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Sedation In the Neuro-ICU
           2009

   PJ Papadakos MD FCCM
   Director CCM
   Professor Anesthesiology,
   Surgery and Neurosurgery
   Rochester NY USA
University of Rochester
Developed the first use guidelines for evaluation of
Neurosurgery patients with Propofol (Ireland et al.,
Proceedings American Association of Neurological
Surgeons . 1992)
Development of Fast Tracking for Open Heart
Surgery. 1991
Development of use protocols for sedation in Critically
ill patients 1993.
Development of guidelines for Dexmedetomidine in
Burn patients 2001
University of Rochester
Developed the first use guidelines for evaluation of
Neurosurgery patients with Propofol (Ireland et al.,
Proceedings American Association of Neurological
Surgeons . 1992)
Development of Fast Tracking for Open Heart
Surgery. 1991
Development of use protocols for sedation in Critically
ill patients 1993.
Development of guidelines for Dexmedetomidine in
Burn patients 2001
Articles on Sedation
Several Practice Standards
   are in the Literature

    In 2001 a large conference was held:




Crit Care Med 2002 Vol 30 #1
ICU Sedation

ICU sedation is a complex clinical
problem
Current therapeutic approaches all
have potential adverse side effects
Agitated patients are often
hypertensive, increase stress
hormones, and require more intensive
nursing care
Goals of Sedation in the
          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, titratable, with a short
elimination half-time
Sedation with ease of orientation and
arousability
Anxiolytic
Hemodynamic stability
Agitated Patients
Can injure themselves or others
    Self-extubation, decannulation, wound dehiscence


    Peripheral oxygen consumption
    Risks of hypoxemia, organ ischemia


    Physiologic stress
    Change in immune response, wound healing,

    coagulation, release cytokines
Require more intensive nursing care
    Restraints

    Risks of excessive sedation

Sedative Drugs
Most commonly used
  drugs in the ICU
Why do we use these
        drugs
Pain
Agitation
Anxiety
Keep patient intubated
Protect Patient from Harm
?Cytokine Modulation?
Causes of Anxiety
Factors Provoking
                   Anxiety                       Pain
                                                                     Fear
                          Memory Loss

                                                                                  Sleep Deprivation
                    Confusion


Inconsiderate Providers                                                             Loss of Control

                                                 ICU
Chemical/Physiologic
                                              Psychosis                              Surgical Stress
   Imbalance

          Medications                                                                Temperature


                 Alarms                                                           Noises


         Mechanical Devices                                              Lights
                                        Nonchanging Environment

Tesar, Stern. J Intensive Care Med. 1986;1:137-148. Harvey. Am J Crit Care. 1996;5:7-16.
Crippen. Crit Care Clin. 1990;6:369-392.
To Use these drugs



We need a common language to
speak to all levels of care givers
Sedation Scales



Should be used in every unit.
Faces Pain Rating Scale


       0                                              3               4             5
                       1               2



   0       1       2       3       4       5      6       7       8       9       10

  No                                                                             Worst
                                       Moderate
  pain                                                                        possible pain
                                         pain


Adapted with permission from Chambers, Craig. Pain. 1998;78:29.
Sriwatanakul et al. Clin Pharmacol Ther. 1982;32:143-148.
Ramsay Sedation Scale
Score                        Definition

1        Anxious, agitated, or restless
2        Cooperative, oriented, and tranquil
3        Responds to commands
4        Asleep, but with brisk response to light glabellar tap
         or loud auditory stimuli
5        Asleep, sluggish response to light glabellar tap or
         loud auditory stimuli
6        Asleep, no response
Adapted with permission from Ramsay et al. BMJ. 1974;2:656-659.
SAS: Sedation-Agitation
                     Scale Description
    Score Definition
    7   Dangerous agitation    Striking staff, thrashing
    6 Very agitated            Does not calm, needs
    restraints
    5   Agitated               Calms with verbal instructions
    4   Calm and cooperative   Follows commands
    3   Sedated                Difficult to arouse
    2   Very sedated           Does not follow commands
    1 Unarousable              No response to noxious
    stimuli
.
Drugs to Use:
Pharmacologic Agents

Opioids1
   Morphine sulfate
 
  Fentanyl and Remifentanyl

Benzodiazepines1
   Lorazepam
 
  Midazolam

Sedative/hypnotics1
     Propofol
 

Butyrophenones1
     Haloperidol
 

   Agonists2
 2
     Dexmedetomidine
 
Benzodiazepines:
       Mechanisms of Action
      Benzodiazepines
            GABAA receptor modulation in CNS1
        

