Labetalol: Comprehensive Drug Monograph

Pharmacokinetic Profile

Half-Life

~6–8 hours after oral administration; ~5.5 hours after IV infusion. Steady state by ~third day of dosing

Metabolism

Mainly hepatic glucuronide conjugation; not a major CYP substrate — fewer CYP-mediated drug interactions than most beta-blockers

Bioavailability

~25% (extensive first-pass); increased when administered with food

α : β Blockade Ratio

Approximately 1:3 oral; 1:7 intravenous per the FDA PI

Protein Binding

Approximately 50%

Excretion

~55–60% in urine as conjugates or unchanged within first 24 hours; biliary excretion to faeces. Not significantly removed by haemodialysis or peritoneal dialysis (<1%)

Clinical Information

Drug Class

Combined selective α1- and non-selective β-adrenergic antagonist; molecular complex of two diastereoisomeric pairs (four stereoisomers); R,R’-stereoisomer (dilevalol) accounts for 25% of racemate per the FDA PI

Available Doses

Tablets: 100 mg, 200 mg, 300 mg · Injection: 5 mg/mL (supplied as 20-mL/100-mg and 40-mL/200-mg vials per Trandate Injection labelling)

Route

Oral twice daily (chronic); IV slow push or continuous infusion (acute settings)

Renal Adjustment

No formal adjustment — half-life unchanged in renal impairment per the FDA PI; not significantly dialysable

Hepatic Adjustment

Bioavailability increased due to reduced first-pass metabolism per the FDA PI; rare but serious hepatotoxicity reported — discontinue if signs of liver injury develop

Pregnancy

Per the 2024 FDA PI, no drug-associated risk of major birth defects identified from extensive published data. Crosses placenta — neonatal monitoring for hypotension, bradycardia, hypoglycaemia, and respiratory depression. Considered first-line by ACOG for chronic hypertension in pregnancy and for severe-range pregnancy hypertension

Lactation

Excreted in human milk at low levels (~0.004% of maternal dose per Trandate Tablets PI); generally compatible with breastfeeding

Schedule

Rx only; not controlled

Distinguishing Feature

The only widely used antihypertensive that combines alpha-1 and beta-blockade in one molecule with rapid onset, IV availability, and an established pregnancy safety profile

Indications

Labetalol occupies a distinctive niche in cardiovascular pharmacotherapy: it is the only widely used antihypertensive that combines α1-adrenergic blockade (vasodilation) with non-selective β-blockade (negative chronotropy, inotropy, and dromotropy) within a single molecule. The result is reliable blood-pressure reduction without reflex tachycardia — particularly useful in acute haemodynamic management, hypertensive emergencies, and pregnancy.

Indication	Population / Formulation	Therapy Type	Status
Hypertension — to lower blood pressure and reduce risk of fatal and non-fatal cardiovascular events	Adults; oral tablets (100, 200, 300 mg)	Monotherapy or combination, especially with thiazide and loop diuretics	FDA Approved (oral)
Severe hypertension — for control of blood pressure in severe hypertension in hospitalised patients per the Trandate Injection labelling	Adults; injection (5 mg/mL)	IV slow push or continuous infusion in monitored setting	FDA Approved (Trandate Injection)
Hypertension in pregnancy (chronic hypertension, gestational hypertension, pre-eclampsia)	Pregnant adults; oral and IV	First-line per ACOG; oral for chronic management, IV for acute severe-range BP	Off-Label (guideline first-line)
Hypertensive emergency in non-pregnant adults — rapid BP control in acute end-organ-threatening hypertension	Adults; IV in monitored setting	Among preferred first-line agents per ESC and major reviews	Off-Label (guideline-supported)
Pheochromocytoma — adjunctive blood-pressure and symptom control after adequate alpha-blockade	Adults	Adjunct to phenoxybenzamine or doxazosin; per the FDA PI, higher than usual doses may be required and paradoxical hypertensive responses have been reported	Off-Label (mentioned in Trandate Injection labelling)
Acute aortic dissection — initial blood-pressure and shear-stress control	Adults; IV in monitored setting	Preferred agent in many institutional protocols (alongside esmolol)	Off-Label (guideline-supported)
Hypertension in acute ischaemic stroke — when blood-pressure lowering is indicated (e.g., for thrombolysis eligibility)	Adults; IV	One of the recommended IV agents per AHA/ASA guidelines	Off-Label (guideline-supported)
Perioperative / intraoperative hypertension	Adults; IV	Acute control during anaesthesia and post-operative period	Off-Label (well-established practice)
Autonomic dysreflexia in spinal cord injury	Adults; IV or oral	Symptomatic adrenergic control	Off-Label
Cocaine- or methamphetamine-induced hypertension	Adults; IV	Selected as it provides both alpha- and beta-blockade in a single agent	Off-Label (institutional protocols vary)

