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Propofol
Dr. S. Parthasarathy
MD., DA., DNB, MD (Acu), Dip. Diab. DCA,
Dip. Software statistics-
PhD ( physiology), IDRA
History
• 1970 – discovery
• 1977 found the hypnotic use
• 1986- only popular use
• Insoluble – cremophor – EL – anaphylactic
reactions
Chemistry
• 2,6 Di isopropylphenol propofol (10 mg/mL)
was reintroduced as an egg lecithin emulsion
formulation (Diprivan), consisting of
• 10% soybean oil,
• 2.25% glycerol,
• 1.2% egg phosphatide.
Ampofol
• More recently, a lower-lipid formulation of
propofol has been introduced into clinical
practice
• The increased “free” fraction of propofol leads
to increased pain when it is injected into small
veins. Therefore, it is important to add
lidocaine to the Ampofol formulation to
minimize the pain on injection.
Aquavan
• A new water-soluble prodrug of propofol
• This prodrug is rapidly hydrolyzed by plasma
alkaline phosphatases in the circulation to
release free propofol.
• It has a slower onset but a similar recovery
profile.
• does not produce injection site discomfort, a
transient burning sensation has been reported
in the perineal region following IV injection.
Chemistry
• Egg lecithin – iatrogenic sepsis
• 0.005% ethylene diamine tetraacetic acid
(EDTA), 0.025% metabisulfite, or 0.1% benzyl
alcohol.- bacteriocide preservative
• Propofol undergoes dimerization and
oxidation to a quinone when exposed to
oxygen. – yellow color
• Open to atmosphere – maximum six hours
Chemistry
• 1 % solution
• Milky white viscous preparation
• Rarely 2 % solution
• 0.5 % solution for pediatric use
• Sodium salt, to be diluted in water or saline to
create 1% solution, pH >10
• pKa - 11
• 50 ml dispo syringes preloaded available
Propofol
• Highly lipid soluble
• 98% protein bound
• Redistribution 3-5 minutes
• T half is 4-6 hours
• Clearance is approx ten times higher
MECHANISM
• relatively selective modulator of γ-aminobutyric
acid (GABAA) receptors
• transmembrane chloride conductance increases,
• hyperpolarization of the postsynaptic cell
membrane and functional inhibition of the
postsynaptic neuron.
• does not appear to modulate other ligand gated
ion channels at clinically relevant concentrations.
Kinetics
• IV bolus dose of propofol, the plasma level initially
declines rapidly due to redistribution from highly
perfused but lower capacity tissue such as brain, to high
capacity but lower perfusion sites such as muscle, liver,
spleen ---
• 5 minutes -- more clear headed recovery than
thiopentone ---
• Outpatients
Propofol (1%)
• Sedation (infusion) IV- 25 - 100 µg/Kg/min
• Induction IV--- 1 - 2 mg/Kg
• Maintenance IV- 50 - 200 µg/Kg/min
No
other
route
CP50
• 3 µ/ ml -- with sedatives and opioids – skin
incision
• 16 µ/ ml –without sedatives and opioids –
skin incision
• Sedation = 1.6 µ/ ml
• Propofol is rapidly metabolized in the liver by
conjugation, to produce inactive water-soluble
glucuronide and sulfate compounds, which
are excreted by the kidneys.
Thio – action is same – but some
differences √
• Sedation , hynosis , anesthesia anticonvulsant, ?
Decreased ICP decreased CMRO2 but ---
• MAP reduction and CPP
• Less antanalgesia
• Less Nausea and vomiting ? D2 receptors
• Less spasm - Supraglottic device √
• Myoclonic jerks + subcortical inhibitory glycine
antagonism by propofol
• Amnesia is better
When to stop ?
• Loss of eye lash reflex - ?
