEDICINE
  • 3. What do we know about agitation/discomfort? •Prevelance - 50% incidence in those with length of stay >24 hours • Primary cause • Unrelieved pain • Delirium • Anxiety • Sleep deprivation
  • 4. ICU Agitation/discomfort sequelae Immediate • Patient-ventilator dyssynchrony • Increased oxygen consumption • Self (and health care provider) injury • Family anxiety Long term • Chronic anxiety disorders • Post-traumatic stress disorder.
  • 5. Goals of sedation in ICU • Patient comfort • Control of Pain • Anxiolysis and amnesia • Blunting adverse autonomic and hemodynamic responses • Facilitate nursing management • Facilitate mechanical ventilation • Avoid self-extubation • Reduce oxygen consumption
  • 6. Characteristics of an ideal sedation agent for the ICU • Lack of respiratory depression • Analgesia, especially for surgical patients. • Rapid onset, titrable, with short elimination half-time • Sedation with ease of orientation and arousability • Anxiolytic • Haemodynamic stability • The optimal level of sedation for most patients is what offers comfort while allowing for interaction with the environment
  • 7. Validated sedation assessment tools • Richmond Agitation-sedation Scale[RASS] • Ramsay sedation scale [RSS] • Riker sedation- agitation Scale [SAS] • Observer assessment of Alertness/Sedation scale [OAASS] • Motor activity assessment scale [MAAS]
  • 8.
  • 10. Daily goal is arousable, comfortable sedation Sedation needs to be protocolised and titrated to goal: • Ideal sedation goal : patient to be awake and comfortable with minimal to no distress (eg 0 on RASS scale
  • 11. Effect of this strategy on outcomes: • 15% reduction in overall mortality, • 1.73-day reduction in ICU length of stay • 3.55-day reduction in hospital length of stay • 31% reduction in tracheostomy
  • 12. Administration • Current practice favours intermittent bolus dose, daily interruption or dose minimization titrated to lighter levels of sedation (RASS -2 to 0) of continuous infusion
  • 13. Sedativeoptions How to sedate? • Benzodiazepines • Propofol • Alpha 2 agonists
  • 14. Sedation options: Benzodiazepines (Midazolam and Lorazepam) Features Midazolam Lorazepam Onset of action 2-5 minutes 15-20 minutes Elimination half-time 1-4 hours (Reves Et al 1985) 10-20 hours Duration of action (after bolus) 1-2 hours 6-10 hours Metabolism In liver by P450 enzymes In liver by glucoronidation Active metabolite 1 hydroxymidazolam None Loading dose 0.01-0.05 mg/kg 0.02-0.04 mg/kg (</= 2 mg) Continuous infusion 0.02-0.1 mg/kg/hr 0.01-0.1 mg/kg/hr (</= 10 mg/hr)
  • 15. Benefits • Anxiolytic • Amnestic • Sedating • Anticonvulsant Risks • Delirium • No analgesia • Excessive sedation : especially after long term sustained use • Propylene glycol toxicity after parentral lorezepam • Unexplained metabolic acidosis during prolonged (> 24 hours) infusion
  • 16. Sedation option : Propofol • Mechanism of action- GABA agonist • Pharmacokinetics/ pharmacodynamics- • Onset- 1-2 minutes • Duration of action- 10 minutes • Context sensitive half-time for infusion lasitng upto 8 hrs : < 40 minutes. ( Hughes Et al 1992) • Metabolism-Hepatic ( glucoronidation) • Elimination – renal
  • 17. • Dose -25-75 mcg/kg/min • Benefits • Rapid onset and offset and easily titrated • Hypnotic and anti emetic • Anticonvulsant action • Risks • No analgesia • Hypotension • Hypertriglyceridemia • Respiratory depression • Propofol infusion syndrome • Prolonged high dose infusion >75mcg/kg/min for >24 hrs ( Badr Et al 2001) • Rhobdomyolysis • Severe metabolic acidosis • Cardiac failure
  • 18. Sedation option : Dexmedetomedine • Mechanism of action – alpha 2 receptor agonist( alpha 2:alpha 1 selectivity :: 1620:1) • Pharmacokinetics and pharmacodynamics- • Onset of action -5-10 minutes • Elimination half time- Approx. 2 hrs • Metabolism- in liver ( glucuronidation,hydroxylation,n-methylation) • Dose • loading –1mcg/kg over 10 minutes • Maintainance- 0.2-0.7 mcg/kg/hr
  • 19. • Benefits • Doesn’t cause respiratory depression • Arousal is maintained despite deep levels of sedation • Risks • Life threatening bradycardia
  • 20. Other modality for sedation • AnaConDa system- Inhalational anesthesia system designed in Sweden. • For use with ventlators in ICU. • Better pharmacokinetic profile than than many i.v sedatives.
