Ketamine

8 min read Last updated April 8, 2026

How to use ketamine in practice

  • Induction (IV): 1–2 mg/kg produces anaesthesia in ~30–60 s; duration ~10–20 min
    • Consider lower doses (0.5–1 mg/kg) in shocked/hypovolaemic patients; titrate to effect
    • Co-administer benzodiazepine (e.g. midazolam) to reduce emergence phenomena; consider anticholinergic if troublesome hypersalivation
  • Analgesic/sub-anaesthetic dosing: 0.1–0.3 mg/kg IV bolus; infusion commonly 0.05–0.3 mg/kg/h (institution-dependent)
    • Useful as opioid-sparing adjunct in acute pain, perioperative analgesia, opioid tolerance, and some chronic pain states
    • Monitor for psychotomimetic effects; consider co-analgesics and sedation strategy
  • Procedural sedation/ED: 0.5–1 mg/kg IV (or 4–5 mg/kg IM) with appropriate monitoring and airway readiness
    • Maintain vigilance for laryngospasm (rare), apnoea after rapid IV bolus, and vomiting during recovery
  • RSI/haemodynamic instability: useful where maintenance of blood pressure is desirable; ensure adequate depth and consider co-induction agent/opioid depending on physiology
    • Sympathomimetic response depends on intact catecholamine stores; in severe sepsis/prolonged shock, direct myocardial depression may predominate
  • Asthma/bronchospasm: bronchodilator properties can be helpful; treat secretions and ensure adequate ventilation strategy
    • Increased secretions may worsen airway reactivity in some; consider anticholinergic and suction readiness

When to avoid or use with caution

  • Raised intracranial pressure/space-occupying lesion: avoid or use only with controlled ventilation and specialist context (evidence mixed; CO2 control is key)
    • Ketamine can increase cerebral blood flow/CMRO2 in some settings; hypercapnia and inadequate anaesthesia increase ICP risk
  • Severe ischaemic heart disease, uncontrolled hypertension, aortic dissection: sympathomimetic effects may be harmful
    • Consider alternatives or blunt response with opioid/benzodiazepine/alpha-2 agonist as appropriate
  • Psychiatric illness (e.g. schizophrenia/active psychosis): increased risk of dysphoria/hallucinations
    • Emergence reactions reduced by calm environment and benzodiazepine co-administration
  • Raised intraocular pressure/open globe injury: traditionally avoided (IOP may rise transiently)
    • If used, avoid hypoventilation and coughing/straining; ensure adequate depth

Class, formulation, and chemistry

  • Phencyclidine (PCP) derivative; arylcyclohexylamine producing dissociative anaesthesia (functional and electrophysiological dissociation between thalamocortical and limbic systems)
  • Racemic mixture (R/S); S-ketamine is more potent (analgesia/anaesthesia) with potentially fewer psychotomimetic effects (availability varies)
  • Presentation commonly 10 mg/mL or 50 mg/mL; acidic solution; preservative-containing vials exist (check local product)

Mechanism of action

  • Primary: non-competitive NMDA receptor antagonism (PCP site) → reduced excitatory glutamatergic transmission; key for analgesia and dissociation
  • Additional actions: interaction with opioid receptors (μ, κ), monoaminergic pathways (inhibits reuptake of noradrenaline/serotonin), voltage-gated Ca2+ channels, HCN channels; local anaesthetic (Na+ channel) effects at higher concentrations
  • Sympathomimetic effects largely indirect via central stimulation and inhibition of catecholamine reuptake; direct negative inotropy exists but is usually masked unless catecholamine-depleted

Pharmacokinetics

  • Highly lipid soluble; rapid CNS uptake; onset IV ~30–60 s; IM onset ~3–5 min
  • Distribution: large Vd; high protein binding (moderate); redistribution contributes to short clinical duration after bolus
  • Metabolism: hepatic (CYP-mediated) N-demethylation to norketamine (active) then hydroxylation/conjugation; enterohepatic considerations minimal clinically
  • Elimination: renal excretion of metabolites; context-sensitive half-time increases with prolonged infusion; terminal half-life often quoted ~2–3 h (product-dependent)
  • Oral bioavailability low due to first-pass metabolism; intranasal/oral/transmucosal routes used in pain/psychiatry with different kinetics