            Facilitate binding of GABA1
        

            Hyperpolarize cells, more resistant to
        

            excitation
            Receptors mainly postsynaptic
        



1. Lerch, Park. Br Med Bull. 1999;55:76-95.
Benzodiazepines:
           Pharmacodynamics
      Amnesia
      Sedation/anxiolysis
      Anticonvulsant
      Relief of muscle spasm

Lerch, Park. Br Med Bull. 1999;55:89.
Lorazepam: Clinical
                 Effects
      Sedation, anxiolysis, and amnesia1
      Preferred for prolonged sedation2
      Slower onset of action than
      midazolam2,3
      Propylene glycol toxicity with higher
      doses1
      Less hypotension than with midazolam2
      Retrograde and anterograde amnesia4
1. Lerch, Park. Br Med Bull. 1999;55, 90. 2. Shafer. Crit Care Med. 1998;26:952-953.
3. Wagner, O’Hara. Clin Pharmacokinet. 1997;33:430, 434. 4. Harvey. Am J Crit Care. 1996;5:11.
Benzodiazepines:
                Reversal Agents
      Flumazenil
            Transiently antagonizes the benzodiazepine
        

            component of ventilatory depression and
            sedation during use with opioids
            Reverses CNS and circulatory side effects of
        

            benzodiazepines within 2 minutes
            Useful for diagnostic evaluation
        




Stoelting. Pharmacology and Physiology in Anesthetic Practice. 3rd ed. 1999:138.
Benzodiazepines
  Advantages                                     Limitations
  • Amnesia1                                     • Weaning prolonged2,3
  • Anxiolysis1                                  • Polyethylene glycol toxicity3
  • Sedation1                                    • Respiratory depression2,4
                                                 • Hypotension2
                                                 • Lack of analgesia4
                                                 • Oversedation/deep sedation2
                                                 • Dependence/tolerance2
                                                 • Paradoxic agitation2

1. Pepperman. Care of the Critically Ill. 1989;5:197. 2. Harvey. Am J Crit Care. 1996;5:10, 11.
3. Lerch, Park. Br Med Bull. 1999;55:89, 90. 4. Crippen. Crit Care Clin. 1990;6:380.
Propofol:
       Mechanisms of Action
      Not well-understood
      GABAA receptor modulation is most
      likely




Davies. Can J Physiol Pharmacol. 1998;76:46.
Propofol:
           Pharmacodynamics
      Sedation/anesthesia1
      Decreases ICP1,2
      Decreases SNS activity1,2
      Cardiovascular depression1,3
      Decreases ventilation time1

1. Wagner, O’Hara. Clin Pharmacokinet. 1997;33:434, 436. 2. Harvey. Am J Crit Care. 1996;5:12.
3. Lerch, Park. Br Med Bull. 1999;55:90,
Propofol: Clinical Effects
     Anesthesia and sedation1
     Rapid onset of action1,2
     Very short half-life2
     Decrease in BP and HR from sympathetic
     effects1
     Decreases ventilation time3,4
     Time to extubation faster than with midazolam3,4
1. Lerch, Park. Br Med Bull. 1999:55:90. 2. Harvey. Am J Crit Care. 1996;5:7-16. 3. Wagner,
O’Hara. Clin Pharmacokinet. 1997;33:434. 4. Ostermann et al. JAMA. 2000;283:1457.
Propofol
                                           Limitations
 Advantages
                                           • Respiratory depression (enhanced
 • Sedation1
                                             by opioids)1
 • Hypnosis1
                                           • Hypotension1
 • Anxiolysis1
                                           • Decreased contractility2
 • Muscle relaxation1                      • Lack of analgesia3
 •  ICP1                                  • Hypertriglyceridemia1
 •  Cerebral metabolic                    • Preservative issues4
   rate1                                   • Potential for infection necessitates
                                             need for regular changing of lines5
 • Relief of bronchospasm1

1. Harvey. Am J Crit Care.1996;5:7-16. 2. Lerch, Park. Br Med Bull. 1999;55:90. 3. Wagner,
O’Hara. Clin Pharmacokinet. 1997;33:435. 4. Propofol [package insert]. 5. Prielipp et al. Crit
Care Clin. 1995;11:986.
The Stress Response
and Immunomodulation
In Sedated ICU Patients
Crit Care Med 2006 Vol.34 #2 453-460
Sedation