  • 21. Significance of ICU delirium • Prevelance – The prevalence of delirium reported in medical and surgical ICU cohort studies has varied from 20% to 80%, depending upon severity of illness observed and diagnostic methods used. (Thomason JW Et al, 2008) • Definition – Disturbance of consciousness (ie, reduced clarity of awareness of the environment) occurs, with reduced ability to focus, sustain, or shift attention. (DSM-5 diagnostic criteria for delirium)
  • 22. Types of delirium • decreased responsiveness • withdrawal • apathy Hypoactive delirium • agitation • restlessness • emotional lability hyperactive delirium
  • 23.
  • 24. Validated tools for delirium assessment •CAM ICU (Confusion Assessment method for the intensive care unit) •ICDSC (Intensive Care delirium screening Checklist)
  • 25. CAM -ICU Content of consciousness is assessed (delirium is diagnosed) using the Confusion Assessment Method for the ICU (CAM-ICU) [50,53]. When three of four diagnostic features are present (either features 1, 2, and 3, or features 1, 2, and 4), delirium is diagnosed .
  • 26. Pharmacological intervention : Haloperidol • Mechanism of action : Dopamine receptor blocker • Onset of action : 10-20 minutes • Duration of action : 10-20 minutes • Dose • Mild anxiety 0.5 -2 mg • Moderate anxiety 5-10 mg • Severe anxiety 10-20 mg • REDUCE trial conducted across 21 ICU in Netherland showed Prophylactic treatment with 2 mg Haloperidol 8 hourly did not prevent the onset of delirium (33% 2 mg Haloperidol vs. 33% Placebo, difference 0.4%, 95% CI, −4.6% to 5.4%) and did not alter delirium/coma-free days (median difference, 0 days, IQR 0 to 0 days)
  • 27. BENEFITS • Hemodynamic neutrality • No respiratory depression Adverse effects • QTc prolongation and torsades pointes • Extrapyramidal side effects : less common when given intravenously
  • 28. Atypical antipsychotics : Quetiapine, Olanzepine,Risperidone, Ziprasidone One prospective randomized study showing equal efficacy of olanzapine to haloperidol with less extra pyramidal symptoms.
  • 29. 2018 Pain ,Agitaion/sedation, Delirium, Immobility and Sleep disruption (PADIS) guideline -SCCM • Focus – on improving post- ICU outcomes. • Investigating – sedation delivery paradigm ( light vs deep) specific sedative medications
  • 30. Sedation delivery paradigm - light vs deep sedation •Evidence – 8 RCTs and 3 Observational studies
  • 31. • 90 days mortality ( 2RCTs, 324 patients) • Not significant. RR 1.01 (95%CI, 0.80 to 1.27; low quality) • Self extubation (4 RCTs, 546pts) • Not significant RR 1.29 (95% CI , 0.58 to 2.88;low quality) • Light sedation was not associated with reduction in • PTSD (2 RCTs, 62 pts) RR 0.67 (95% CI, 0.12 to3.79) • Depression (2 RCTs, 128 pts) , RR 0.76 (95% CI ,0.10 to 5.58) • Delirium ( 2 RCTs , 140 pts) RR 0.96 ( (%% CI, 0.80 to 1.16)
  • 32. • Tracheostomy rate (1 RCT & 1 Observational , 452 pts) • Reduced RR 0.57 (95 % CI , 0.41 to 0.80) • Time to extubation ( 3 RCTs 453 pts ;low quality) • Associated with shorter time , MD – 0.77 days ( 95% CI , -0.24to 0.50) • Time to extubation ( 3 observation, 1524 pts ; low quality) • Associated with shorter time MD- 3.46 days (95% CL, -5.70 to -1.23)
  • 33. Recommendation • Light sedation ( vs deep sedation ) is recommended in critically ill , mechanically ventilated adults ( low quality of evidence)..