The 2024 FDA-approved indication for oral labetalol is hypertension only. The Trandate Injection labelling supports use for control of blood pressure in severe hypertension. Other applications — including pregnancy hypertension, hypertensive emergency in non-pregnant adults, aortic dissection, and acute stroke — are off-label but extensively supported by major guideline organisations including ACOG, AHA/ASA, and the European Society of Cardiology.

Off-Label and Special-Population Uses

Pregnancy hypertension and pre-eclampsia — Per ACOG Practice Bulletin 203, labetalol is one of the preferred oral agents for chronic hypertension in pregnancy (alongside extended-release nifedipine; methyldopa and hydrochlorothiazide are secondary). Per ACOG Committee Opinion 767, IV labetalol is one of three first-line agents for acute-onset severe hypertension in pregnancy (alongside IV hydralazine and immediate-release oral nifedipine). The CHIPS trial (Magee 2015) and CHAP trial (Tita 2022) provided contemporary evidence on BP targets in pregnancy. Evidence quality: high.

Hypertensive emergency — IV labetalol is among the preferred agents for rapid BP reduction in most hypertensive emergencies and is particularly useful in acute aortic dissection because of its concurrent negative chronotropic and inotropic effects on aortic shear stress. Evidence quality: high (long-standing clinical practice).

Acute ischaemic stroke — Per AHA/ASA stroke guidelines, IV labetalol is one of the recommended agents for blood-pressure lowering when needed before thrombolysis (target <185/110 mmHg) or for severely elevated BP after stroke. Evidence quality: high (guideline-supported).