• Apnea may come
• Loss of verbal contact is better
Propofol – RS
• dose-dependent decrease in ventilatory drive,
• decreased tidal volume and minute ventilation
and an increased Paco2
• Apnea more common
• Depressed protective reflexes
CVS
• Vasodilation – both decreased preload and
after load
• No tachycardia
• More fall
• But in healthy patients its transient and
insignificant
Other Effects
• decreases renal blood flow and causes increased
secretion of antidiuretic hormone.
• Sub hypnotic doses appear to be effective in
reversing the itching produced by cholestasis or by
epidural morphine.
• safe to give to patients with all types of porphyria
and for those with malignant hyperthermia.
Other Effects
• Like thiopentone, propofol does not
potentiate the neuromuscular blockade,
• It does not affect the corticosteroid synthesis
• Multiple drug allergies – cautious
• Propofol does not adversely affect hepatic or
renal function,
• No effect on coagulation
Infusions
• The context-sensitive half-time (CSHT) describes the
time required for the central compartment blood
concentration to fall by half as a function of the
duration of an infusion
• 11 minutes + 4 +4 ----
• For every hour after 1 hour
TCI pumps
• The patient’s age, body weight, and desired
blood (effect site) concentration are entered,
and the pump delivers a propofol bolus
followed by a variable-rate infusion.
• The rate is automatically adjusted to match
predicted losses from distribution and
elimination in order to maintain a constant
propofol concentration.
Side effects
• propofol may be mixed with preservative-free
lidocaine, 0.5% or 1%, in a ratio up to 20:1 with
aseptic precautions and immediate administration,
and with alfentanil, 500 ug mL-I,in a ratio from 20:1
to 50:1 for use within 6 h of preparation.
• NSAIDs, opioids, ketamine
• microfiltration , cold drug, saline, needle big in
cubital vein
Pain on injection ? 60 %
Pain
• Free propofol may exert its painful effect by
stimulating the kallikrein-kinin system, resulting in
the generation of bradykinin, which stimulates
intravascular nociceptors.
• Administration of nafamostat, an inhibitor of
kallikrein, before propofol injection has significantly
decreased the incidence and severity of pain
Propofol in children ?
• The role in pediatric anesthesia is more
controversial.
• not approved by the manufacturer for
anesthesia in children less than 3 years old or
for sedation for intensive care or surgical and
diagnostic procedures.
• Propofol sedation was blamed for the deaths
of several children with respiratory tract
infections, who developed severe
acidosis,lipemia, and multiple organ failure.
• Is propofol safe for procedural sedation in children? A
prospective evaluation of propofol versus ketamine in
pediatric critical care.
• Vardi A1, Salem Y, Padeh S, Paret G, Barzilay Z.
• Propofol-based sedation regimen for infants and children
undergoing ambulatory magnetic resonance imaging
• A.-M. Machata*, H. Willschke, B. Kabon, S. C. Kettner
• British Journal of Anaesthesia 94 (5): 630–5 (2005)
PAEDIATRIC ANAESTHESIA Propofol 6% as sedative in children
under 2 years of age following major craniofacial surgery
But Ok – lot of studies
Lactic acidosis or propofol infusion
syndrome
• in pediatric and adult patients receiving
prolonged high-dose infusions of propofol
(>75 µg/kg per minute) for longer than 24
hours.
• Unexpected refractory bradycardia occurring
during propofol anesthesia should prompt a
laboratory evaluation for possible metabolic
(lactic) acidosis.
PRIS
• Associated high lactate
• High TGL
• Lipemic plasma
• rhabdomyolysis or myoglobinuria
• 3 days after usually
Etiopathology
• A measurement of arterial blood gases and serum lactate
concentrations is recommended.