Pharmacodynamics: CNS

  • Produces dissociative anaesthesia: profound analgesia, amnesia, catalepsy; eyes may remain open with nystagmus; increased muscle tone; reflexes may be preserved
  • EEG: increased high-frequency activity; BIS may be unreliable (can be higher than expected for depth)
  • Emergence phenomena: vivid dreams, hallucinations, dysphoria; more common in adults, higher doses, rapid emergence, and anxious patients
    • Reduction strategies: benzodiazepine, alpha-2 agonist, adequate analgesia, quiet environment, slow titration
  • Cerebral physiology: tends to increase CBF and CMRO2; may increase ICP especially with hypoventilation/hypercapnia; preserves airway reflexes but not reliably protective

Pharmacodynamics: respiratory

  • Minimal respiratory depression compared with other induction agents; apnoea can occur with rapid IV bolus or with co-administered sedatives/opioids
  • Airway: increased salivation/secretions; rare laryngospasm (notably in children/procedural sedation); bronchodilation via sympathetic and direct smooth muscle effects

Pharmacodynamics: cardiovascular

  • Typically increases HR, BP, CO, and SVR (sympathomimetic); useful in haemodynamic compromise
  • Direct myocardial depression (negative inotropy) may be unmasked in catecholamine-depleted states (septic shock, prolonged critical illness) → hypotension possible
  • Increases myocardial oxygen demand; caution in severe CAD, tachyarrhythmias, pulmonary hypertension (may increase PVR variably)

Other system effects

  • GI: nausea/vomiting can occur (often during recovery); consider antiemetic strategy for procedural sedation
  • Eye: may increase IOP; nystagmus common; lacrimation increased
  • Urology (chronic misuse): ulcerative cystitis and lower urinary tract symptoms; relevant in long-term recreational use history

Indications

  • Induction/maintenance of anaesthesia where haemodynamic stability is required (trauma, hypovolaemia) and as part of TIVA/infusion techniques
  • Analgesia: perioperative opioid-sparing, acute severe pain, opioid tolerance, burn dressings, trauma analgesia; adjunct in regional anaesthesia pathways
  • Procedural sedation (ED, radiology, burns, paediatrics) with appropriate monitoring and airway capability
  • Status asthmaticus/bronchospasm (adjunct) and refractory agitation requiring rapid control (specialist protocols)

Contraindications and cautions (exam framing)

  • Relative: uncontrolled hypertension, severe IHD, aortic dissection, tachyarrhythmias, severe pulmonary hypertension
  • Relative: raised ICP/space-occupying lesion, open globe injury, severe psychiatric illness/psychosis
  • Caution with co-administered CNS depressants (opioids/benzodiazepines/propofol) → apnoea; caution in hepatic impairment (metabolism) and prolonged infusions

Adverse effects

  • Psychotomimetic: emergence delirium, hallucinations, dysphoria; less with benzodiazepines/alpha-2 agonists and calm environment
  • CV: hypertension, tachycardia, increased myocardial oxygen demand; hypotension in catecholamine-depleted states
  • Respiratory/airway: hypersalivation, laryngospasm (rare), vomiting/aspiration risk if not fasted; apnoea with rapid bolus
  • Neurological: increased muscle tone, involuntary movements; not a reliable marker of inadequate anaesthesia

Practical tips and comparisons

  • Compared with propofol/thiopentone: better cardiovascular stability and analgesia, but more psychotomimetic effects and secretions; recovery can be less smooth
  • Co-induction: small-dose ketamine with propofol can reduce propofol requirement and hypotension; balance against PONV/emergence and secretions
  • Monitoring: depth monitors may mislead; rely on clinical signs, haemodynamics, and multimodal assessment
Describe ketamine: class, mechanism of action, and the concept of dissociative anaesthesia.

A common pharmacology viva: define the drug, then give primary and secondary mechanisms and link to clinical effects.

  • Class: phencyclidine derivative; IV anaesthetic producing dissociative anaesthesia
  • Primary mechanism: non-competitive NMDA receptor antagonism → analgesia, amnesia, dissociation
  • Secondary actions: opioid receptor interactions, monoamine reuptake inhibition (NA/5-HT), ion channel effects
  • Dissociative anaesthesia: functional separation of thalamocortical from limbic systems → catalepsy, analgesia, amnesia; eyes may be open; reflexes variably preserved
Outline the pharmacokinetics of ketamine and explain why its clinical duration is short after a bolus.

Examiners want: onset, redistribution, metabolism to active metabolite, and half-life concepts.

  • Rapid onset due to high lipid solubility and high cerebral blood flow
  • Short clinical duration after bolus mainly due to redistribution from brain to peripheral tissues (large Vd)
  • Hepatic metabolism (CYP) to norketamine (active) then further metabolism and conjugation
  • With infusion, context-sensitive half-time increases; recovery may be prolonged compared with single bolus
Discuss the cardiovascular effects of ketamine and explain why it can cause hypotension in some critically ill patients.