   May affect Patient outcome
through affect on cytokine release
Propofol with EDTA



   There is a difference
Herr et al, Intensive
Care Medicine; 2000; 26
In a surgical ICU
Serious Adverse Events 25 vs 8%
Mortality 17.5 vs 2%
11 deaths in plain propofol vs 1 among
the propofol with EDTA
Propofol with EDTA
Boost lipoidal antixidant defenses in
tissue
Chelator of heavy metals Iron is
important for cytokine secretion
Decrease Trace elements
Decreased Free Radicals
What we wish to
       investigate
Do different drugs affect levels of
cytokines released by the lung
Can they protect the compartment of
the lung from systemic cytokine release
Do they prevent the release of cytokines
from the lung
How does Propofol
with EDTA Affect
Cytokine Levels


   Erasmus MC Rotterdam
Papadakos, Lachmann Haitsma
         ATS 2006
Propofol with EDTA affect
    on electrolytes:
Dexmedetomidine
Physiology of alpha
     receptor
Peripheral         Receptors
               2




                             A
                        2A




           B
      2B
                   2A
Central Sites of Action:
       2 Agonists


               Sedation
               Anxiolysis
               Sympathetic inhibition



               Analgesia
Agonists
              2
                        Dexmedetomidine
Clonidine
                         Selectivity: 2: 1
 Selectivity: 2: 1
                         1620:13
 200:11
 t1/2 10 hrs1            t1/2 2 hrs3
 PO, patch, epidural2    Intravenous3
 Antihypertensive1       Sedative-analgesic3
 Analgesic adjunct1      Primary sedative
 IV formulation not
                         Only IV 2 available for
 available in US
                         use in the US
Clinical Effects of                                               2
                Agonists
      Sedation/hypnosis1
      Anxiolysis1
      Analgesia1
      Decreased sympathetic activity1
      Decreased BP and HR2
      Vasoconstriction at high doses1
Kamibayashi, Maze. Anesthesiology. 2000;93:1345-1349. 2. Wagner, O’Hara. Clin
Pharmacokinet. 1997;33:426-453.
Dexmedetomidine:
Indications
  Sedation of initially intubated and MV patients
   during treatment in the ICU
Contraindications
 Caution in patients with advanced heart block

Drug interactions
 Vagal effects can be counteracted by IV
  administration of anticholinergic agents
Disease effecting clearance
 Clearance is lower in patients with hepatic
   impairment
Dexmedetomidine
Advantages                                       Limitations
• Has sedative, analgesic,                       • May reduce HR and BP (caution in
  and anxiolytic effects1                          hypovolemia, shock, and heart
                                                   block)4
• Respiratory stability2
                                                 • Potentiates effects of opioids,
• Predictable hemodynamic
                                                   sedatives and anesthetics4
  response1
                                                 • Dry mouth4
• Arousable and oriented patient3
                                                 • Vasoconstriction at high dose4
• No need to discontinue before
  extubation4
• Antishivering5


1. Aantaa et al. Drugs of the Future. 1993;18:49-56. 2. Frangoulidou et al. In: Redefining Sedation.
1998:40-50. 3. Mantz, Singer. In: Redefining Sedation. 1998:23-29. 4. Precedex™ [package
insert]. 5. Kamibayashi, Maze. Anesthesiology. 2000;93:1345-1349.
Other interesting
Drugs
COX – 2 Inhibitors



  Prostaglandin Modulation
Recent Data:
      May have important role in treatment of
      Septic Patients
      Normalization of Endotoxin
      Attenuation of macrophage depression
      of hematopoietic proliforation
      Augmentation of white cell count
Shoup M et al J Trauma Inj Inf Crit Care 1998;45:215-219
Several Studies in Burn
         Injury
Highly affective in murine burn injury
80% increase in COX-2 protein
compared to control at 4 hours post
injury
COX-2 Drugs have
however been recalled
for increased Cardiac
         Risk
Neurontin



  Increases GABA Levels
Neurontin
Decreases requirement of narcotics
Decreases Alcohol Withdrawal
We now use this Drug
commonly in Withdrawal
     Syndromes
The Fine Balance in
  Patient Comfort
The Fine Balance in
  Patient Comfort