• Metabolic acidosis in its early stages is reversible with
discontinuation of propofol administration
• The mechanism is unclear but may reflect a poisoning
(cytopathic hypoxia) of the electron transport chain and
impaired oxidation of long-chain fatty acids by propofol
or a propofol metabolite in uniquely susceptible patients
The differential diagnosis
• suspected includes hyperchloremic metabolic
acidosis associated with large volume
infusions of 0.9% saline
• metabolic acidosis associated with the
excessive generation of organic acids, such as
lactate and ketones (diabetic acidosis, release
of a tourniquet).
if PRIS , prevention and treatment
• Suspicion and monitoring of lactate and creatine
kinase levels
• Stop propofol
• High carbohydrate therapy
• Inotropes ?
• Usually ECMO
• 18 -20 % mortality
Contraindications
• contraindicated in patients with a known hypersensitivity
to propofol or any of Injectable Emulsion components.
• Injectable Emulsion is contraindicated in patients with
allergies to eggs, egg products, soybeans or soy products.
• No evidence for contraindications to the use of propofol in
adults ...
• by LL Asserhøj - - Br J Anaesth. 2016 Jan;116(1):77-82.
• No evidence for contraindications to the use of propofol in
adults allergic to egg, soy or peanut†.
Propofol in pregnancy
• Some reservations
• Crosses placenta and cause problems
• Grade C approval by the manufacturer
• Some studies have proven safety
• Yes , we can use when benefits outweigh risks
Who is this and how he died ?
Fospropofol
• Fospropofol is a water-soluble prodrug of
propofol. It is metabolized by alkaline
phosphatases in the liver to yield propofol,
phosphate, and formaldehyde
• Not a lipid preparation
• Fospropofol is approved for procedural sedation.
• The recommended dose is 6.5 mg/kg administered
as a bolus, followed by intermittent bolus doses of
1.5 mg/kg.
• 4-8 minutes is the onset
• Procedural sedation
• Scopies
• Fentanyl 1 mic / kg followed by fos propofol
• CNS resp CVS actions will be there
• Fospropofol is not recommended for use in
labor, caesarean section deliveries, nursing
mothers
• patients <18 years as its safety is not yet
established
• Less painful but cough and paresthesia may
come
Summary
• Chemistry
• Pharmacokinetics
• Effects
• Side effects
• Contraindications ?

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Propofol

  • 1. Propofol Dr. S. Parthasarathy MD., DA., DNB, MD (Acu), Dip. Diab. DCA, Dip. Software statistics- PhD ( physiology), IDRA
  • 2. History • 1970 – discovery • 1977 found the hypnotic use • 1986- only popular use • Insoluble – cremophor – EL – anaphylactic reactions
  • 3. Chemistry • 2,6 Di isopropylphenol propofol (10 mg/mL) was reintroduced as an egg lecithin emulsion formulation (Diprivan), consisting of • 10% soybean oil, • 2.25% glycerol, • 1.2% egg phosphatide.
  • 4. Ampofol • More recently, a lower-lipid formulation of propofol has been introduced into clinical practice • The increased “free” fraction of propofol leads to increased pain when it is injected into small veins. Therefore, it is important to add lidocaine to the Ampofol formulation to minimize the pain on injection.
  • 5. Aquavan • A new water-soluble prodrug of propofol • This prodrug is rapidly hydrolyzed by plasma alkaline phosphatases in the circulation to release free propofol. • It has a slower onset but a similar recovery profile. • does not produce injection site discomfort, a transient burning sensation has been reported in the perineal region following IV injection.
  • 6. Chemistry • Egg lecithin – iatrogenic sepsis • 0.005% ethylene diamine tetraacetic acid (EDTA), 0.025% metabisulfite, or 0.1% benzyl alcohol.- bacteriocide preservative • Propofol undergoes dimerization and oxidation to a quinone when exposed to oxygen. – yellow color • Open to atmosphere – maximum six hours
  • 7. Chemistry • 1 % solution • Milky white viscous preparation • Rarely 2 % solution • 0.5 % solution for pediatric use • Sodium salt, to be diluted in water or saline to create 1% solution, pH >10 • pKa - 11 • 50 ml dispo syringes preloaded available
  • 8. Propofol • Highly lipid soluble • 98% protein bound • Redistribution 3-5 minutes • T half is 4-6 hours • Clearance is approx ten times higher
  • 9. MECHANISM • relatively selective modulator of γ-aminobutyric acid (GABAA) receptors • transmembrane chloride conductance increases, • hyperpolarization of the postsynaptic cell membrane and functional inhibition of the postsynaptic neuron. • does not appear to modulate other ligand gated ion channels at clinically relevant concentrations.
