Morphine

9 min read Last updated April 8, 2026

How to prescribe/use (adult perioperative)

  • IV titration for acute pain: give small boluses and reassess frequently
    • Typical: 1–2 mg IV every 2–3 min (or 0.02–0.05 mg/kg in increments) until comfortable; then observe for sedation/respiratory depression
    • Aim for analgesia with minimal sedation; document sedation score and RR
  • PCA morphine (common adult settings; local policy varies)
    • Demand dose often 1 mg; lockout 5 min; no background infusion in opioid-naïve adults
    • Use antiemetic strategy and regular non-opioid analgesics to reduce opioid requirement
  • Neuraxial (intrathecal/epidural) morphine: long-acting hydrophilic opioid—requires extended monitoring
    • Intrathecal: typical 100–200 micrograms (obstetric often 100 micrograms); epidural: 2–5 mg (institution-dependent)
    • Risk of delayed respiratory depression (often 6–12 h; can be up to 24 h); ensure protocolised obs and naloxone availability
  • Renal impairment: avoid or reduce dose and extend interval; consider alternatives (e.g., fentanyl) due to active metabolites
    • Morphine-6-glucuronide accumulates → prolonged opioid effect/respiratory depression; morphine-3-glucuronide → neuroexcitation
  • Hepatic impairment: reduced clearance and increased bioavailability; start low, go slow
    • Reduced first-pass metabolism increases effect of oral dosing; monitor sedation closely

Monitoring and safety

  • Minimum monitoring after parenteral/neuraxial morphine: RR, sedation score, SpO2 (and ideally capnography in high-risk), pain score, nausea/itching
    • High-risk: OSA, elderly/frail, renal failure, obesity, concomitant sedatives, neuraxial morphine
  • Treat opioid-induced respiratory depression: stimulate, airway support, oxygen/ventilation; titrated naloxone if needed
    • Give small IV boluses (e.g., 40–100 micrograms) to restore ventilation while preserving analgesia; consider infusion if recurrent due to longer opioid duration

Class and receptor pharmacology

  • Phenanthrene opioid; prototype strong opioid analgesic
  • Receptor actions: primarily μ (μ1 analgesia, μ2 respiratory depression/constipation), also κ and δ to lesser extent
  • Mechanism: Gi/o-coupled receptors → ↓ adenylyl cyclase, ↓ presynaptic Ca2+ influx, ↑ postsynaptic K+ efflux → reduced neurotransmitter release (e.g., substance P) and neuronal hyperpolarisation
  • Physiological effects: analgesia (spinal/supraspinal), sedation, euphoria/dysphoria, respiratory depression, cough suppression, miosis, reduced GI motility, biliary spasm, histamine release

Pharmacokinetics (PK)

  • Physicochemical: relatively hydrophilic compared with fentanyl; slower CNS equilibration; more rostral spread in CSF when neuraxial
  • Absorption: oral bioavailability low–moderate due to significant first-pass metabolism (variable between individuals)
  • Distribution: moderate protein binding; crosses placenta; Vd moderate–large
  • Metabolism: hepatic glucuronidation (UGT2B7) to active M6G and neuroexcitatory M3G; minor N-demethylation
  • Elimination: renal excretion of metabolites; accumulation in renal failure; half-life ~2–3 h (longer in elderly/renal impairment)
  • Context: duration of analgesia typically 3–4 h after IV/IM; neuraxial duration much longer (up to 24 h)

Pharmacodynamics (PD) and dose–response

  • Analgesic potency: reference opioid; fentanyl ~100× more potent (approx), oxycodone ~1.5× oral potency vs oral morphine (approx; varies)
  • Ceiling effect: none for analgesia/respiratory depression (full agonist at μ)
  • Respiratory depression: reduced brainstem CO2 responsiveness; worsened by sleep, sedatives, OSA, neuraxial morphine, renal failure
  • Cardiovascular: usually stable; histamine release can cause vasodilation, hypotension, flushing; bradycardia via vagal tone
  • GI/GU: nausea/vomiting (CTZ/vestibular), constipation (reduced peristalsis), urinary retention (esp neuraxial), biliary colic (sphincter of Oddi spasm)
  • CNS: sedation, pruritus (esp neuraxial; central mechanism), miosis; at high doses or with M3G accumulation → myoclonus, agitation, delirium

Indications (anaesthesia/ICU/pain)

  • Moderate–severe acute pain: perioperative, trauma, burns; adjunct in balanced anaesthesia (less common now than fentanyl/remifentanil for intra-op)
  • Neuraxial opioid for postoperative analgesia (e.g., major abdominal, caesarean section) where long duration desirable
  • Palliative care: chronic cancer pain (oral modified release and immediate release for breakthrough)
  • Acute pulmonary oedema (historical/selected use): anxiolysis/venodilation; use cautiously due to respiratory depression and evidence base