  • 34. Choice of sedative: medical and surgical patients ( non cardiac surgery) • For sedation in critically ill and mechanically ventilated adults comparison of the following drugs have been done- Propofol vs benzodiazepines Dexmed vs benzodiazepines Dexmed vs propofol
  • 35. • Propofol vs benzodiazepines • Time to extubation ( 10 RCTs, 423 pts ) • Reduced by 11.6 hr ( 95%CI , -15.6 to 7.6 ; low quality) • Time to light sedation (10 RCTs, 357 pts) • Reduced by 7.2 hr ( 95 % CI , -8.9to -5.5 ;low quality ) • Dexmed vs Benzodiazepines • No significant benefit of Dexmed ovr BZD infusion for- • Duration of mechanical ventilation • ICU length of stay • Risk of delirium • Dexmed vs Propofol • No significant difference in time to extubation (3 RCTs , 850 pts)
  • 36. Recommendation • Either Profopol or Dexmed is suggested over benzodiazepines for sedation in critically ill, mechanically ventilated adults In the existing studies for this recommendation – Bzodiazepines mostly given as infusion rather than bolus.
  • 37. Recommendation •Routinely using Haloperidol and antipsychotic to treat delirium not suggested (low quality evidence)
  • 38. Neuromuscular Blockade (NMB) (Paralytics) in the Adult ICU • Used most often acutely (single dose) to facilitate intubation or selected procedures • Issues NO ANALGESIC or SEDATIVE properties If administering for prolonged period (> 6 - 12 hours), use an objective monitor to assess degree of paralysis.
  • 39. Indications • Facilitate mechanical ventilation, especially with abdominal compartment syndrome, high airway pressures, and dyssynchrony • Assist in control of elevated intracranial pressures • Reduce oxygen consumption • Prevent muscle spasm in neuroleptic malignant syndrome, tetanus, etc.
  • 40. Two classes of NMBS Depolarizers -Succhinylcholine - Prolonged binding to acetylcholine receptor to produce depolarization (fasciculations) and subsequent desensitization so that the motor endplate cannot respond to further stimulation right away Nondepolarizers - Blocks acetylcholine from postsynaptic receptor competitively - Benzylisoquinoliniums - Curare, atracurium, cisatracurium, mivacurium, doxacuronium - - Aminosteroids - Pancuronium, vecuronium, rococuronium
  • 41. Quick Onset Muscle Relaxants for Intubation Patients with aspiration risk need rapid onset paralysis for intubation. • Rocuronium Duration 60 minutes Dose is 1.2 mg/kg to have intubating conditions in 45 seconds Succinylcholine Duration - 10 minutes Dose is 1 - 2 mg/kg to have intubating conditions in 30 seconds
  • 42. Potential Contraindications of Succinylcholine • Increases serum potassium by 0.5 to 1 meq/liter in all patients • Can cause bradycardia, anaphylaxis, and muscle pain • Potentially increases intragastric, intraocular, and intracranial pressure • Severely elevates potassium due to proliferation of extrajunctional receptors in patients with denervation injury, stroke, trauma, or burns of more than 24 hours
  • 43. Nondepolarizing muscle relaxants Pancuronium, vecuronium,atra/cisatracurium All rapid onset (2 - 3 minutes) • Differ in duration (pancuronium >50 minutes, vecuronium,atra/ cisatracurium 20 to 50 minutes) • Differ in route of elimination (pancuronium = renal/liver, vecuronium = renal/bile, atra/cisatracurium = Hoffman degradation)
  • 44. Infusion doses • Pancuronium 0.048 - 0.1 mg/kg/h (Greenberg 2013) • Vecuronium 0.048 - 0.72 mg/kg/h • Atracurium 0.24 – 1.2 mg/kg/h (Murray 2002) • Cisatracurium 0.06- 0.18 mg/kg/hr (Greenberg 2013) Other distinguishing features • Pancuronium causes tachycardia • Vecuronium has neutral effects on hemodynamics but has several renally excreted active metabolites • Elimination of atra/cisatracurium is not affected by organ dysfunction
  • 45. Monitoring NMBAs • Goal - To prevent prolonged weakness associated with excessive NMBA administration. • Methods Peripheral nerve stimulation • Train of four response consists of four stimulae of 2 Hz, 0.2 msec in duration, and 500 msec apart. • 4 twitches seen 0-75% receptors are blocked • 3 twitches seen at least 75% receptors are blocked • 2 twitches seen 80% of receptors are blocked • 1 twitch 90% receptors are blocked For monitoring sedation during paralysis BIS (Bispectral index) is used.