This is a frequent FRCA theme: indirect sympathomimetic vs direct myocardial depression.

  • Typical response: ↑HR, ↑BP, ↑CO, ↑SVR due to central sympathetic stimulation and inhibition of catecholamine reuptake
  • Direct effect: negative inotropy exists but is usually masked by sympathetic stimulation
  • Catecholamine-depleted states (sepsis, prolonged shock, severe illness): indirect sympathetic effect reduced → direct depression may predominate → hypotension
  • Clinical implication: titrate dose, consider vasopressors/inotropes and alternative induction agents depending on physiology
Describe the respiratory effects of ketamine and the airway complications relevant to procedural sedation.

Key points: relative preservation of ventilation, secretions, laryngospasm, and effect of co-drugs.

  • Minimal respiratory depression compared with propofol/opioids; apnoea can still occur with rapid IV bolus or co-sedatives
  • Increases salivation/secretions → suction readiness; consider anticholinergic if problematic
  • Laryngospasm: rare but important in sedation (especially children); manage with airway manoeuvres, CPAP, deepening anaesthesia, and paralysis if needed
  • Bronchodilation: useful in bronchospasm/status asthmaticus as an adjunct
What are emergence phenomena with ketamine? How do you prevent and treat them?

Often asked as: ‘unwanted effects and how to mitigate’.

  • Features: vivid dreams, hallucinations, dysphoria, agitation; more common in adults and with higher doses/rapid emergence
  • Prevention: benzodiazepine (e.g. midazolam), alpha-2 agonist, adequate analgesia, quiet environment, slow titration
  • Treatment: reassurance, reduce stimulation, small doses of benzodiazepine/propofol as clinically appropriate; exclude hypoxia/hypercarbia/pain
Discuss ketamine and intracranial pressure: what is the concern and how would you use it (if at all) in head injury?

A recurring exam topic: avoid simplistic ‘contraindicated’ answers—state physiology and conditions.

  • Concern: ketamine may increase CBF and CMRO2 and can increase ICP, particularly if ventilation is inadequate (hypercapnia) or anaesthesia is light
  • Modern view: with controlled ventilation, adequate anaesthesia, and avoidance of hypercapnia/hypoxia, ketamine may be acceptable in selected patients; local policy/specialist practice varies
  • In head injury with hypotension: potential benefit in maintaining MAP/CPP must be balanced against ICP considerations; ensure airway control and CO2 management
Give the indications for ketamine as an analgesic adjunct and outline a typical perioperative regimen.

Examiners want practical dosing ranges and rationale (opioid-sparing, tolerance).

  • Indications: major painful surgery, opioid tolerance, chronic pain patients, burns/trauma, prevention/treatment of opioid-induced hyperalgesia (context-dependent)
  • Regimen example: 0.1–0.3 mg/kg IV bolus then infusion 0.05–0.3 mg/kg/h (or institution protocol); reduce dose in elderly/psychiatric risk
  • Monitoring: sedation score, haemodynamics, psychotomimetic effects; plan for stop time to allow recovery
Compare ketamine with propofol as an induction agent in a shocked trauma patient.

A classic applied pharmacology comparison.

  • Ketamine: tends to maintain/increase BP and HR; provides analgesia; preserves ventilation better; risks include tachycardia, hypertension, secretions, emergence
  • Propofol: profound vasodilation and myocardial depression → hypotension; no analgesia; antiemetic; rapid clear-headed recovery
  • In severe shock/sepsis: ketamine may still cause hypotension if catecholamine-depleted; dose reduction and vasopressor readiness are essential
What are the contraindications/cautions for ketamine and why?

Give relative contraindications and link each to a mechanism.

  • Severe IHD/uncontrolled hypertension/aortic dissection: sympathomimetic response increases BP/HR and myocardial oxygen demand
  • Psychosis: risk of hallucinations and dysphoria
  • Raised ICP/space-occupying lesion: potential ↑CBF/ICP, especially if hypoventilated
  • Open globe injury/raised IOP: potential transient IOP rise and risk with coughing/straining
Explain why BIS/processed EEG monitoring can be misleading with ketamine.

This is a common ‘monitoring and depth’ viva question.

  • Ketamine increases high-frequency EEG activity and can increase BIS values despite adequate hypnosis/dissociation
  • Therefore BIS may overestimate wakefulness; interpret alongside clinical signs and other monitoring

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