                 Anxiety
                Agitation
              Hypertension
               Tachycardia
               Arrhythmias
            Myocardial ischemia
             Wound disruption
              Patient injury
The Fine Balance in
      Patient Comfort
Depersonalization
Delayed emergence
Delayed weaning
 Pressure injury
  Venous stasis
 Muscle atrophy
  Increased cost
Sedation
Modulates immune
system
Provides comfort
Modulates Length of
Stay
Affects health care
costs
How to manage Sedation in Neuro ICU

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How to manage Sedation in Neuro ICU

  • 1. Sedation In the Neuro-ICU 2009 PJ Papadakos MD FCCM Director CCM Professor Anesthesiology, Surgery and Neurosurgery Rochester NY USA
  • 2. University of Rochester Developed the first use guidelines for evaluation of Neurosurgery patients with Propofol (Ireland et al., Proceedings American Association of Neurological Surgeons . 1992) Development of Fast Tracking for Open Heart Surgery. 1991 Development of use protocols for sedation in Critically ill patients 1993. Development of guidelines for Dexmedetomidine in Burn patients 2001
  • 3. University of Rochester Developed the first use guidelines for evaluation of Neurosurgery patients with Propofol (Ireland et al., Proceedings American Association of Neurological Surgeons . 1992) Development of Fast Tracking for Open Heart Surgery. 1991 Development of use protocols for sedation in Critically ill patients 1993. Development of guidelines for Dexmedetomidine in Burn patients 2001
  • 5. Several Practice Standards are in the Literature In 2001 a large conference was held: Crit Care Med 2002 Vol 30 #1
  • 6. ICU Sedation ICU sedation is a complex clinical problem Current therapeutic approaches all have potential adverse side effects Agitated patients are often hypertensive, increase stress hormones, and require more intensive nursing care
  • 7. Goals of Sedation in the 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
  • 8. Characteristics of an Ideal Sedation Agent for the ICU Lack of respiratory depression Analgesia, especially for surgical patients Rapid onset, titratable, with a short elimination half-time Sedation with ease of orientation and arousability Anxiolytic Hemodynamic stability
  • 9. Agitated Patients Can injure themselves or others Self-extubation, decannulation, wound dehiscence  Peripheral oxygen consumption Risks of hypoxemia, organ ischemia  Physiologic stress Change in immune response, wound healing,  coagulation, release cytokines Require more intensive nursing care Restraints  Risks of excessive sedation 
  • 11. Most commonly used drugs in the ICU
  • 12. Why do we use these drugs Pain Agitation Anxiety Keep patient intubated Protect Patient from Harm ?Cytokine Modulation?
  • 14. Factors Provoking Anxiety Pain Fear Memory Loss Sleep Deprivation Confusion Inconsiderate Providers Loss of Control ICU Chemical/Physiologic Psychosis Surgical Stress Imbalance Medications Temperature Alarms Noises Mechanical Devices Lights Nonchanging Environment Tesar, Stern. J Intensive Care Med. 1986;1:137-148. Harvey. Am J Crit Care. 1996;5:7-16. Crippen. Crit Care Clin. 1990;6:369-392.
  • 15. To Use these drugs We need a common language to speak to all levels of care givers
  • 16. Sedation Scales Should be used in every unit.
  • 17. Faces Pain Rating Scale 0 3 4 5 1 2 0 1 2 3 4 5 6 7 8 9 10 No Worst Moderate pain possible pain pain Adapted with permission from Chambers, Craig. Pain. 1998;78:29. Sriwatanakul et al. Clin Pharmacol Ther. 1982;32:143-148.
  • 18. Ramsay Sedation Scale Score Definition 1 Anxious, agitated, or restless 2 Cooperative, oriented, and tranquil 3 Responds to commands 4 Asleep, but with brisk response to light glabellar tap or loud auditory stimuli 5 Asleep, sluggish response to light glabellar tap or loud auditory stimuli 6 Asleep, no response Adapted with permission from Ramsay et al. BMJ. 1974;2:656-659.