Contraindications and cautions

  • Absolute/strong: hypersensitivity; acute severe respiratory depression without ventilatory support
  • Caution: OSA, obesity, elderly, head injury/raised ICP (CO2 retention → cerebral vasodilation), severe asthma/COPD, hypotension, hypovolaemia
  • Renal failure: avoid or major dose reduction; monitor for prolonged sedation, myoclonus, delirium
  • Biliary disease/pancreatitis: may worsen pain due to sphincter of Oddi spasm (class effect; clinical relevance variable)
  • Concomitant CNS depressants (benzodiazepines, gabapentinoids, alcohol) increase risk of sedation and respiratory depression

Adverse effects and management

  • Respiratory depression: reduce/stop opioid, support airway/ventilation; titrated naloxone; consider infusion due to shorter naloxone half-life
  • Nausea/vomiting: antiemetics (ondansetron, cyclizine, droperidol per policy), hydration, reduce opioid dose with multimodal analgesia
  • Pruritus (esp neuraxial): low-dose naloxone infusion, nalbuphine, antihistamines often less effective if central mechanism
  • Constipation: stimulant + softener (e.g., senna + docusate) and/or macrogols; consider peripherally acting μ-antagonists in refractory cases
  • Urinary retention: monitor bladder; catheterise if needed; more common with neuraxial opioids
  • Histamine-mediated hypotension/bronchospasm: slow administration, fluids/vasopressors; consider alternative opioid if problematic

Drug interactions

  • Additive CNS/respiratory depression with benzodiazepines, propofol, volatile agents, gabapentinoids, sedating antihistamines, alcohol
  • MAOIs/serotonergic drugs: morphine has minimal serotonergic activity compared with some opioids (e.g., tramadol, meperidine), but caution with polypharmacy and altered mental state
  • Mixed agonist–antagonists (e.g., nalbuphine, buprenorphine) can reduce morphine effect or precipitate withdrawal in dependent patients

Special situations

  • Pregnancy/labour: crosses placenta; neonatal respiratory depression possible; neuraxial morphine commonly used post-caesarean with monitoring
  • Breastfeeding: generally compatible in usual doses but monitor infant for sedation/poor feeding; avoid high doses and prolonged use
  • Opioid tolerance/dependence: higher doses required; avoid abrupt cessation; consider multimodal and regional techniques; plan for withdrawal risk
  • Acute pain in chronic opioid users: continue baseline opioid, add short-acting opioid for acute pain, and use non-opioid adjuncts; consider ketamine, clonidine/dexmedetomidine, regional
Describe the pharmacology of morphine.

Structure your answer: class/receptors → mechanism → PK → PD effects → metabolism/metabolites → key cautions.

  • Class: strong opioid; phenanthrene; predominantly μ-receptor agonist
  • Mechanism: Gi/o-coupled μ receptor → ↓cAMP, ↓presynaptic Ca2+ entry, ↑postsynaptic K+ efflux → reduced nociceptive transmission
  • PK: relatively hydrophilic; slower CNS onset than fentanyl; oral bioavailability reduced by first-pass; hepatic glucuronidation; renal excretion of metabolites
  • Metabolites: M6G active (analgesia/resp depression); M3G neuroexcitatory (myoclonus, agitation); both accumulate in renal failure
  • PD: analgesia, sedation, respiratory depression, miosis, nausea/vomiting, constipation, pruritus, urinary retention; histamine release → hypotension
Why is morphine problematic in renal failure? What would you use instead?

Examiners want metabolites + clinical consequences + safer alternatives.

  • Morphine is glucuronidated to M6G (active) and M3G (neuroexcitatory); both are renally excreted and accumulate when GFR is low
  • Consequences: prolonged sedation and respiratory depression (M6G), confusion/delirium and myoclonus (M3G)
  • Management: avoid or reduce dose markedly and extend interval; close monitoring; treat toxicity with ventilatory support and titrated naloxone
  • Alternatives in severe renal impairment: fentanyl/alfentanil (no active renally cleared metabolites), remifentanil (esterases), consider oxycodone with caution; seek pain/renal guidance
Compare morphine with fentanyl (PK/PD and clinical implications).

A common FRCA comparison: lipid solubility, onset/duration, histamine, neuraxial spread, metabolism.