Dose

Dosing

Clinical Scenario	Starting Dose	Titration / Maintenance	Maximum Dose	Notes
Hypertension — adult, oral (FDA-approved)	100 mg PO twice daily alone or added to a diuretic regimen	Adjust in increments of 100 mg twice daily at 2–3-day intervals; usual maintenance 200–400 mg twice daily per the FDA PI	Per the FDA PI: severe hypertension may require 1,200–2,400 mg/day (titrate in increments not to exceed 200 mg twice daily)	Steady-state BP response within 24–72 hours of dosing Twice-daily dosing reflects pharmacokinetics
Hypertension — elderly, oral	100 mg PO twice daily	Many elderly patients require 100–200 mg twice daily per the FDA PI	Per response and tolerability	Elderly are more likely to experience orthostatic hypotension, dizziness, and lightheadedness
Severe hypertension — adult, IV bolus per Trandate Injection labelling	20 mg IV slow injection over 2 minutes (corresponds to 0.25 mg/kg for an 80-kg patient)	Additional injections of 40 or 80 mg at 10-minute intervals until target BP achieved	300 mg cumulative per the Trandate Injection labelling	Patient must remain supine during and for up to 3 hours after IV administration. Continuous BP monitoring; supine BP measured immediately before injection and at 5 and 10 minutes after Maximal effect of each dose typically within 5 minutes; BP rises gradually toward baseline within average 16–18 hours after IV discontinuation
Severe hypertension — adult, IV continuous infusion	Prepare 1 mg/mL solution by diluting 40 mL Trandate Injection in 160 mL IV fluid; infuse at 2 mL/min to deliver 2 mg/min	Adjust rate per BP response; effective IV dose usually 50–200 mg per the Trandate Injection labelling	300 mg cumulative per the Trandate Injection labelling; up to 3 g/day over 2–3 days has been anecdotally reported (with hypotension or bradycardia in some patients)	Steady-state blood levels not reached during typical infusion duration; controlled administration via burette or infusion pump preferred
Transition from IV to oral therapy	Per the Trandate Injection PI: begin oral dosing when supine diastolic BP has begun to rise. Initial oral dose 200 mg PO	Followed in 6–12 hours by an additional 200 or 400 mg PO, depending on BP response	Per inpatient titration table: 200 BID → 400 BID → 800 BID → 1,200 BID (max 2,400 mg/day, ± three divided doses)	Inpatient titration may proceed at 1-day intervals to achieve desired BP reduction
Acute severe hypertension in pregnancy — IV (off-label, ACOG-supported)	20 mg IV slow push over 2 minutes if BP remains ≥160/110 mmHg after 15 minutes	Repeat at 40 mg, then 80 mg, then 80 mg IV at 10–15-minute intervals until target BP achieved	220 mg cumulative per ACOG protocols; consider alternative agent if not controlled at this dose	Continuous fetal monitoring; transition to oral once stable. Avoid in patients with bradycardia or asthma IV hydralazine and oral immediate-release nifedipine are the alternatives per ACOG Committee Opinion 767
Chronic hypertension in pregnancy — adult, oral (off-label, ACOG first-line)	100 mg PO twice daily	Increase as needed; usual maintenance up to 2,400 mg/day divided	2,400 mg/day per the FDA oral PI	Alongside extended-release nifedipine, one of the preferred first-line oral agents for chronic HTN in pregnancy per ACOG Practice Bulletin 203. Monitor maternal BP, HR, LFTs and fetal growth
Acute aortic dissection — adult, IV (off-label, guideline-supported)	20 mg IV slow push followed by infusion typically 2 mg/min	Titrate to SBP 100–120 mmHg and HR <60 bpm	Per haemodynamic targets	Combined alpha- and beta-blockade ideal for shear-stress reduction. Esmolol is an alternative when shorter half-life is preferred
Hypertension in acute ischaemic stroke — IV (off-label, AHA/ASA-supported)	10–20 mg IV over 1–2 minutes	May repeat once after 10–20 minutes; continuous infusion can be used per institutional protocol	Per BP target	Goal BP <185/110 mmHg before thrombolysis; <180/105 mmHg during/after thrombolysis
Discontinuation	Reduce gradually; per the FDA PI, do not abruptly discontinue			Abrupt withdrawal may cause exacerbation of angina or, in some cases, MI in patients with coronary artery disease

Population-Specific Considerations

Population	Adjustment	Rationale
Renal impairment	No formal adjustment	Per the FDA PI, the elimination half-life of labetalol is not altered in renal impairment; not significantly removed by haemodialysis or peritoneal dialysis (<1%)
Hepatic impairment	Use with caution; consider lower starting dose	Per the FDA PI, half-life is not altered but bioavailability is increased due to decreased first-pass metabolism. Hepatocellular injury (rare but potentially fatal) warrants monitoring for symptoms
Elderly	Initiate at standard 100 mg BID; many require lower maintenance dosing	Per the FDA PI, elimination is reduced in elderly patients; orthostatic hypotension and dizziness more common
Paediatric	Safety and effectiveness not established	Per the FDA PI; off-label use exists in paediatric hypertensive emergency at 0.2–1 mg/kg IV bolus or continuous infusion per institutional protocol
Pregnancy	Used at standard adult dosing; preferred agent in many guideline-supported scenarios	Per the FDA PI, extensive published experience has not identified a drug-associated risk for major birth defects, miscarriage, or adverse maternal/fetal outcomes. Crosses placenta — neonates require monitoring at delivery
Lactation	Generally compatible	Per the Trandate Tablets PI, approximately 0.004% of the maternal dose is excreted in human milk