  • 10. Kinetics • IV bolus dose of propofol, the plasma level initially declines rapidly due to redistribution from highly perfused but lower capacity tissue such as brain, to high capacity but lower perfusion sites such as muscle, liver, spleen --- • 5 minutes -- more clear headed recovery than thiopentone --- • Outpatients
  • 11. Propofol (1%) • Sedation (infusion) IV- 25 - 100 µg/Kg/min • Induction IV--- 1 - 2 mg/Kg • Maintenance IV- 50 - 200 µg/Kg/min No other route
  • 12. CP50 • 3 µ/ ml -- with sedatives and opioids – skin incision • 16 µ/ ml –without sedatives and opioids – skin incision • Sedation = 1.6 µ/ ml
  • 13. • Propofol is rapidly metabolized in the liver by conjugation, to produce inactive water-soluble glucuronide and sulfate compounds, which are excreted by the kidneys.
  • 14. Thio – action is same – but some differences √ • Sedation , hynosis , anesthesia anticonvulsant, ? Decreased ICP decreased CMRO2 but --- • MAP reduction and CPP • Less antanalgesia • Less Nausea and vomiting ? D2 receptors • Less spasm - Supraglottic device √ • Myoclonic jerks + subcortical inhibitory glycine antagonism by propofol • Amnesia is better
  • 15. When to stop ? • Loss of eye lash reflex - ? • Apnea may come • Loss of verbal contact is better
  • 16. Propofol – RS • dose-dependent decrease in ventilatory drive, • decreased tidal volume and minute ventilation and an increased Paco2 • Apnea more common • Depressed protective reflexes
  • 17. CVS • Vasodilation – both decreased preload and after load • No tachycardia • More fall • But in healthy patients its transient and insignificant
  • 18. Other Effects • decreases renal blood flow and causes increased secretion of antidiuretic hormone. • Sub hypnotic doses appear to be effective in reversing the itching produced by cholestasis or by epidural morphine. • safe to give to patients with all types of porphyria and for those with malignant hyperthermia.
  • 19. Other Effects • Like thiopentone, propofol does not potentiate the neuromuscular blockade, • It does not affect the corticosteroid synthesis • Multiple drug allergies – cautious • Propofol does not adversely affect hepatic or renal function, • No effect on coagulation
  • 20. Infusions • The context-sensitive half-time (CSHT) describes the time required for the central compartment blood concentration to fall by half as a function of the duration of an infusion • 11 minutes + 4 +4 ---- • For every hour after 1 hour
  • 21. TCI pumps • The patient’s age, body weight, and desired blood (effect site) concentration are entered, and the pump delivers a propofol bolus followed by a variable-rate infusion. • The rate is automatically adjusted to match predicted losses from distribution and elimination in order to maintain a constant propofol concentration.
  • 22. Side effects • propofol may be mixed with preservative-free lidocaine, 0.5% or 1%, in a ratio up to 20:1 with aseptic precautions and immediate administration, and with alfentanil, 500 ug mL-I,in a ratio from 20:1 to 50:1 for use within 6 h of preparation. • NSAIDs, opioids, ketamine • microfiltration , cold drug, saline, needle big in cubital vein Pain on injection ? 60 %
  • 23. Pain • Free propofol may exert its painful effect by stimulating the kallikrein-kinin system, resulting in the generation of bradykinin, which stimulates intravascular nociceptors. • Administration of nafamostat, an inhibitor of kallikrein, before propofol injection has significantly decreased the incidence and severity of pain
  • 24. Propofol in children ? • The role in pediatric anesthesia is more controversial. • not approved by the manufacturer for anesthesia in children less than 3 years old or for sedation for intensive care or surgical and diagnostic procedures. • Propofol sedation was blamed for the deaths of several children with respiratory tract infections, who developed severe acidosis,lipemia, and multiple organ failure.
