Propranolol: Comprehensive Drug Monograph

Pharmacokinetic Profile

Half-Life

3–6 hours (immediate-release); ~8–11 hours (long-acting / extended-release)

Metabolism

Hepatic via CYP2D6, CYP1A2, and CYP2C19

Bioavailability

~25% (extensive first-pass hepatic extraction)

Protein Binding

~90% (high; primarily to albumin and α1-acid glycoprotein)

Renal Excretion (Unchanged)

<1% (predominantly metabolised); not significantly dialysable

Clinical Information

Drug Class

Non-selective beta-adrenergic antagonist (β1 + β2); no ISA, no significant α-blockade at clinical doses

Available Doses (Reference Labels)

Inderal IR tablets: 10, 20, 40, 60, 80 mg · Inderal LA capsules: 60, 80, 120, 160 mg · Inderal XL / InnoPran XL capsules: 80, 120 mg · Hemangeol oral solution: 4.28 mg/mL · Generic oral solution: 4 or 8 mg/mL · IV: 1 mg/mL

Route

Oral (BID–QID for IR; once-daily for LA/XL); oral solution for paediatric dosing; IV for acute arrhythmia or thyroid storm

Renal Adjustment

No formal adjustment in mild–moderate impairment; use with caution in severe disease; not significantly dialysable

Hepatic Adjustment

Yes — initiate at lower doses; titrate gradually due to extensive hepatic extraction

Pregnancy

Crosses placenta; reports of intrauterine growth retardation, small placentas, neonatal bradycardia, hypoglycaemia, and respiratory depression

Lactation

Excreted in human milk at low levels; effects on breastfed infants generally not significant but caution advised

Schedule

Rx only; not controlled

Initial U.S. Approval

1967 (oral); first beta-blocker on the market — earned Sir James Black the 1988 Nobel Prize in Medicine

Indications

Propranolol was the first clinically successful beta-blocker and remains one of the most versatile drugs in pharmacology, with FDA-approved indications spanning cardiology, neurology, endocrinology, and paediatric dermatology. As a non-selective antagonist of both β1 and β2 receptors, it has a broader effect profile than the cardioselective beta-blockers (metoprolol, bisoprolol, atenolol), making it especially useful for indications where peripheral β2 blockade is therapeutic — essential tremor, migraine prophylaxis, performance anxiety, and infantile haemangioma — but also more likely to cause bronchospasm and unmasked vasoconstriction.

Indication	Population / Formulation	Therapy Type	Status
Hypertension — to lower blood pressure and reduce cardiovascular events	Adults; all oral formulations (Inderal, Inderal LA, Inderal XL, InnoPran XL)	Monotherapy or combination, particularly with thiazide diuretic	FDA Approved
Angina pectoris — long-term management of chronic stable angina due to coronary atherosclerosis	Adults; Inderal (IR) and Inderal LA	Monotherapy or with nitrates / calcium channel blockers	FDA Approved
Atrial fibrillation — control of ventricular rate; also for atrial flutter, supraventricular tachycardia, and digitalis-induced tachyarrhythmias	Adults; Inderal (IR oral and IV)	Monotherapy or with digoxin / non-DHP CCB	FDA Approved
Myocardial infarction — to reduce cardiovascular mortality after recent MI	Adults who survived the acute phase; Inderal (IR)	Long-term post-MI secondary prevention	FDA Approved
Migraine prophylaxis — prevention of common (episodic) migraine	Adults; Inderal (IR) and Inderal LA	Adjunct to lifestyle modification and trigger avoidance	FDA Approved (AAN Level A)
Essential tremor — familial or hereditary essential tremor	Adults; Inderal (IR)	First-line pharmacotherapy (with primidone)	FDA Approved
Hypertrophic obstructive cardiomyopathy (hypertrophic subaortic stenosis) — symptomatic relief of dynamic LV outflow obstruction	Adults; Inderal (IR)	First-line pharmacotherapy for symptomatic HOCM	FDA Approved
Pheochromocytoma — adjunctive control of tachycardia and tremor during preoperative management or in inoperable patients	Adults; Inderal (IR) — only after adequate alpha-blockade is established	Adjunct to alpha-adrenergic blocker	FDA Approved
Proliferating infantile haemangioma requiring systemic therapy	Infants 5 weeks to 5 months at initiation; Hemangeol oral solution	First-line systemic therapy	FDA Approved (2014; Hemangeol)
Performance anxiety / situational anxiety — symptom-targeted use for somatic anxiety	Adults; Inderal (IR), low intermittent doses	As-needed before triggering events	Off-Label (widely used)
Variceal bleeding prophylaxis in cirrhosis	Adults with documented oesophageal varices	Primary or secondary prophylaxis (alternative to carvedilol)	Off-Label (guideline-supported)
Thyrotoxicosis / thyroid storm — symptomatic adrenergic control	Adults; Inderal (IR oral and IV)	Adjunct to definitive thyroid therapy	Off-Label (well-established)
Antipsychotic-induced akathisia	Adults; Inderal (IR), low doses	First-line pharmacotherapy	Off-Label (clinically established)
Post-traumatic stress disorder (PTSD) — adjunctive symptom management	Adults	Adjunct to standard PTSD therapy	Off-Label (limited evidence)

The breadth of propranolol’s indication list reflects its mechanistic versatility: peripheral β2 blockade addresses physical anxiety symptoms (tremor, palpitations) and tremor itself; central CNS penetration mediates migraine prophylaxis (mechanism incompletely understood); and the unique 2014 paediatric approval for infantile haemangioma (Hemangeol) followed the serendipitous 2008 observation by Léauté-Labrèze and colleagues that an infant treated for cardiomyopathy showed dramatic regression of a facial haemangioma. Hemangeol is the only FDA-approved systemic therapy for proliferating infantile haemangioma.

Off-Label and Special-Population Uses

Performance anxiety — propranolol 10–40 mg taken 30–60 minutes before a triggering event blunts the somatic adrenergic response (tachycardia, tremor) without sedation. Particularly useful for musicians, public speakers, and surgical trainees. Evidence quality: moderate (small trials).

Variceal bleeding prophylaxis — non-selective beta-blockade reduces portal pressure via splanchnic vasoconstriction (β2 effect) and decreased cardiac output. Evidence quality: high (long-standing guideline support).

Akathisia (antipsychotic-induced) — propranolol 30–80 mg/day in divided doses is frequently first-line; benztropine is preferred for parkinsonism. Evidence quality: moderate.

Thyroid storm — propranolol 60–80 mg PO every 4 hours, or 0.5–1 mg IV slow push (titrated cautiously); also has weak inhibitory effect on peripheral T4-to-T3 conversion. Evidence quality: high (standard of care).