Clinical Pearl — Why Labetalol Is the Workhorse of Acute Severe Hypertension

The combination of α1-blockade (vasodilation, BP reduction) and non-selective β-blockade (negative chronotropy, attenuation of reflex tachycardia) gives labetalol four practical advantages: (1) predictable BP reduction without reflex tachycardia, (2) rapid onset (maximal effect within 5 minutes IV) suitable for hypertensive emergencies, (3) relatively short duration of action allowing easy titration, and (4) lack of significant CYP-mediated drug interactions (predominantly glucuronidated). The α:β ratio of approximately 1:7 with IV administration means labetalol behaves predominantly as a beta-blocker IV, with the alpha component contributing supplementary vasodilation — this is why it does not produce the dramatic BP drops sometimes seen with pure alpha-blockers.

Pharmacology

Mechanism of Action

Labetalol hydrochloride combines selective competitive α1-adrenergic blockade with non-selective competitive β-adrenergic blockade in a single molecule. Per the FDA PI, the α:β blockade ratio is approximately 1:3 after oral administration and 1:7 after intravenous administration. The α1-blockade attenuates the pressor response to phenylephrine and the cold-pressor test in humans, contributing peripheral vasodilation. β1-blockade decreases resting heart rate modestly, attenuates exercise-induced tachycardia, and blunts the reflex tachycardia produced by amyl nitrite-induced hypotension. β2-blockade is demonstrated by inhibition of isoproterenol-induced fall in diastolic blood pressure.

The net haemodynamic result is dose-related blood-pressure reduction without reflex tachycardia and without significant reduction in cardiac output, achieved through a balanced reduction of total peripheral resistance (from α1-blockade) and prevention of compensatory sympathetic responses (from β-blockade). Plasma renin activity is reduced. Because of α1-mediated postural vasodilation, blood pressure falls more in the standing than the supine position — the basis for the FDA-required supine positioning during and for 3 hours after IV administration.

Per the FDA PI, labetalol exists as a molecular complex of two diastereoisomeric pairs (four stereoisomers total). The R,R’-stereoisomer (dilevalol) accounts for 25% of racemic labetalol. Of historical relevance, dilevalol was developed as a separate single-isomer product but was withdrawn after reports of severe hepatic injury — a signal that informs labetalol’s hepatic safety surveillance, since dilevalol is one of the four isomers contained within labetalol.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Rapidly absorbed orally; peak plasma levels 1–2 hours after oral administration. Absolute bioavailability ~25% (extensive first-pass hepatic metabolism). Peak effect of single oral dose at 2–4 hours; duration ≥8 hours after 100 mg, >12 hours after 300 mg per the FDA PI. Bioavailability is increased by food	Twice-daily oral dosing; meals enhance absorption modestly. IV onset rapid (maximal effect within 5 minutes per the Trandate Injection PI)
Distribution	Approximately 50% protein-bound (lower than most beta-blockers). Crosses the placenta. Per the Trandate Injection PI, only negligible amounts of the drug crossed the blood-brain barrier in animal studies. Excreted in human milk at low levels (~0.004% of maternal dose per the Trandate Tablets PI)	Lower protein binding than propranolol or carvedilol; modest CNS penetration (less lipophilic than propranolol — fewer CNS adverse effects)
Metabolism	Mainly hepatic, predominantly via glucuronide conjugation (Phase II metabolism). Per the FDA PI, labetalol is not a major substrate of cytochrome P450 enzymes	Few clinically significant CYP-mediated drug interactions — a significant advantage over propranolol and metoprolol. The principal pharmacokinetic interaction noted in the PI is with cimetidine, which increases bioavailability
Elimination	Plasma half-life ~6–8 hours after oral administration; ~5.5 hours after IV infusion per the Trandate Injection PI. Steady state by ~third day of dosing. Approximately 55–60% excreted in urine as conjugates or unchanged labetalol within first 24 hours; biliary excretion to faeces accounts for the remainder. Not significantly removed by haemodialysis or peritoneal dialysis (<1%)	No renal-dose adjustment needed per the FDA PI. Dialysis does not enhance clearance in overdose