  • Lipid solubility: morphine less lipophilic → slower onset; fentanyl highly lipophilic → rapid onset
  • Duration: morphine longer clinical duration after bolus; fentanyl shorter after small bolus but can accumulate with infusion (context-sensitive half-time increases)
  • Histamine: morphine can cause histamine-mediated vasodilation/hypotension; fentanyl minimal histamine release
  • Neuraxial: morphine hydrophilic → wider CSF spread and delayed respiratory depression; fentanyl lipophilic → faster onset, more segmental, less delayed depression
  • Metabolism: morphine → M6G/M3G (renal issues); fentanyl hepatic metabolism to inactive metabolites
Explain opioid-induced respiratory depression and how you would manage it after morphine.

Focus on physiology, risk factors, and practical naloxone titration.

  • Mechanism: μ-receptor activation in brainstem reduces ventilatory response to CO2 and hypoxia; sedation worsens airway obstruction (especially OSA)
  • Recognise: rising sedation score precedes apnoea; low RR, shallow breathing, hypercapnia; miosis may be present
  • Immediate management: call for help; stimulate; airway manoeuvres; oxygen; support ventilation (bag-mask/NIV/intubation as required)
  • Naloxone: titrate IV boluses (e.g., 40–100 micrograms) to adequate ventilation; avoid large bolus that abolishes analgesia and precipitates acute withdrawal
  • Re-sedation: naloxone duration may be shorter than morphine/M6G; consider infusion and ongoing monitoring
What are the advantages and disadvantages of intrathecal morphine?

Key points: long duration, excellent analgesia, but delayed respiratory depression and pruritus.

  • Advantages: profound postoperative analgesia (often 12–24 h), opioid-sparing, improved mobilisation and respiratory mechanics when pain is well controlled
  • Disadvantages: pruritus, nausea/vomiting, urinary retention, and delayed respiratory depression due to rostral CSF spread
  • Risk factors for respiratory depression: higher dose, elderly, OSA, obesity, concomitant sedatives, magnesium, and systemic opioids
  • Monitoring: protocolised observations for at least 12–24 h (depending on local policy), with sedation score and RR; naloxone available
A patient has severe pain despite repeated morphine boluses. How do you approach this?

Demonstrate safe titration, reassessment, and differential diagnosis of uncontrolled pain.

  • Reassess: confirm pain source and exclude surgical complication (bleeding, compartment syndrome, ischaemia), neuropathic pain, bladder retention, tight cast/dressing
  • Assess opioid effect: sedation score, RR, SpO2/EtCO2; avoid chasing pain into respiratory depression
  • Optimise multimodal: paracetamol, NSAID (if appropriate), regional/neuraxial techniques, ketamine (opioid-tolerant), clonidine/dexmedetomidine where suitable
  • Consider opioid issues: tolerance, opioid-induced hyperalgesia (less typical with morphine than remifentanil but possible), wrong diagnosis, inadequate dosing interval
  • If escalating doses: senior review; consider alternative opioid (e.g., fentanyl) and monitored setting
Explain the causes of pruritus after neuraxial morphine and how you treat it.

Central mechanism and opioid antagonist/agonist-antagonist treatments are key.

  • Mechanism: mainly central (μ-receptor-mediated) rather than histamine; therefore antihistamines may sedate but often do not treat itch effectively
  • Treatment options: low-dose naloxone infusion (reduces itch with minimal analgesia loss), nalbuphine (κ-agonist/μ-antagonist), ondansetron sometimes used
  • Supportive: reassure, cool packs; avoid excessive sedating antihistamines in patients at risk of respiratory depression
List the main side effects of morphine and give a brief mechanism for each.

A classic viva list: respiratory, CVS, GI, CNS, GU, skin.

  • Respiratory depression: reduced brainstem CO2 sensitivity (μ2)
  • Nausea/vomiting: CTZ stimulation + vestibular sensitisation; delayed gastric emptying
  • Constipation: reduced peristalsis and increased sphincter tone (μ in gut)
  • Hypotension/flushing: histamine release and vasodilation; bradycardia via vagal tone
  • Pruritus: central μ effect (especially neuraxial)
  • Urinary retention: increased sphincter tone and reduced detrusor contractility (worse with neuraxial)
  • Miosis: parasympathetic stimulation of Edinger–Westphal nucleus
How would you convert oral morphine to IV morphine in the perioperative period?

State that ratios vary; show safe principles: reduce dose, titrate, and monitor.

  • Recognise variability: oral morphine bioavailability is variable; conversion ratios are approximate and depend on formulation and patient factors
  • Rule-of-thumb often used: IV morphine is roughly 2–3 times as potent as oral (i.e., oral:IV ≈ 2–3:1), but start conservatively and titrate to effect
  • Account for: age, renal/hepatic function, pain severity, opioid tolerance, and concurrent sedatives
  • Practical approach: continue baseline opioid where possible; if NBM convert to parenteral with dose reduction and close monitoring; consider PCA

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