Dose

Dosing

Clinical Scenario	Starting Dose	Titration / Maintenance	Maximum Dose	Notes
Hypertension — adult, immediate-release (Inderal)	40 mg PO twice daily (alone or added to a diuretic)	Increase gradually; usual maintenance 120–240 mg/day in 2–3 divided doses	640 mg/day	Twice-daily dosing typically sufficient; some patients require TID dosing for 24-hour control Full antihypertensive response may take several weeks
Hypertension — adult, long-acting (Inderal LA)	80 mg PO once daily	Maintenance 120–160 mg once daily	640 mg/day	Once-daily dosing supports adherence; equivalent total daily dose to IR
Hypertension — adult, extended-release (InnoPran XL / Inderal XL)	80 mg PO once daily at bedtime (~10 p.m.)	May increase every 2–3 weeks; maintenance 80–120 mg/day	120 mg/day	Bedtime dosing produces peak plasma levels in the early morning, targeting the morning BP surge Doses above 120 mg confer no additional BP-lowering effect per the Inderal XL PI
Chronic stable angina — adult, IR	10–20 mg PO three times daily (or 80 mg LA once daily)	Increase weekly; usual range 80–320 mg/day in 2–4 divided doses	320 mg/day	Resting heart rate target generally 55–60 bpm
Atrial arrhythmias / SVT — IV (acute)	1–3 mg IV slow push at maximum rate of 1 mg/minute	May repeat after 2 minutes; subsequent doses no sooner than every 4 hours	Typically 5 mg cumulative in acute setting	Continuous ECG and BP monitoring; have atropine, fluids, glucagon available Transition to oral therapy as soon as feasible
Atrial arrhythmias / SVT — oral, IR	10–30 mg PO three to four times daily before meals and at bedtime	Titrate to rate control and symptom relief	Per indication and tolerability	For chronic AF rate control, total daily doses of 80–240 mg are common
Post-MI mortality reduction — adult, IR	40 mg PO three times daily initially	Increase to 60–80 mg three times daily as tolerated; total daily dose 180–240 mg in 3–4 divided doses	240 mg/day per the Inderal PI for this indication	Begin in early convalescence (typically 5–21 days post-infarction). Patients are generally transitioned to a once-daily long-acting beta-blocker for chronic post-MI therapy Cardioselective agents (metoprolol succinate, bisoprolol) are now usually preferred
Migraine prophylaxis — adult, IR	80 mg/day PO in divided doses (or 80 mg LA once daily)	Increase gradually; usual range 160–240 mg/day	240 mg/day per the Inderal PI for this indication	If satisfactory response not seen within 4–6 weeks at the maximum tolerated dose, discontinue gradually
Essential tremor — adult, IR	40 mg PO twice daily	Increase as tolerated; usual maintenance 120–320 mg/day in divided doses	320 mg/day per the Inderal PI for this indication	Best response often at 80–160 mg/day; primidone is the alternative first-line agent
Hypertrophic obstructive cardiomyopathy — adult, IR	20–40 mg PO three to four times daily before meals and at bedtime	Titrate to symptom relief	Per tolerability	Higher doses than for hypertension may be needed
Pheochromocytoma (preoperative) — adult, IR	60 mg/day PO in divided doses for 3 days before surgery	Adjusted to control tachycardia and tremor	Per tolerability	Only after adequate alpha-blockade is established — beta-blocker alone causes paradoxical hypertension. For inoperable malignant pheochromocytoma: ~30 mg/day in divided doses
Performance / situational anxiety (off-label)	10–40 mg PO taken 30–60 minutes before the triggering event	Adjust based on response and tolerability for future events	Use intermittent dosing; not for daily/chronic anxiety	Lowest effective dose; avoid if asthma history
Akathisia — adult, IR (off-label)	10–20 mg PO three times daily	Titrate to symptom relief; usual range 30–80 mg/day	120 mg/day	Onset of relief typically within hours to days
Variceal bleeding prophylaxis — adult, IR (off-label)	20 mg PO twice daily	Titrate to ~25% reduction in resting HR or HR ~55 bpm; usual range 40–160 mg/day	320 mg/day	Carvedilol is increasingly preferred per current guidance; nadolol is an equivalent non-selective alternative
Thyroid storm — adult, IR oral or IV (off-label)	PO: 60–80 mg every 4 hours IV: 0.5–1 mg slow IV push with continuous monitoring	Titrate to HR and adrenergic symptom control	Per haemodynamics	Caution in patients with thyroid-storm-related cardiomyopathy (may precipitate decompensation)
Proliferating infantile haemangioma — Hemangeol oral solution	0.6 mg/kg twice daily (0.15 mL/kg of 4.28 mg/mL solution), at least 9 hours apart	Week 2: increase to 1.1 mg/kg twice daily Week 3 onward: 1.7 mg/kg twice daily for 6 months total	1.7 mg/kg twice daily (3.4 mg/kg/day)	Initiate at 5 weeks to 5 months of age; not for infants <2 kg or <5 weeks corrected age. Give during or right after a feeding to reduce hypoglycaemia risk; skip dose if not feeding or vomiting Monitor HR and BP for 2 hours after first dose and after each dose increase. Generic oral propranolol (4 or 8 mg/mL) is also widely used at 1–3 mg/kg/day in divided doses but requires careful prescribing to avoid concentration-related dosing errors
Discontinuation	Reduce gradually over 1–2 weeks (typical halving every 3–7 days)			Abrupt withdrawal may exacerbate ischaemia, precipitate MI in CAD, cause rebound tachycardia/hypertension, or precipitate thyroid storm in thyrotoxic patients

Population-Specific Considerations

Population	Adjustment	Rationale
Renal impairment	Use with caution	Less than 1% excreted unchanged; metabolites have minimal beta-blocking activity. Use cautiously per the Inderal PI; not significantly removed by haemodialysis
Hepatic impairment	Initiate at lower doses; titrate gradually	Extensive first-pass hepatic metabolism — bioavailability and plasma levels increase substantially with hepatic dysfunction
Elderly	Lower starting dose; cautious titration	Per the Inderal PI: greater frequency of decreased hepatic, renal, or cardiac function; concomitant disease and drug therapy
Paediatric (general indications)	Safety and effectiveness not established for adult cardiovascular indications	Bronchospasm and congestive heart failure have been reported coincident with paediatric administration per the Inderal PI
Paediatric (infantile haemangioma)	Hemangeol per body weight as above; do not use in infants <2 kg or <5 weeks corrected age	FDA-approved indication with age- and weight-specific labelling
CYP2D6 poor metabolisers	Expect higher exposure; cautious titration	Multiple metabolic pathways (CYP2D6, 1A2, 2C19) provide some compensation, but propranolol exposure is meaningfully higher in CYP2D6 poor metabolisers
Pregnancy	Use only if benefit clearly outweighs risk	Crosses placenta; reports of intrauterine growth retardation, small placentas, congenital abnormalities. Neonatal monitoring at delivery for bradycardia, hypoglycaemia, and respiratory depression