Pharmacodynamic Note — Combined α/β Blockade

Labetalol’s pharmacological profile sits between the pure beta-blockers (atenolol, metoprolol, propranolol) and the alpha/beta-blocker carvedilol. Compared with carvedilol, labetalol’s alpha component is more pronounced relative to its beta component, especially intravenously, and labetalol has IV availability — making it the drug of choice in acute settings where carvedilol’s chronic-only oral form is unsuitable. Compared with pure beta-blockers, labetalol is less likely to cause cold extremities (because alpha-blockade promotes peripheral vasodilation), less likely to provoke reflex tachycardia after vasodilator co-administration, and is preferred over propranolol in pregnancy. However, labetalol shares the bronchospasm risk of all non-selective beta-blockers and the orthostatic hypotension risk of alpha-blockers, particularly with the first dose or after IV administration.

Side Effects

Labetalol’s adverse effects reflect both alpha-1 antagonism (orthostatic hypotension, nasal stuffiness, intraoperative floppy iris syndrome) and non-selective beta-blockade (bradycardia, bronchospasm, hypoglycaemia masking). Per the FDA PI, in controlled clinical trials of 3 to 4 months’ duration, discontinuation of labetalol due to one or more adverse effects was required in 7% of all patients. Most adverse effects are mild and transient, occurring early in the course of treatment.

≥2% (Placebo-Controlled Trials) Adverse Reactions Occurring in ≥2% of Patients and More Frequent on Labetalol than Placebo (FDA PI Table 1)

Adverse Effect	Labetalol (n = 227)	Placebo (n = 98)	Clinical Note
Dizziness	11%	3%	Most common adverse effect; frequently orthostatic — counsel patients to rise slowly
Nausea	6%	1%	Usually mild and self-limited
Fatigue	5%	0%	Often improves over the first 2–4 weeks
Nasal stuffiness	3%	0%	Reflects α1-blockade in nasal mucosa — distinctive of α-blocker–containing antihypertensives
Dyspepsia	3%	1%	Take with food if bothersome
Headache	2%	1%	Often improves with continued therapy
Dyspnoea	2%	0%	May reflect early beta-blocker effect or unmasking of subclinical bronchospasm — assess history of reactive airways disease
Vertigo	2%	1%	Often related to orthostatic effect; transient

Dose-Related Dose-Stratified Incidence (Trandate Injection PI Oral Therapeutic Trials Database)

Adverse Effect	Daily Dose 200 mg	Daily Dose 800 mg	Daily Dose 2,400 mg
Dizziness	2%	5%	16%
Fatigue	2%	5%	10%
Nausea	<1%	4%	19%
Vomiting	0%	<1%	3%
Dyspepsia	1%	1%	4%
Paresthesia	2%	1%	5%
Nasal stuffiness	1%	2%	6%
Ejaculation failure	0%	3%	5%
Impotence	1%	2%	3%
Oedema	1%	1%	2%

IV Administration Adverse Reactions Reported with Trandate Injection (per 100 patients)

