Fentanyl | Medication Reference

Bedside Snapshot

Drug Class: Synthetic opioid analgesic; potent μ-opioid receptor agonist
Core Uses: Potent synthetic μ-opioid agonist (about 50–100 times more potent than morphine by weight) used IV/IN for rapid-onset analgesia, adjunct to induction/intubation, and ICU/OR analgesia-sedation; transdermal and transmucosal forms are for chronic pain, not acute titration
Hemodynamic Profile: Relatively hemodynamically stable compared with many other opioids when given slowly, but can still cause hypotension (especially with hypovolemia or sedative co-admins) and almost always causes some respiratory depression dose-dependently
IV Adult Analgesic Bolus: 25–100 mcg IV every 5–10 minutes titrated to effect (roughly 0.35–1.5 mcg/kg for an average adult). For more controlled titration, 0.5–1 mcg/kg IV over 2–5 minutes is common, with smaller redoses
RSI/Induction Adjunct: 1–3 mcg/kg IV (ideal body weight) administered over 30–60 seconds before laryngoscopy to blunt sympathetic response and provide analgesia, particularly in patients with suspected elevated ICP, acute coronary syndromes, or aortic dissection
ICU/OR Continuous Infusion: Often 0.5–10 mcg/kg/hour IV (0.01–0.17 mcg/kg/min), titrated to pain/sedation scores; some protocols use even higher transient rates in the OR. Context-sensitive half-time increases with infusion duration, so accumulation occurs with prolonged use
Intranasal (IN) Fentanyl: Commonly 1–2 mcg/kg (max 100–200 mcg) for acute severe pain, using 50 mcg/mL IV solution via mucosal atomization device; doses are often divided between nares. Useful in prehospital and pediatric settings when IV access is delayed
Onset: IV onset within 1–2 minutes with peak effect at ~3–5 minutes; duration after a small bolus is usually 30–60 minutes. IN onset is typically within 5–10 minutes with peak around 10–20 minutes
Major Acute Risks: Respiratory depression and apnea, chest wall and glottic rigidity (especially with high, fast IV doses), bradycardia, hypotension, nausea/vomiting, and rarely laryngospasm. Naloxone reverses respiratory depression but may also precipitate acute withdrawal or severe pain
Critical Warning: Transdermal and transmucosal fentanyl products are reserved for opioid-tolerant chronic pain patients because of high potency, delayed offset, and overdose risk; they should NOT be initiated for acute pain in opioid-naïve patients in the ED/ICU

Brand & Generic Names

Generic Name: Fentanyl citrate (most parenteral formulations)
Brand Names: Sublimaze (IV), Duragesic (transdermal), Actiq/Fentora/Onsolis (transmucosal), multiple generics—availability is region- and institution-specific

Medication Class

Synthetic opioid analgesic; potent μ-opioid receptor agonist

Pharmacology

Mechanism of Action:

Fentanyl is a highly potent μ-opioid receptor agonist that binds to μ receptors in the CNS and peripheral tissues, inhibiting adenylate cyclase, decreasing cAMP, and modulating ion channels (increased K⁺ efflux and decreased Ca²⁺ influx)
This leads to hyperpolarization of neurons and reduced neurotransmitter release (e.g., substance P, glutamate) in pain pathways, resulting in profound analgesia and blunting of the affective response to pain
At the brainstem and pontine respiratory centers, fentanyl reduces responsiveness to CO₂ and hypoxia, producing dose-dependent respiratory depression and decreased respiratory rate/tidal volume
In the cardiovascular system, fentanyl has relatively minimal direct myocardial depressant effects compared with some sedatives, but vagotonic effects and histamine-independent vasodilation can contribute to bradycardia and hypotension, especially when combined with other agents or in hypovolemia
High-dose, rapid IV administration is associated with rigid chest-wall and glottic muscle tone ("wooden chest"), likely mediated by μ receptors in brainstem loci and spinal cord; this can severely impair ventilation and mask as refractory bronchospasm without muscle relaxant