Clinical Pearl — Choosing the Right Formulation

For chronic indications (hypertension, migraine prophylaxis, essential tremor, post-MI), once-daily long-acting formulations (Inderal LA, Inderal XL, InnoPran XL) generally improve adherence over IR. InnoPran XL is uniquely designed for bedtime dosing with peak plasma concentrations 12–14 hours later — useful for patients with prominent morning blood-pressure surge. For acute or rapidly titrated indications (acute arrhythmia, thyroid storm, situational anxiety, hospitalised patients), the IR tablet or IV preparation is preferred. For infantile haemangioma, Hemangeol is the only formulation with FDA approval for this indication and pre-validated paediatric concentration (4.28 mg/mL); generic oral solutions exist in two concentrations (4 mg/mL and 8 mg/mL) and require careful prescribing to avoid dosing errors.

Pharmacology

Mechanism of Action

Propranolol is a non-selective competitive antagonist at both β1- and β2-adrenergic receptors, with no intrinsic sympathomimetic activity and no significant alpha-adrenergic effect at clinical doses. β1 blockade in the heart reduces resting and exercise heart rate, slows AV nodal conduction, and decreases myocardial contractility — together lowering cardiac output and myocardial oxygen demand. β2 blockade in vascular smooth muscle, bronchi, and metabolic tissues accounts for distinctive features of propranolol versus cardioselective agents: cold extremities and peripheral vasoconstriction; bronchospasm in susceptible patients; impaired hypoglycaemic counter-regulation; reduced essential and physiological tremor; and reduced portal pressure in cirrhotic varices via splanchnic vasoconstriction.

Membrane-stabilising activity is detectable only at concentrations far above those needed for beta-blockade and is not clinically relevant. Propranolol is highly lipophilic, crosses the blood-brain barrier readily, and exerts central effects implicated in its efficacy for migraine prophylaxis, essential tremor, performance anxiety, and akathisia. The mechanism by which propranolol promotes regression of infantile haemangiomas is incompletely understood; proposed mechanisms include vasoconstriction, inhibition of angiogenesis (via downregulation of VEGF and bFGF), and induction of apoptosis in capillary endothelial cells.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Rapidly and almost completely absorbed orally; absolute bioavailability ~25% due to extensive first-pass hepatic metabolism. Peak plasma concentrations within 1–4 hours for IR; for InnoPran XL given at 10 p.m., steady-state Tmax 12–14 hours after dosing. Food may increase bioavailability of IR by reducing first-pass extraction	Substantial inter-patient variability in plasma levels with the same oral dose. The IV-to-oral dose ratio is approximately 1:10 because of first-pass metabolism
Distribution	Approximately 90% bound to plasma proteins (primarily albumin and α1-acid glycoprotein). Highly lipophilic — readily crosses the blood-brain barrier with appreciable CSF concentrations; also crosses the placenta and is excreted in breast milk	CNS penetration accounts for fatigue, vivid dreams, depressive symptoms, and the central efficacy in migraine and tremor. The high protein binding is rarely clinically meaningful but is relevant in severe hypoalbuminaemia
Metabolism	Extensively metabolised in the liver via CYP2D6, CYP1A2, and CYP2C19. Primary metabolites include 4-hydroxypropranolol (active) and naphthyloxylactic acid. Multiple metabolic pathways provide partial protection against any single CYP inhibitor or polymorphism	Strong inhibitors of CYP2D6 (paroxetine, fluoxetine, bupropion, quinidine), CYP1A2 (cimetidine, fluvoxamine, ciprofloxacin, smoking cessation), or CYP2C19 (fluvoxamine, fluconazole) raise propranolol exposure. Inducers of CYP1A2 (smoking, rifampicin) or CYP2C19 (rifampicin) lower exposure
Elimination	Plasma half-life 3–6 hours for IR; ~8 hours for InnoPran XL; 8–11 hours for sustained-release formulations. Less than 1% of an oral dose is excreted unchanged in urine — propranolol is essentially eliminated as inactive or partly active metabolites. Not significantly dialysable	No renal dose adjustment generally needed. Hepatic impairment substantially raises exposure — initiate at lower dose. The longer apparent half-life of LA/XR formulations reflects sustained release rather than slower elimination

Pharmacodynamic Note — Non-Selective Profile

Propranolol’s non-selectivity is both its strength and its limitation. The β2 effect underlies several distinctive therapeutic uses (essential tremor, migraine, performance anxiety, variceal prophylaxis, infantile haemangioma) and several distinctive adverse effects (bronchospasm, peripheral vasoconstriction, exaggerated hypoglycaemic episodes). For patients in whom the β1 cardiac effect is the primary therapeutic goal — chronic heart failure, isolated hypertension in patients with reactive airways disease, diabetics — a cardioselective beta-blocker (metoprolol succinate, bisoprolol) is generally preferred. Propranolol’s CNS penetration also makes it more likely than less-lipophilic agents (atenolol, nadolol) to cause fatigue, sleep disturbance, vivid dreams, and depressive symptoms.

Side Effects

Propranolol’s adverse-effect profile reflects β1 (cardiac) antagonism, β2 (peripheral and metabolic) antagonism, and prominent CNS penetration. The Inderal prescribing information notes that “the following adverse reactions have been observed, but there is not enough systematic collection of data to support an estimate of their frequency” — historic clinical-trial reporting predates the modern requirement for tabulated incidence rates. Specific quantitative rates below are drawn from the InnoPran XL PI (Table 1, ≥3% reporting threshold) and from the Hemangeol paediatric trials. Most adverse effects are mild and transient.

≥3% (InnoPran XL) Treatment-Emergent Adverse Events Reported in ≥3% of Subjects (InnoPran XL clinical trials)

Adverse Effect	Reported Incidence	Clinical Note
Fatigue	Common (≥3%)	Often dose-related; may improve over the first 2–4 weeks. A common reason for early discontinuation; consider lowering dose before stopping.
Dizziness	Common (≥3%)	Frequently orthostatic; counsel patients to rise slowly. More common at initiation and after dose increases.
Bradycardia	Common (≥3%)	Symptomatic if HR <50 bpm or accompanied by hypotension; reduce dose or discontinue.
Cold extremities	Common (β2-mediated)	Reflects loss of β2-mediated peripheral vasodilatation; more common with non-selective agents than with cardioselective beta-blockers.
Headache, insomnia, vivid dreams, nightmares	CNS-penetrant beta-blocker class effect	Switching to a less lipophilic agent (atenolol, nadolol) may help; bedtime dosing of long-acting formulations occasionally helps.
Gastrointestinal: nausea, diarrhoea, constipation	Common	Usually mild and self-limited.