  • 19. SAS: Sedation-Agitation Scale Description Score Definition 7 Dangerous agitation Striking staff, thrashing 6 Very agitated Does not calm, needs restraints 5 Agitated Calms with verbal instructions 4 Calm and cooperative Follows commands 3 Sedated Difficult to arouse 2 Very sedated Does not follow commands 1 Unarousable No response to noxious stimuli .
  • 21. Pharmacologic Agents Opioids1 Morphine sulfate   Fentanyl and Remifentanyl Benzodiazepines1 Lorazepam   Midazolam Sedative/hypnotics1 Propofol  Butyrophenones1 Haloperidol  Agonists2 2 Dexmedetomidine 
  • 22.
  • 23. Benzodiazepines: Mechanisms of Action Benzodiazepines GABAA receptor modulation in CNS1  Facilitate binding of GABA1  Hyperpolarize cells, more resistant to  excitation Receptors mainly postsynaptic  1. Lerch, Park. Br Med Bull. 1999;55:76-95.
  • 24. Benzodiazepines: Pharmacodynamics Amnesia Sedation/anxiolysis Anticonvulsant Relief of muscle spasm Lerch, Park. Br Med Bull. 1999;55:89.
  • 25. Lorazepam: Clinical Effects Sedation, anxiolysis, and amnesia1 Preferred for prolonged sedation2 Slower onset of action than midazolam2,3 Propylene glycol toxicity with higher doses1 Less hypotension than with midazolam2 Retrograde and anterograde amnesia4 1. Lerch, Park. Br Med Bull. 1999;55, 90. 2. Shafer. Crit Care Med. 1998;26:952-953. 3. Wagner, O’Hara. Clin Pharmacokinet. 1997;33:430, 434. 4. Harvey. Am J Crit Care. 1996;5:11.
  • 26. Benzodiazepines: Reversal Agents Flumazenil Transiently antagonizes the benzodiazepine  component of ventilatory depression and sedation during use with opioids Reverses CNS and circulatory side effects of  benzodiazepines within 2 minutes Useful for diagnostic evaluation  Stoelting. Pharmacology and Physiology in Anesthetic Practice. 3rd ed. 1999:138.
  • 27. Benzodiazepines Advantages Limitations • Amnesia1 • Weaning prolonged2,3 • Anxiolysis1 • Polyethylene glycol toxicity3 • Sedation1 • Respiratory depression2,4 • Hypotension2 • Lack of analgesia4 • Oversedation/deep sedation2 • Dependence/tolerance2 • Paradoxic agitation2 1. Pepperman. Care of the Critically Ill. 1989;5:197. 2. Harvey. Am J Crit Care. 1996;5:10, 11. 3. Lerch, Park. Br Med Bull. 1999;55:89, 90. 4. Crippen. Crit Care Clin. 1990;6:380.
  • 28. Propofol: Mechanisms of Action Not well-understood GABAA receptor modulation is most likely Davies. Can J Physiol Pharmacol. 1998;76:46.
  • 29. Propofol: Pharmacodynamics Sedation/anesthesia1 Decreases ICP1,2 Decreases SNS activity1,2 Cardiovascular depression1,3 Decreases ventilation time1 1. Wagner, O’Hara. Clin Pharmacokinet. 1997;33:434, 436. 2. Harvey. Am J Crit Care. 1996;5:12. 3. Lerch, Park. Br Med Bull. 1999;55:90,
  • 30. Propofol: Clinical Effects Anesthesia and sedation1 Rapid onset of action1,2 Very short half-life2 Decrease in BP and HR from sympathetic effects1 Decreases ventilation time3,4 Time to extubation faster than with midazolam3,4 1. Lerch, Park. Br Med Bull. 1999:55:90. 2. Harvey. Am J Crit Care. 1996;5:7-16. 3. Wagner, O’Hara. Clin Pharmacokinet. 1997;33:434. 4. Ostermann et al. JAMA. 2000;283:1457.
  • 31. Propofol Limitations Advantages • Respiratory depression (enhanced • Sedation1 by opioids)1 • Hypnosis1 • Hypotension1 • Anxiolysis1 • Decreased contractility2 • Muscle relaxation1 • Lack of analgesia3 •  ICP1 • Hypertriglyceridemia1 •  Cerebral metabolic • Preservative issues4 rate1 • Potential for infection necessitates need for regular changing of lines5 • Relief of bronchospasm1 1. Harvey. Am J Crit Care.1996;5:7-16. 2. Lerch, Park. Br Med Bull. 1999;55:90. 3. Wagner, O’Hara. Clin Pharmacokinet. 1997;33:435. 4. Propofol [package insert]. 5. Prielipp et al. Crit Care Clin. 1995;11:986.
  • 32. The Stress Response and Immunomodulation In Sedated ICU Patients
  • 33. Crit Care Med 2006 Vol.34 #2 453-460