Pharmacokinetics (IV and Intranasal):

Formulations: IV injection solution typically 50 mcg/mL (in 2 mL or 10 mL vials), higher-concentration vials or premixed infusions in some institutions; transdermal patches (12–100 mcg/hour) and various transmucosal products for chronic pain
Onset (IV): Analgesic effect begins within 1–2 minutes after IV bolus, with peak effect ~3–5 minutes. Duration of a small bolus is typically 30–60 minutes, depending on dose and patient factors
Onset (IN): Analgesic effect generally begins within 5–10 minutes, with peak effect around 10–20 minutes; bioavailability via IN route is approximately 70–90% depending on formulation and technique
Distribution: Highly lipophilic with rapid distribution to CNS and other highly perfused tissues; large volume of distribution (~3–8 L/kg). Rapid redistribution from brain to peripheral tissues explains the short duration of a single bolus
Protein Binding: ~80–85% bound to plasma proteins (mostly α1-acid glycoprotein)
Metabolism: Primarily hepatic metabolism via CYP3A4 to inactive metabolites (e.g., norfentanyl); minimal active metabolites compared with some other opioids
Elimination: Metabolites are primarily excreted in urine; terminal elimination half-life is typically 3–8 hours, but the context-sensitive half-time increases substantially with prolonged infusions (hours to >10 hours in long infusions)
Renal Impairment: Clearance of fentanyl itself is relatively preserved, but accumulation of metabolites and altered protein binding can occur; dose reductions and slower titration are recommended in severe renal dysfunction
Hepatic Impairment: Reduced metabolism can increase fentanyl exposure and prolong effect; use lower initial doses and slower titration with close monitoring

Indications

Acute moderate-to-severe pain in the ED, prehospital, or inpatient setting when IV/IN opioids are indicated (trauma, post-op, abdominal pain, ACS, etc.)
Adjunct to induction and rapid sequence intubation to provide analgesia and blunt sympathetic responses to laryngoscopy (tachycardia, hypertension, increased ICP)
Analgesia-sedation in mechanically ventilated ICU patients (often as a continuous infusion with or without other sedatives)
Perioperative analgesia in the OR as part of balanced anesthesia
Intranasal fentanyl for rapid analgesia when IV access is delayed or challenging, especially in pediatric or prehospital populations
Transdermal and transmucosal formulations for chronic cancer or chronic non-cancer pain in opioid-tolerant patients (specialist-directed)
Traumatic injuries (fractures, burns, soft tissue injury) requiring rapid IV/IN analgesia
Acute coronary syndromes and other severe chest pain syndromes (used with caution due to potential masking of ischemic pain and hemodynamic effects)
Postoperative pain control (IV bolus or infusion, transitioning to other regimens)
Severe abdominal pain (e.g., pancreatitis, bowel obstruction, renal colic) requiring titratable opioid analgesia

Dosing & Administration

Available Forms:

IV Injection: Typically 50 mcg/mL in 2 mL (100 mcg) or 10 mL (500 mcg) vials/ampoules. Some facilities stock premixed infusions (e.g., 1000–2500 mcg in 50–100 mL NS/D5W)
Intranasal Use (Off-Label in Many Regions): IV 50 mcg/mL solution delivered via mucosal atomization device; doses often split between nares
Transdermal Patches: 12, 25, 50, 75, 100 mcg/hour (intended for opioid-tolerant chronic pain patients; NOT for acute titration)
Transmucosal Products: Oral lozenges, buccal tablets/films, and nasal sprays for breakthrough cancer pain in opioid-tolerant individuals

Critical Dosing Warning: Always check vial strength and total microgram content carefully; fentanyl dosing errors (e.g., confusing mcg and mg) can be rapidly fatal. Transdermal and transmucosal fentanyl products are contraindicated for acute pain in opioid-naïve patients.