Hemangeol (Paediatric) Most Common Adverse Reactions in Paediatric Trials of Hemangeol

Adverse Effect	Reported Frequency	Clinical Note
Sleep disorders / disturbance	Most common	Most commonly reported AE in the Hemangeol paediatric trial; usually mild and not requiring discontinuation.
Worsening respiratory tract infections (bronchiolitis, bronchitis)	Common	Per the Hemangeol PI, treatment should be interrupted in the event of a lower respiratory tract infection associated with dyspnoea and wheezing.
Diarrhoea, vomiting	Common	Skip the dose if the infant is not feeding or is vomiting (hypoglycaemia risk); resume when feeding normally.
Bradycardia (mean ~7 bpm decrease)	Mean change in HF studies; severe bradycardia uncommon	Per the Hemangeol PI, discontinue treatment if severe bradycardia (<80 bpm) or symptomatic bradycardia or hypotension occurs.

Serious Serious / Rare but Important (Including Post-Marketing)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Bronchospasm	Particular concern in patients with reactive airways disease — propranolol contraindicated in bronchial asthma	Within hours of dose	Inhaled β2-agonist (high-dose may be needed); discontinue propranolol; consider inhaled ipratropium and systemic corticosteroids if severe
Symptomatic bradycardia, sinus pause, AV block, cardiac arrest	Rare; risk higher with concomitant non-DHP CCB or in conduction disease	Hours to days after initiation or dose increase	Hold drug; atropine; transcutaneous or transvenous pacing for severe AV block; IV glucagon (3–10 mg) for refractory beta-blocker toxicity. Per the InnoPran XL PI, epinephrine may provoke uncontrolled hypertension and is not indicated for propranolol overdose
Severe rebound on abrupt withdrawal (ischaemia, MI, ventricular arrhythmia, thyroid storm in thyrotoxic patients)	Documented	Days after stopping	Avoid abrupt withdrawal; taper over 1–2 weeks; reinstitute promptly if rebound occurs
Severe / prolonged hypoglycaemia (especially in children, fasting patients, patients on insulin, perioperatively)	Greater concern with non-selective beta-blockers	During hypoglycaemic episodes	Counsel on non-adrenergic warning signs; in Hemangeol-treated infants, give doses with feeds and skip if not eating. Severe hypoglycaemia warrants emergency treatment
Anaphylaxis with relative resistance to adrenaline	Rare but particularly concerning with non-selective agents	Variable	Higher-dose adrenaline, IV glucagon (especially helpful for beta-blocker–related refractoriness), IV fluids, antihistamines, corticosteroids
Hypertensive crisis in unrecognised pheochromocytoma (without alpha-blockade)	Rare but predictable	Within hours	Always start alpha-blocker before any beta-blocker in suspected pheochromocytoma. If crisis occurs: IV phentolamine
Worsening peripheral arterial disease, Raynaud-type symptoms	Reported; non-selective agents are more likely to aggravate than cardioselective	Variable	Assess claudication and distal perfusion; consider switching to a vasodilating beta-blocker (carvedilol, nebivolol) if symptomatic
Heart failure exacerbation	Reported with abrupt initiation in HF	Days to weeks	Propranolol is NOT FDA-approved for chronic heart failure; metoprolol succinate, bisoprolol, or carvedilol are the evidence-based agents for this indication
Stroke (in PHACE syndrome)	Specific concern in infants with PHACE syndrome and severe cerebrovascular disease	Variable	Per the Hemangeol PI, lowering BP may increase stroke risk in PHACE syndrome patients with severe arteriopathy of the head and neck; screen large segmental facial haemangiomas for PHACE features
Hypersensitivity / anaphylactic-anaphylactoid reactions, agranulocytosis, thrombocytopenic and nonthrombocytopenic purpura (post-marketing)	Very rare	Variable	Discontinue; haematology assessment as appropriate
Cutaneous reactions: Stevens-Johnson syndrome, toxic epidermal necrolysis, exfoliative dermatitis, erythema multiforme, urticaria (post-marketing)	Very rare	Variable	Permanent discontinuation; dermatology referral; supportive care
Drug-induced lupus / SLE-like reactions, psoriasiform rashes, alopecia (post-marketing)	Very rare	Months to years	Discontinuation usually leads to resolution
Sexual dysfunction (erectile dysfunction, decreased libido, Peyronie’s disease)	Reported in PI; class effect	Variable	Often underreported; consider switching to a vasodilating beta-blocker (nebivolol) if this becomes a barrier to adherence

Discontinuation Discontinuation Patterns

Adult Cardiovascular & Migraine Indications

Modest

Top reasons: fatigue, sexual dysfunction, vivid dreams or sleep disturbance, cold extremities, depressive symptoms. Most discontinuations are for tolerability rather than safety.

Hemangeol (Infantile Haemangioma)

Low

Top reasons in trial: intolerable sleep disturbance, recurrent respiratory tract infections with dyspnoea, hypoglycaemia events, severe bradycardia or hypotension. Discontinuation rate in the pivotal Hemangeol trial was low.

Reason for Discontinuation	Relative Frequency	Context
Fatigue / exercise intolerance	Most common tolerability reason	Often improves over 2–4 weeks; consider dose reduction before discontinuation.
CNS effects (vivid dreams, depression, sleep disturbance)	More common than with cardioselective beta-blockers	Switching to atenolol or nadolol (less lipophilic) may resolve.
Bronchospasm	Particular concern in patients with reactive airways disease	Reactive airways disease is a contraindication to non-selective beta-blockers; switch to cardioselective (with caution) if absolutely necessary.
Worsening peripheral vascular disease, Raynaud’s symptoms, cold extremities	More common with non-selective agents	Switch to a vasodilating beta-blocker (nebivolol, carvedilol) if continuation is needed.
Sexual dysfunction	Common but underreported	Class effect; nebivolol may have a more favourable profile.

Management — Beta-Blocker Toxicity

Severe propranolol toxicity (intentional or accidental overdose, drug interaction, or hepatic impairment) presents with bradycardia, hypotension, AV block, bronchospasm, hypoglycaemia, seizures, and impaired consciousness. Critical management points: (1) IV glucagon (3–10 mg bolus, then infusion 2–5 mg/hour) is the most reliable antidote — it bypasses beta-receptor blockade and stimulates cardiac contractility via Gs-mediated cAMP. (2) Per the InnoPran XL PI, adrenaline should be used cautiously because beta-blockade with unopposed alpha-stimulation can provoke uncontrolled hypertension; isoproterenol or dobutamine (competitive β-agonists) may be more appropriate. (3) Atropine for bradycardia, transcutaneous pacing for severe AV block, IV fluids and vasopressors for hypotension. (4) Inhaled β2-agonists (potentially high doses) for bronchospasm; aminophylline if needed. (5) Propranolol is not significantly removed by haemodialysis.