  • 34.
  • 35. Sedation May affect Patient outcome through affect on cytokine release
  • 36. Propofol with EDTA There is a difference
  • 37. Herr et al, Intensive Care Medicine; 2000; 26 In a surgical ICU Serious Adverse Events 25 vs 8% Mortality 17.5 vs 2% 11 deaths in plain propofol vs 1 among the propofol with EDTA
  • 38.
  • 39. Propofol with EDTA Boost lipoidal antixidant defenses in tissue Chelator of heavy metals Iron is important for cytokine secretion Decrease Trace elements Decreased Free Radicals
  • 40. What we wish to investigate Do different drugs affect levels of cytokines released by the lung Can they protect the compartment of the lung from systemic cytokine release Do they prevent the release of cytokines from the lung
  • 41. How does Propofol with EDTA Affect Cytokine Levels Erasmus MC Rotterdam Papadakos, Lachmann Haitsma ATS 2006
  • 42. Propofol with EDTA affect on electrolytes:
  • 45. Peripheral Receptors 2 A 2A B 2B 2A
  • 46. Central Sites of Action: 2 Agonists Sedation Anxiolysis Sympathetic inhibition Analgesia
  • 47. Agonists 2 Dexmedetomidine Clonidine Selectivity: 2: 1 Selectivity: 2: 1 1620:13 200:11 t1/2 10 hrs1 t1/2 2 hrs3 PO, patch, epidural2 Intravenous3 Antihypertensive1 Sedative-analgesic3 Analgesic adjunct1 Primary sedative IV formulation not Only IV 2 available for available in US use in the US
  • 48. Clinical Effects of 2 Agonists Sedation/hypnosis1 Anxiolysis1 Analgesia1 Decreased sympathetic activity1 Decreased BP and HR2 Vasoconstriction at high doses1 Kamibayashi, Maze. Anesthesiology. 2000;93:1345-1349. 2. Wagner, O’Hara. Clin Pharmacokinet. 1997;33:426-453.
  • 49. Dexmedetomidine: Indications  Sedation of initially intubated and MV patients during treatment in the ICU Contraindications  Caution in patients with advanced heart block Drug interactions  Vagal effects can be counteracted by IV administration of anticholinergic agents Disease effecting clearance  Clearance is lower in patients with hepatic impairment
  • 50. Dexmedetomidine Advantages Limitations • Has sedative, analgesic, • May reduce HR and BP (caution in and anxiolytic effects1 hypovolemia, shock, and heart block)4 • Respiratory stability2 • Potentiates effects of opioids, • Predictable hemodynamic sedatives and anesthetics4 response1 • Dry mouth4 • Arousable and oriented patient3 • Vasoconstriction at high dose4 • No need to discontinue before extubation4 • Antishivering5 1. Aantaa et al. Drugs of the Future. 1993;18:49-56. 2. Frangoulidou et al. In: Redefining Sedation. 1998:40-50. 3. Mantz, Singer. In: Redefining Sedation. 1998:23-29. 4. Precedex™ [package insert]. 5. Kamibayashi, Maze. Anesthesiology. 2000;93:1345-1349.
  • 52. COX – 2 Inhibitors Prostaglandin Modulation
  • 53. Recent Data: May have important role in treatment of Septic Patients Normalization of Endotoxin Attenuation of macrophage depression of hematopoietic proliforation Augmentation of white cell count Shoup M et al J Trauma Inj Inf Crit Care 1998;45:215-219
  • 54. Several Studies in Burn Injury Highly affective in murine burn injury 80% increase in COX-2 protein compared to control at 4 hours post injury
  • 55. COX-2 Drugs have however been recalled for increased Cardiac Risk
  • 56. Neurontin Increases GABA Levels
  • 57. Neurontin Decreases requirement of narcotics Decreases Alcohol Withdrawal
  • 58. We now use this Drug commonly in Withdrawal Syndromes
  • 59. The Fine Balance in Patient Comfort
  • 60. The Fine Balance in Patient Comfort Anxiety Agitation Hypertension Tachycardia Arrhythmias Myocardial ischemia Wound disruption Patient injury
  • 61. The Fine Balance in Patient Comfort Depersonalization Delayed emergence Delayed weaning Pressure injury Venous stasis Muscle atrophy Increased cost
  • 62. Sedation Modulates immune system Provides comfort Modulates Length of Stay Affects health care costs