Adverse Effect	Reported Frequency	Clinical Note
Symptomatic postural hypotension (if tilted within 3 hours)	58%	Per the Trandate Injection PI; the basis for the supine-positioning requirement
Nausea	13 per 100	Often mild
Dizziness	9 per 100	Particularly during BP nadir
Transient elevation in BUN / creatinine	8 per 100	Per the Trandate Injection PI, generally associated with drops in blood pressure in patients with prior renal insufficiency
Tingling of scalp / skin	7 per 100	Distinctive to labetalol; transient and usually resolves with continued therapy
Sweating	4 per 100	Usually transient
Vomiting	4 per 100	Mild and self-limiting
Somnolence / yawning	3 per 100	Reflects post-administration BP reduction
Moderate hypotension (supine)	1 per 100	Manage with supine positioning, leg elevation, IV fluids
Ventricular arrhythmia, hypoaesthesia, vertigo, flushing, wheezing, pruritus	1 per 100 each	Per the Trandate Injection PI; uncommon but reported

Laboratory / Other Laboratory Findings and Other Reactions

Adverse Effect	Reported Frequency	Clinical Note
Reversible elevation in serum transaminases (oral)	~4% of patients tested per the Trandate Injection PI (referencing oral data)	Mostly mild and reversible; severe hepatocellular injury is rare but a recognised serious adverse reaction
Tremor (with concomitant TCA)	2.3% with TCA vs 0.7% with labetalol alone per the FDA PI	Distinctive interaction; dose adjustment of either agent may be needed
Postural / orthostatic hypotension (oral)	~2% in oral trials; more common with first dose and large dose increases	Most likely 2–4 hours after a dose, especially with large initial doses or large changes in dose per the FDA PI

Serious Serious / Rare but Important

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Severe hepatocellular injury (hepatic necrosis, hepatitis, cholestatic jaundice)	Rare per the FDA PI; usually reversible but hepatic necrosis and death have been reported. Confirmed by rechallenge in at least one case per the Trandate Injection PI	After short- or long-term treatment; may be slowly progressive despite minimal symptoms	Discontinue labetalol if signs/symptoms of liver injury develop. Investigate cause; per the FDA PI, do not restart unless another explanation found
Severe orthostatic hypotension / syncope	More likely with first dose and after large dose increases per the FDA PI	2–4 hours after dose	Patient supine; legs elevated; IV fluids if severe. After IV labetalol, patient must remain supine during and for up to 3 hours after administration
Bradycardia, sinus pause, heart block, cardiac arrest	Rare; risk increased with concomitant non-DHP CCB or digitalis per the FDA PI	Hours to days	Hold drug; atropine; transcutaneous or transvenous pacing for high-degree AV block; IV glucagon for refractory beta-blocker toxicity
Bronchospasm	Bronchial asthma and obstructive airway disease are absolute contraindications per the FDA PI	Within hours	Avoid in reactive airways disease; inhaled β2-agonist (high doses may be required); systemic corticosteroids if severe
Heart failure precipitation / decompensation	Decompensated heart failure is an absolute contraindication; overt CHF is also contraindicated per the FDA PI	Days to weeks	Discontinue if signs/symptoms of HF develop; treat appropriately. Labetalol is NOT FDA-approved for chronic heart failure (carvedilol is the alpha/beta-blocker for HF)
Severe / prolonged hypoglycaemia	Risk increased especially in patients with diabetes mellitus, children, and fasting patients per the FDA PI	During hypoglycaemic episodes	Beta-blockers may mask early warning signs (tachycardia); counsel diabetics. Increase glucose monitoring frequency
Paradoxical hypertensive response in pheochromocytoma	Reported in a few patients per the FDA PI	During treatment	Higher than usual doses may be needed for pheochromocytoma; monitor BP closely; alpha-blockade should be established first
Anaphylactic / anaphylactoid reactions with relative resistance to adrenaline	Per the FDA PI; reported in patients on beta-blockers	Variable	Avoid labetalol in patients at high risk of anaphylaxis per the FDA PI. Higher-dose adrenaline, IV glucagon, IV fluids, antihistamines, corticosteroids
Intraoperative floppy iris syndrome (IFIS) during cataract surgery	Per the FDA PI; observed in patients treated with α1-blockers (labetalol is alpha/beta)	Intraoperative	Inform the patient’s ophthalmologist preoperatively. Surgical modifications (iris hooks, dilator rings, viscoelastics) may be needed. Per the Trandate Injection PI, no benefit demonstrated for stopping alpha-1 blocker therapy prior to cataract surgery
Severe hypotension during halothane anaesthesia	Synergism between IV labetalol and halothane per the FDA PI	Intraoperative	Avoid high-concentration halothane (≥3%) with IV labetalol; communicate with anaesthesia team about beta-blocker therapy
Acute exacerbation of angina or MI on abrupt withdrawal	Class effect per the FDA PI	Days after stopping	Do not abruptly discontinue; taper gradually. If angina worsens, promptly reinstitute and manage as unstable angina
Cutaneous reactions including rash, urticaria, pruritus, angioedema	Rare per the Trandate Injection PI; hypersensitivity reactions reported	Variable	Discontinue; treat as for hypersensitivity