Int

Drug Interactions

Propranolol’s interaction profile is broader than that of cardioselective beta-blockers because it is metabolised by three CYP enzymes (CYP2D6, CYP1A2, CYP2C19) and because non-selective β-blockade has more pharmacodynamic interaction targets — particularly with adrenaline (vasoconstrictor crisis) and bronchodilators (β2 antagonism). Pharmacodynamic interactions are at least as clinically important as the pharmacokinetic ones.

Major Adrenaline (epinephrine) — for anaphylaxis or vasoconstriction

MechanismBeta-blockade leaves alpha-adrenergic vasoconstriction unopposed when adrenaline is given; also blunts the desired cardiac response in anaphylaxis

EffectUncontrolled hypertension and reflex bradycardia; reduced anaphylaxis response. Per the InnoPran XL PI, epinephrine is NOT indicated for propranolol overdose

ManagementUse IV glucagon, IV fluids, antihistamines, and corticosteroids preferentially. If adrenaline is used, prepare for higher doses; have phentolamine available for hypertensive crisis

FDA PI

Major Verapamil, diltiazem (non-DHP calcium channel blockers)

MechanismAdditive negative chronotropy, dromotropy, and inotropy at the AV node

EffectRisk of severe bradycardia, AV block, hypotension, and cardiogenic shock — particularly with IV verapamil

ManagementAvoid IV verapamil in patients on propranolol. Oral combination requires close monitoring; lower doses of both agents

FDA PI

Major Clonidine

MechanismBeta-blockade exacerbates rebound hypertension that follows clonidine withdrawal

EffectSevere rebound hypertension on clonidine cessation

ManagementWithdraw beta-blocker several days before gradual clonidine withdrawal. If switching from clonidine to a beta-blocker, delay beta-blocker initiation several days after stopping clonidine

FDA PI

Major Strong CYP2D6 inhibitors (paroxetine, fluoxetine, bupropion, quinidine, terbinafine)

MechanismInhibition of one of the three major CYP pathways for propranolol metabolism

EffectIncreased propranolol exposure; exaggerated bradycardia, hypotension, fatigue, CNS effects

ManagementUse lower starting dose; choose a non-CYP2D6 SSRI (sertraline, citalopram, escitalopram) when possible; monitor HR and BP closely

FDA PI

Moderate Strong CYP1A2 inhibitors (cimetidine, fluvoxamine, ciprofloxacin)

MechanismInhibition of CYP1A2 metabolism of propranolol

EffectIncreased propranolol exposure; cimetidine and fluvoxamine increase levels several-fold

ManagementSubstitute famotidine or pantoprazole for cimetidine; choose alternative quinolones when possible. Monitor HR and BP if combination cannot be avoided

FDA PI

Moderate CYP1A2 inducers (rifampicin, smoking, phenytoin, carbamazepine)

MechanismInduction of CYP1A2 (and partially CYP2C19) increases propranolol clearance

EffectReduced propranolol exposure and efficacy. Smoking cessation may unmask elevated levels

ManagementHigher doses may be needed in heavy smokers; reassess after smoking cessation. Monitor HR/BP when starting or stopping inducers

FDA PI

Moderate Warfarin

MechanismPropranolol can prolong prothrombin time

EffectPossible elevation in INR with concurrent use

ManagementPer the Inderal XL PI, monitor prothrombin time when propranolol is co-administered with warfarin

FDA PI

Moderate Lidocaine

MechanismPropranolol reduces hepatic blood flow and lidocaine clearance

EffectIncreased lidocaine plasma levels and risk of toxicity

ManagementUse lower lidocaine doses and monitor for toxicity (paraesthesia, confusion, seizures, conduction abnormalities)

FDA PI

Moderate Insulin and oral hypoglycaemics

MechanismNon-selective beta-blockade masks adrenergic warning signs of hypoglycaemia (tachycardia, tremor) AND impairs hepatic glucose mobilisation via β2 antagonism

EffectGreater hypoglycaemia risk than with cardioselective beta-blockers; both unrecognition AND prolonged hypoglycaemia

ManagementCardioselective beta-blocker (metoprolol, bisoprolol) preferred in diabetics requiring beta-blocker therapy. If propranolol used, intensive glucose monitoring

FDA PI

Moderate NSAIDs (ibuprofen, naproxen, indomethacin)

MechanismReduce renal prostaglandin synthesis; sodium and water retention

EffectAttenuated antihypertensive effect

ManagementUse NSAIDs at lowest effective dose for shortest duration; reassess BP if regular use

Class effect

Minor Aluminium-containing antacids

MechanismReduce propranolol absorption

EffectModestly decreased propranolol levels

ManagementSeparate administration by ≥2 hours

Lexicomp

Minor Alcohol

MechanismAlcohol may transiently increase propranolol plasma levels

EffectAdditive hypotension and CNS depression

ManagementCounsel patients to avoid heavy alcohol intake

FDA PI

Practical Take-Home — Three Interactions That Matter Most

(1) Adrenaline interaction — the most clinically dangerous: in patients on chronic propranolol who develop anaphylaxis, the usual adrenaline doses may be insufficient, and unopposed alpha-stimulation may cause hypertensive crisis. Have IV glucagon available. (2) Verapamil/diltiazem combination — the most common cardiology pitfall, particularly in atrial fibrillation rate control. (3) CYP1A2 dynamics with smoking — heavy smokers may need higher doses; smoking cessation can unmask elevated propranolol levels and excess bradycardia.