  • 25. • Is propofol safe for procedural sedation in children? A prospective evaluation of propofol versus ketamine in pediatric critical care. • Vardi A1, Salem Y, Padeh S, Paret G, Barzilay Z. • Propofol-based sedation regimen for infants and children undergoing ambulatory magnetic resonance imaging • A.-M. Machata*, H. Willschke, B. Kabon, S. C. Kettner • British Journal of Anaesthesia 94 (5): 630–5 (2005) PAEDIATRIC ANAESTHESIA Propofol 6% as sedative in children under 2 years of age following major craniofacial surgery But Ok – lot of studies
  • 26. Lactic acidosis or propofol infusion syndrome • in pediatric and adult patients receiving prolonged high-dose infusions of propofol (>75 µg/kg per minute) for longer than 24 hours. • Unexpected refractory bradycardia occurring during propofol anesthesia should prompt a laboratory evaluation for possible metabolic (lactic) acidosis.
  • 27. PRIS • Associated high lactate • High TGL • Lipemic plasma • rhabdomyolysis or myoglobinuria • 3 days after usually
  • 28. Etiopathology • A measurement of arterial blood gases and serum lactate concentrations is recommended. • Metabolic acidosis in its early stages is reversible with discontinuation of propofol administration • The mechanism is unclear but may reflect a poisoning (cytopathic hypoxia) of the electron transport chain and impaired oxidation of long-chain fatty acids by propofol or a propofol metabolite in uniquely susceptible patients
  • 29. The differential diagnosis • suspected includes hyperchloremic metabolic acidosis associated with large volume infusions of 0.9% saline • metabolic acidosis associated with the excessive generation of organic acids, such as lactate and ketones (diabetic acidosis, release of a tourniquet).
  • 30. if PRIS , prevention and treatment • Suspicion and monitoring of lactate and creatine kinase levels • Stop propofol • High carbohydrate therapy • Inotropes ? • Usually ECMO • 18 -20 % mortality
  • 31. Contraindications • contraindicated in patients with a known hypersensitivity to propofol or any of Injectable Emulsion components. • Injectable Emulsion is contraindicated in patients with allergies to eggs, egg products, soybeans or soy products. • No evidence for contraindications to the use of propofol in adults ... • by LL Asserhøj - - Br J Anaesth. 2016 Jan;116(1):77-82. • No evidence for contraindications to the use of propofol in adults allergic to egg, soy or peanut†.
  • 32. Propofol in pregnancy • Some reservations • Crosses placenta and cause problems • Grade C approval by the manufacturer • Some studies have proven safety • Yes , we can use when benefits outweigh risks
  • 33. Who is this and how he died ?
  • 34. Fospropofol • Fospropofol is a water-soluble prodrug of propofol. It is metabolized by alkaline phosphatases in the liver to yield propofol, phosphate, and formaldehyde • Not a lipid preparation
  • 35.
  • 36. • Fospropofol is approved for procedural sedation. • The recommended dose is 6.5 mg/kg administered as a bolus, followed by intermittent bolus doses of 1.5 mg/kg. • 4-8 minutes is the onset
  • 37. • Procedural sedation • Scopies • Fentanyl 1 mic / kg followed by fos propofol • CNS resp CVS actions will be there
  • 38. • Fospropofol is not recommended for use in labor, caesarean section deliveries, nursing mothers • patients <18 years as its safety is not yet established • Less painful but cough and paresthesia may come
  • 39. Summary • Chemistry • Pharmacokinetics • Effects • Side effects • Contraindications ?