Standard Dosing – Fentanyl (IV and Intranasal – Always Follow Local Protocols and Opioid/Sedation Guidelines):

Indication / Population	Dose & Route	Frequency / Titration	Notes
Adult acute pain – IV bolus	25–100 mcg IV (≈0.35–1.5 mcg/kg)	Every 5–10 min as needed, titrated to pain and respiratory status	Use lower end (25–50 mcg) in elderly, frail, or opioid-naïve patients
Adult RSI / induction adjunct	1–3 mcg/kg IV over 30–60 seconds	Single dose given 1–3 min before laryngoscopy	Use lower doses in unstable patients; monitor for hypotension and chest rigidity
Adult ICU/OR continuous infusion (analgesia-sedation)	0.5–10 mcg/kg/hour IV (0.01–0.17 mcg/kg/min)	Titrate to pain/sedation goals; may require higher rates briefly in OR	Context-sensitive half-time increases with duration—be cautious with long infusions and weaning
Pediatric acute pain – IV bolus (specialist use)	0.5–1 mcg/kg IV (max 50–100 mcg per dose depending on age/setting)	Every 5–10 min as needed with close monitoring	Use lower doses in neonates/infants; follow PALS/pediatric anesthesia guidance
Intranasal fentanyl – acute severe pain (adult/peds)	1–2 mcg/kg IN (max 100–200 mcg) using 50 mcg/mL solution	May repeat once after 10–15 min depending on response and protocol	Divide dose between nares; ensure no major nasal obstruction; monitor as for IV opioids

Additional Dosing Notes:

Always titrate fentanyl to effect using the lowest effective dose, particularly in opioid-naïve, elderly, or frail patients
Bolus doses should be given slowly (over 1–2 minutes for standard analgesic boluses) to reduce risk of chest wall rigidity and abrupt hemodynamic changes
Avoid rapid large boluses (e.g., >5 mcg/kg given as a push) outside of controlled OR/anesthesia contexts with expert support, as these significantly increase risk of chest rigidity and apnea
In ventilated ICU patients, overlap fentanyl infusions with enteral or longer-acting analgesics when weaning to avoid withdrawal and rebound pain
Transdermal and transmucosal fentanyl products are contraindicated for acute pain in opioid-naïve patients; adhere strictly to opioid-tolerance criteria in their labeling

Contraindications

Contraindications (Acute IV/IN Use):

Known hypersensitivity to fentanyl or other phenylpiperidine opioids (e.g., sufentanil, alfentanil, remifentanil)
Severe, uncorrected respiratory depression or acute severe asthma in non-ventilated patients (relative; may still be used with airway support)
Caution/avoidance in patients with acute or severe bronchospasm where chest wall rigidity may worsen ventilation if muscle relaxants and airway control are not immediately available

Major Precautions:

Elderly, frail, or opioid-naïve patients: Increased sensitivity to respiratory depression and hypotension; use reduced doses and slower titration
Severe COPD, OSA, neuromuscular disease, or intracranial pathology: Monitor closely for hypoventilation and CO₂ retention; consider lower doses and alternative agents as appropriate
Concurrent CNS depressants (benzodiazepines, propofol, alcohol, gabapentinoids): Additive respiratory and hemodynamic depression; adjust doses accordingly and intensify monitoring
Bradyarrhythmias or conduction disease: Fentanyl can cause vagally mediated bradycardia; consider anticholinergic premedication in high-risk OR cases
Hepatic impairment: Reduced clearance and prolonged effect; start with lower doses and titrate cautiously
Transdermal/transmucosal fentanyl: Use only in opioid-tolerant patients meeting labeled criteria; inappropriate initiation in opioid-naïve individuals is a major overdose risk

Adverse Effects

Common:

Dose-dependent respiratory depression and hypoventilation
Sedation, dizziness, and altered mental status
Nausea and vomiting
Constipation with repeated dosing or infusions
Pruritus and mild flushing

Serious:

Apnea and severe respiratory depression: Requiring airway support and naloxone
Chest wall rigidity and glottic rigidity: Especially with high, rapid IV doses; may require neuromuscular blockade and mechanical ventilation
Profound bradycardia or asystole: Especially with high doses or in combination with other negative chronotropes
Severe hypotension: Particularly in hypovolemic or hemodynamically unstable patients
Opioid use disorder, tolerance, and withdrawal: With prolonged use
Accidental overdose and death: Particularly with high-potency formulations (concentrated IV, transdermal, transmucosal) and in opioid-naïve patients

Special Populations

Pediatrics: Use weight-based dosing (0.5–1 mcg/kg IV for acute pain); lower doses in neonates/infants; requires specialist guidance and close monitoring
Pregnancy: Opioids cross the placenta; chronic use during pregnancy can lead to neonatal abstinence syndrome; use lowest effective dose for shortest duration when necessary
Older Adults: Increased sensitivity to respiratory depression and sedation; start with lower doses (e.g., 25 mcg IV) and titrate slowly
Renal Impairment: Clearance of fentanyl itself is relatively preserved, but dose reductions and slower titration recommended in severe dysfunction
Hepatic Impairment: Reduced metabolism can increase exposure and prolong effect; use lower initial doses and slower titration with close monitoring

Monitoring Parameters (ED/ICU/Transport)

Continuous pulse oximetry and frequent respiratory rate assessment: After IV/IN dosing; capnography for moderate/deep sedation, ventilated patients, or high-risk individuals
Blood pressure and heart rate: At baseline and after dosing, especially in patients with cardiovascular disease or when co-administered with sedatives
Pain scores, sedation scales (e.g., RASS), and agitation/delirium assessments: In ICU patients receiving continuous fentanyl infusions
Signs of opioid toxicity: Pinpoint pupils, hypoventilation, unresponsiveness; readiness to administer naloxone when indicated
For long-term use: Monitor for constipation, endocrine effects, tolerance and dependence, and signs of misuse or diversion

Clinical Pearls

Rapid onset, accumulation with infusions: Fentanyl's rapid onset and short duration after small boluses make it ideal for titratable ED/ICU analgesia and for pre-intubation blunting of sympathetic surge, but prolonged infusions accumulate—plan for weaning and transition to longer-acting agents.

Chest wall rigidity recognition: If you see sudden difficulty ventilating after a big or rapid fentanyl bolus—especially with high airway pressures and a "tight" chest—think chest wall rigidity; treat with neuromuscular blockade and controlled ventilation rather than more bronchodilator alone.

Intranasal fentanyl utility: Intranasal fentanyl is a powerful tool when IV access is delayed: it provides rapid analgesia with minimal equipment and is well tolerated in children; monitor it like IV opioid, not like a "weak" nasal med.

ACS considerations: In ACS, balance analgesia with the risk of masking worsening ischemia; follow cardiology/local protocols regarding opioid use in acute coronary syndromes.

Naloxone reversal strategy: Naloxone should be titrated in small incremental doses (e.g., 40–80 mcg IV at a time) when reversing iatrogenic fentanyl-induced respiratory depression to avoid abrupt pain and catecholamine surge.

Dosing error prevention: Clear labeling of concentration (mcg/mL) and total dose in infusions is critical to avoid catastrophic dosing errors, especially in transport and interfacility handoffs.

References

1. Cheng, J., & Cohen, S. P. (2024). Fentanyl. In StatPearls [Internet]. StatPearls Publishing. https://www.ncbi.nlm.nih.gov/books/NBK459275/
2. DrugBank Online. (2024). Fentanyl (DB00813). DrugBank. https://go.drugbank.com/drugs/DB00813
3. Murphy, M. F., & Szokol, J. W. (2019). Opioid analgesics in anesthesia practice. In Miller's anesthesia (9th ed.). Elsevier.
4. Sinclair, J., & O'Connor, G. (2016). Intranasal fentanyl for the management of acute pain in children. Journal of Paediatrics and Child Health, 52(10), 924–931. https://doi.org/10.1111/jpc.13329
5. U.S. Food and Drug Administration. (2023). Fentanyl citrate injection prescribing information. DailyMed. https://dailymed.nlm.nih.gov