Mon

Monitoring

Heart Rate Baseline, at each titration step, then at each follow-up
Routine Target resting HR generally 55–70 bpm depending on indication. For variceal prophylaxis, target ~25% reduction or HR ~55 bpm. For Hemangeol-treated infants, the PI specifies discontinuation if HR <80 bpm or symptomatic bradycardia. Monitor for 2 hours after the first Hemangeol dose and after each dose increase.
Blood Pressure Baseline, at each titration step, then at each follow-up
Routine Check both seated and standing. Symptomatic orthostasis or SBP <100 mmHg in adults, or SBP <50 mmHg in Hemangeol-treated infants, prompts dose reassessment. Continuous monitoring during IV propranolol administration.
ECG Baseline; repeat for symptomatic bradycardia or new conduction symptoms
Trigger-based Particularly important in patients with first-degree AV block, sinus node dysfunction, or conduction disorders (including Wolff-Parkinson-White, where propranolol may unmask severe bradycardia after termination of pre-excited tachycardia).
Respiratory Symptoms At each visit and at each dose escalation
Routine Particularly important given non-selective β2 blockade. Bronchial asthma is a contraindication to propranolol. In Hemangeol-treated infants, treatment should be interrupted during lower respiratory tract infections with dyspnoea or wheezing.
Glycaemic Status (in diabetics; all Hemangeol patients) Routinely in diabetics; symptom-guided in infants
Routine Non-selective beta-blockade impairs both adrenergic warning signs AND hepatic glucose mobilisation, increasing risk of severe and prolonged hypoglycaemia compared with cardioselective agents. For Hemangeol: give with feeds, skip if not feeding/vomiting, parents counselled on hypoglycaemia signs.
Mood, Sleep, Cognitive Function At each visit (open-ended enquiry)
Routine CNS effects (vivid dreams, depressive symptoms, impaired concentration, mental clouding) are more common with lipophilic non-selective propranolol than with hydrophilic agents. Switching to atenolol or nadolol may help.
Sexual Function At each follow-up (open-ended enquiry)
Routine Class effect, often underreported. Vasodilating beta-blockers (nebivolol) may have a more favourable profile if sexual dysfunction becomes a barrier to adherence.
Peripheral Perfusion At each visit if PVD or Raynaud’s history
Trigger-based Cold extremities are common; worsening claudication, new resting pain, or trophic skin changes warrant reassessment.
PHACE Syndrome Screening (in infantile haemangioma patients) Before initiating Hemangeol for large facial haemangiomas
Trigger-based Per the Hemangeol PI, propranolol-induced BP lowering may increase stroke risk in PHACE syndrome patients with severe arteriopathy of the head and neck. Imaging (MRI/MRA brain) is recommended for large segmental facial haemangiomas before initiation.
Glaucoma Screening Inform optometrist/ophthalmologist if relevant
Trigger-based Beta-blockade reduces intraocular pressure; per the Inderal PI, patients should be told that propranolol may interfere with glaucoma screening tests.
Adherence At each follow-up
Routine Particularly important because abrupt withdrawal — including from missed doses or running out of supply — can precipitate ischaemia in CAD, rebound hypertension, ventricular arrhythmia, or thyroid storm in thyrotoxic patients.

The Two Vitals That Matter Most

For routine adult propranolol monitoring, two vitals dominate: heart rate and blood pressure, checked at every titration step and at each follow-up. For Hemangeol-treated infants, the PI specifies 2 hours of HR and BP monitoring after the first dose and after each dose increase — this is a structured surveillance window that is non-negotiable. Once stable on maintenance dose with stable vitals, follow-up at 3–6 months is typically sufficient for adults; monthly (with weight-based dose adjustments) for Hemangeol over the 6-month treatment course.

Contraindications & Cautions

Absolute Contraindications (Adult Indications, per Inderal / Inderal XL PI)

Cardiogenic shock
Sinus bradycardia and greater than first-degree heart block (unless a permanent pacemaker is in place)
Sick sinus syndrome (unless a permanent pacemaker is in place)
Bronchial asthma — propranolol is a non-selective beta-blocker and is specifically contraindicated; this is a key distinction from cardioselective metoprolol or bisoprolol
Known hypersensitivity (e.g., anaphylactic reaction) to propranolol hydrochloride or any of the components

Additional Hemangeol-Specific Contraindications (Per Hemangeol PI)

Premature infants <5 weeks corrected gestational age
Infants weighing <2 kg
Asthma or history of bronchospasm
Heart rate <80 bpm (for an infant)
Greater than first-degree heart block
Decompensated heart failure
Blood pressure <50/30 mmHg
Pheochromocytoma
Hypersensitivity to propranolol or excipients

Relative Contraindications (Specialist Input Recommended)

Severe peripheral vascular disease with critical limb ischaemia or rest pain — non-selective beta-blockade may exacerbate symptoms; consider a vasodilating beta-blocker (nebivolol, carvedilol)
Prinzmetal (vasospastic) angina — unopposed alpha-mediated coronary vasoconstriction may worsen vasospasm; calcium channel blockers preferred
Severe hepatic impairment — substantially elevated plasma exposure; if used, start at lower than usual dose
Untreated pheochromocytoma — alpha-blocker must be initiated first; beta-blocker alone causes paradoxical hypertensive crisis
Diabetes mellitus, particularly insulin-treated — non-selective beta-blockade increases hypoglycaemia risk more than cardioselective agents; cardioselective agent preferred unless propranolol-specific indication exists
Pregnancy — not absolutely contraindicated and used when treatment is necessary, but crosses placenta; reports of intrauterine growth retardation, neonatal bradycardia, hypoglycaemia, and respiratory depression
PHACE syndrome with severe cerebrovascular arteriopathy (in Hemangeol candidates) — relative contraindication due to stroke risk; case-by-case decision after imaging

Use with Caution

Heart failure — propranolol is NOT FDA-approved for chronic heart failure; metoprolol succinate, bisoprolol, or carvedilol are the evidence-based agents. May be used cautiously when propranolol has a separate indication (e.g., post-MI, AF rate control)
Mild–moderate COPD — generally avoid; if a beta-blocker is essential, choose a cardioselective agent at lowest dose
Hyperthyroidism — useful for adrenergic symptom control but may mask tachycardia. Withdraw gradually after definitive thyroid therapy to avoid precipitating thyroid storm
Anaphylaxis history — beta-blockade may blunt response to adrenaline used for treatment; have IV glucagon available
Major surgery — abrupt withdrawal can precipitate perioperative myocardial ischaemia; continue chronic beta-blocker through the perioperative period whenever feasible. Avoid initiation of high-dose beta-blocker shortly before non-cardiac surgery in beta-blocker-naïve patients (POISE trial)
Concurrent non-DHP calcium channel blocker therapy — additive AV nodal slowing
Myasthenia gravis — may exacerbate muscle weakness

FDA Regulatory Note No Boxed Warning, but Class Cautions Apply

Propranolol does not carry an FDA boxed warning. The FDA prescribing information emphasises the risk of acute exacerbation of myocardial ischaemia or precipitation of MI on abrupt withdrawal in patients with known coronary disease — therapy should be tapered over 1–2 weeks rather than stopped suddenly. The PI also flags propranolol’s specific contraindication in bronchial asthma (a key distinction from cardioselective beta-blockers), warns that epinephrine should be used cautiously in propranolol overdose due to risk of unopposed alpha-stimulation and uncontrolled hypertension, and requires that an alpha-blocker be initiated before propranolol in pheochromocytoma to avoid paradoxical hypertensive crisis.

The Hemangeol PI further specifies a structured 2-hour monitoring window after the first dose and after each dose increase, mandates dose-skipping during fasting or vomiting (hypoglycaemia risk), and identifies stroke as a specific concern in PHACE syndrome with severe arteriopathy of the head and neck.

Patient Counselling

Purpose of Therapy

Explain that propranolol is a “beta-blocker” — one of the oldest and most versatile heart medications. Depending on what it is being prescribed for, it slows the heart, lowers blood pressure, prevents migraines, reduces hand tremor, calms physical anxiety symptoms (rapid heartbeat, shaking), or in infants treats a specific type of birthmark called an infantile haemangioma. Unlike newer beta-blockers (such as metoprolol), propranolol blocks both kinds of beta receptors in the body — making it more useful for some non-cardiac conditions but also more likely to cause cold hands, breathing issues in people with asthma, and sleep changes.

How to Take

Take propranolol exactly as prescribed. Immediate-release tablets are usually taken 2–4 times daily, ideally with or after meals. Long-acting capsules (Inderal LA, Inderal XL) are taken once daily. InnoPran XL extended-release is taken at bedtime, around 10 p.m., to time the medicine to reach peak levels in the morning. Long-acting capsules must be swallowed whole — do not crush, chew, or open them. Take it consistently, the same way each time. Do not stop suddenly. Stopping abruptly can cause chest pain, fast heart rate, rebound high blood pressure, and in people with heart disease can trigger a heart attack. In thyroid disease, sudden stopping can also trigger a thyroid storm. If you need to stop, your prescriber will guide you through a 1–2 week taper.

For Hemangeol (infantile haemangioma): Always give during or right after a feeding to reduce the risk of low blood sugar. Use the dosing syringe that came with the bottle — never a household spoon. Give two doses at least 9 hours apart. If your baby is not eating or is vomiting, skip the dose — do not catch up later. Throw the bottle away 2 months after first opening it. Keep your baby’s clinic appointments — the dose changes as your baby grows.

Tiredness, Dizziness, and Cold Hands or Feet

Tell patient Tiredness and dizziness are common in the first 2–4 weeks and often improve. Cold hands and feet are particularly common with propranolol because it narrows surface blood vessels; layers and warm gloves help. Stand up slowly, especially in the morning.

Call prescriber If dizziness causes falls or fainting, if tiredness is severe enough to interfere with daily life, or if cold extremities become painful or change colour (white, blue, then red — Raynaud-like).

Breathing Symptoms — Particularly Important

Tell patient Propranolol is NOT recommended if you have asthma, even if it has been quiet for years. If you have any history of wheezing, breathlessness, or use of a rescue inhaler, tell your prescriber. Mild shortness of breath with exertion is common at first.

Call prescriber Immediately if wheezing develops, if you feel chest tightness, or if you become short of breath at rest. New rapid weight gain (more than 1–2 kg over 2–3 days) or leg swelling may signal worsening heart failure and needs prompt assessment.

Slow Heart Rate

Tell patient The medicine is meant to slow the heart somewhat — a resting rate in the 50s or 60s is usually expected. Mild slowing is part of how the drug works and is rarely concerning by itself.

Call prescriber If your heart rate drops below 50 beats per minute and you feel tired, light-headed, short of breath, or near-fainting; if you check your pulse and it feels irregular at rest. For Hemangeol-treated infants: contact the prescriber for fatigue, pallor, slow or uneven heartbeat, cold limbs, or fainting.

Mood, Sleep, and Sexual Function

Tell patient Propranolol can cause vivid dreams, nightmares, sleep disturbance, low mood, or trouble concentrating — more often than newer beta-blockers because it crosses into the brain. Some men notice changes in erectile function. These effects often improve with time or with a switch to a different beta-blocker.

Call prescriber If mood changes are persistent, if sleep disturbance is significant, or if sexual side effects are bothering you. These are real reasons to discuss alternatives — they are not something to suffer with quietly.

Diabetes — Watch for Hypoglycaemia

Tell patient If you take insulin or sulfonylureas, propranolol may hide some of the warning signs of low blood sugar — particularly the rapid heartbeat and tremor. Sweating is usually still present. Propranolol also makes hypoglycaemic episodes harder to recover from. Check your blood glucose more often. Cardioselective beta-blockers may be safer; ask your prescriber.

Call prescriber If you have unexplained low blood-sugar episodes, severe hypoglycaemia, or any concern about your hypoglycaemia awareness.

Severe Allergic Reactions Need Special Care

Tell patient If you have ever had a serious allergic reaction (anaphylaxis) — to bee stings, foods, latex, or medications — tell every healthcare provider that you take propranolol. The standard adrenaline (EpiPen) treatment may not work as well, and additional medicines may be needed. Always carry your EpiPen if prescribed and seek emergency care for any severe allergic reaction.

Call prescriber Before any allergy testing or new medication that has caused you an allergic reaction in the past.

Never Stop Suddenly

Tell patient Stopping propranolol abruptly — including missing several doses or running out — can be dangerous. It can cause your heart to suddenly speed up, raise your blood pressure, and trigger chest pain or even a heart attack in patients with coronary disease. In thyroid disease it may trigger a thyroid storm. Always plan refills ahead and never run out.

Call prescriber Before stopping the medication for any reason — including planned surgery, financial concerns, or side-effect worries. There is almost always a safer way to taper than abrupt cessation.

Infantile Haemangioma — Hemangeol-Specific Counselling for Caregivers

Tell carer Always give Hemangeol with a feed or right after a feed. If your baby is not eating well, has a cold or stomach bug, or is vomiting, skip the dose — do not give a double dose later. Use only the syringe that came in the box. Watch for signs of low blood sugar (very sleepy or floppy infant, poor feeding, sweating, jitteriness), slow heartbeat (pale, cool, sluggish baby), and breathing problems (wheezing, chest tightness, fast or laboured breathing).

Call prescriber / Emergency Immediately if your baby has any of the warning signs above; if your baby develops a chest infection with wheezing or breathing difficulty (treatment may need to be paused); or if your baby has pale skin, cold limbs, slow or uneven heartbeats, or unusual sleepiness/fainting. Take any unused medicine to the pharmacy 2 months after first opening — it must not be used after that.

Other Medicines and Pregnancy

Tell patient Several common medicines can change how propranolol works — particularly some antidepressants (paroxetine, fluoxetine, bupropion), some heart-rhythm drugs (verapamil, diltiazem, quinidine), cimetidine (a heartburn medicine), some antibiotics (ciprofloxacin), and rifampicin (a TB drug). Always tell your prescriber and pharmacist about every medicine you take, including over-the-counter products, vitamins, and herbal supplements. Heavy alcohol use and smoking also affect propranolol levels.

Call prescriber If you become pregnant or are planning pregnancy — propranolol crosses the placenta and may affect the baby’s growth or cause low heart rate and low blood sugar at birth. If you start any new prescription, OTC product, or herbal supplement and want to confirm compatibility.

Ref

Sources

Regulatory (PI / SmPC)

U.S. Food and Drug Administration. Inderal (propranolol hydrochloride) tablets prescribing information. Akrimax Pharmaceuticals. FDA label PDF Primary source for immediate-release propranolol indications, dosing, contraindications, and adverse-event reporting across all approved adult indications including hypertension, angina, MI, arrhythmias, migraine, essential tremor, HOCM, and pheochromocytoma.
U.S. Food and Drug Administration. Inderal LA (propranolol hydrochloride) long-acting capsules prescribing information. FDA label PDF Primary source for once-daily long-acting propranolol dosing in hypertension, angina, and migraine prophylaxis.
U.S. Food and Drug Administration. Inderal XL (propranolol hydrochloride) extended-release capsules prescribing information. ANI Pharmaceuticals. DailyMed entry Source for the extended-release bedtime-dosing formulation; defines the upper dose ceiling of 120 mg/day for hypertension and the 80–120 mg dose strengths.
U.S. Food and Drug Administration. InnoPran XL (propranolol hydrochloride) extended-release capsules prescribing information. FDA label PDF Source for adverse-event Table 1 (≥3% reporting threshold) and bedtime extended-release pharmacokinetics (Tmax 12–14 hours, half-life ~8 hours).
U.S. Food and Drug Administration. Hemangeol (propranolol hydrochloride) oral solution prescribing information. Pierre Fabre. FDA label PDF Sole FDA-approved propranolol formulation for proliferating infantile haemangioma; defines age range (5 weeks to 5 months at initiation), weight-based dose escalation, and structured 2-hour monitoring requirements.

Key Clinical Trials

Léauté-Labrèze C, Hoeger P, Mazereeuw-Hautier J, et al. A randomized, controlled trial of oral propranolol in infantile hemangioma. N Engl J Med. 2015;372(8):735-746. DOI: 10.1056/NEJMoa1404710 Pivotal randomised controlled trial supporting Hemangeol approval — 460 infants with proliferating infantile haemangioma compared four propranolol regimens with placebo; the 3.4 mg/kg/day for 6 months regimen achieved 60% complete or near-complete resolution at week 24 versus 4% on placebo.
Léauté-Labrèze C, Dumas de la Roque E, Hubiche T, Boralevi F, Thambo JB, Taïeb A. Propranolol for severe hemangiomas of infancy. N Engl J Med. 2008;358(24):2649-2651. DOI: 10.1056/NEJMc0708819 Original case-series observation that launched propranolol use in infantile haemangioma — the serendipitous discovery that propranolol given for cardiomyopathy caused dramatic regression of a coexisting facial haemangioma.
β-Blocker Heart Attack Trial Research Group. A randomized trial of propranolol in patients with acute myocardial infarction: I. Mortality results. JAMA. 1982;247(12):1707-1714. DOI: 10.1001/jama.1982.03320370021023 BHAT trial — pivotal study supporting propranolol’s post-MI mortality reduction indication; demonstrated 26% reduction in total mortality over 25 months of follow-up.

Guidelines

Silberstein SD, Holland S, Freitag F, et al. Evidence-based guideline update: pharmacologic treatment for episodic migraine prevention in adults. Neurology. 2012;78(17):1337-1345. DOI: 10.1212/WNL.0b013e3182535d20 AAN/American Headache Society guideline classifying propranolol, metoprolol, and timolol as Level A (established as effective) for migraine prophylaxis.
Krowchuk DP, Frieden IJ, Mancini AJ, et al. Clinical practice guideline for the management of infantile hemangiomas. Pediatrics. 2019;143(1):e20183475. DOI: 10.1542/peds.2018-3475 American Academy of Pediatrics guideline establishing oral propranolol as first-line therapy for problematic infantile haemangiomas requiring systemic treatment.
Whelton PK, Carey RM, Aronow WS, et al. 2017 ACC/AHA/AAPA/ABC/ACPM/AGS/APhA/ASH/ASPC/NMA/PCNA guideline for the prevention, detection, evaluation, and management of high blood pressure in adults. J Am Coll Cardiol. 2018;71(19):e127-e248. DOI: 10.1016/j.jacc.2017.11.006 Beta-blockers including propranolol are not first-line for uncomplicated hypertension but are appropriate when there is a compelling indication.
Garcia-Tsao G, Abraldes JG, Berzigotti A, Bosch J. Portal hypertensive bleeding in cirrhosis: risk stratification, diagnosis, and management — 2016 practice guidance by the American Association for the Study of Liver Diseases. Hepatology. 2017;65(1):310-335. DOI: 10.1002/hep.28906 AASLD guidance defining the role of non-selective beta-blockers (propranolol, nadolol, carvedilol) in primary and secondary prophylaxis of variceal bleeding.
Ross DS, Burch HB, Cooper DS, et al. 2016 American Thyroid Association guidelines for diagnosis and management of hyperthyroidism and other causes of thyrotoxicosis. Thyroid. 2016;26(10):1343-1421. DOI: 10.1089/thy.2016.0229 ATA guidelines defining propranolol’s role in symptomatic management of hyperthyroidism and thyroid storm, including its weak inhibitory effect on peripheral T4-to-T3 conversion.

Mechanistic / Basic Science

Black JW, Crowther AF, Shanks RG, Smith LH, Dornhorst AC. A new adrenergic betareceptor antagonist. Lancet. 1964;1(7342):1080-1081. DOI: 10.1016/S0140-6736(64)91275-9 The original 1964 Lancet description of propranolol by Sir James Black and colleagues — the foundational publication that earned Black the 1988 Nobel Prize in Physiology or Medicine.
Storch CH, Hoeger PH. Propranolol for infantile haemangiomas: insights into the molecular mechanisms of action. Br J Dermatol. 2010;163(2):269-274. DOI: 10.1111/j.1365-2133.2010.09848.x Reviews proposed mechanisms of propranolol’s effect on infantile haemangiomas — vasoconstriction, downregulation of VEGF and bFGF, and induction of capillary endothelial apoptosis.

Pharmacokinetics / Special Populations

Drolet BA, Frommelt PC, Chamlin SL, et al. Initiation and use of propranolol for infantile hemangioma: report of a consensus conference. Pediatrics. 2013;131(1):128-140. DOI: 10.1542/peds.2012-1691 Multidisciplinary consensus on practical aspects of propranolol initiation in infantile haemangioma — pretreatment evaluation, dosing, monitoring, and management of intercurrent illness — that informed the Hemangeol prescribing information.
Stoschitzky K, Sakotnik A, Lercher P, et al. Influence of beta-blockers on melatonin release. Eur J Clin Pharmacol. 1999;55(2):111-115. DOI: 10.1007/s002280050604 Mechanistic study explaining the well-recognised sleep disturbance with lipophilic beta-blockers including propranolol — beta-blockade suppresses pineal melatonin secretion.