Discontinuation Discontinuation Patterns

Discontinuation Rate (per FDA PI)

Per the FDA PI: in controlled trials of 3–4 months’ duration, 7% of patients discontinued labetalol due to one or more adverse effects.

Top Reasons for Discontinuation

Tolerability

Dizziness, fatigue, nausea, orthostatic symptoms, sexual dysfunction. Most discontinuations occur early in treatment.

Management — Beta-Blocker Toxicity

Per the FDA PI, overdosage with labetalol causes excessive hypotension that is posture-sensitive and sometimes excessive bradycardia. Critical management points: (1) Place patient supine and elevate legs to improve cerebral perfusion. (2) Excessive bradycardia: atropine or epinephrine; cardiac failure: digitalis glycoside and diuretic, with dopamine or dobutamine if needed. (3) Hypotension: vasopressors (norepinephrine may be the drug of choice per the Trandate Injection PI). (4) Bronchospasm: epinephrine and/or aerosolised β2-agonist. (5) Per the Trandate Injection PI, in severe beta-blocker overdose with hypotension and/or bradycardia, glucagon has been shown to be effective when administered as 5–10 mg rapidly over 30 seconds, followed by continuous infusion of 5 mg/h that can be reduced as the patient improves. (6) Seizures: diazepam. (7) Per the FDA PI, neither haemodialysis nor peritoneal dialysis removes a significant amount of labetalol (<1%).

Int

Drug Interactions

Labetalol’s interaction profile is notably narrower than that of CYP-metabolised beta-blockers (propranolol, metoprolol, carvedilol) because labetalol is primarily eliminated by glucuronide conjugation, not by CYP enzymes. The clinically important interactions are pharmacodynamic (additive haemodynamic effects with other negative chronotropes, bronchodilator antagonism, halothane synergism, anaesthetic interactions) rather than pharmacokinetic. The 2024 FDA oral PI also flags a notable diagnostic-laboratory interaction relevant to pheochromocytoma evaluation.

Major (Contraindicated) Non-DHP calcium-channel antagonists (verapamil, diltiazem)

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

EffectSevere bradycardia, AV block, hypotension, cardiogenic shock

ManagementPer the 2024 FDA oral PI, coadministration of labetalol with non-DHP CCBs is contraindicated. Use a dihydropyridine CCB (amlodipine, nifedipine) if combined antihypertensive therapy is needed

FDA PI

Major Halothane anaesthesia

MechanismPer the FDA PI, synergism has been shown between halothane anaesthesia and IV labetalol

EffectProfound hypotension and reduction in cardiac output; increased central venous pressure

ManagementPer the FDA PI, do not use halothane concentrations of 3% or above with IV labetalol. Communicate beta-blocker therapy to anaesthesia team

FDA PI

Major Adrenaline (epinephrine) — for anaphylaxis

MechanismBeta-blockade may blunt response to adrenaline; alpha-blockade by labetalol partially mitigates the unopposed-alpha vasoconstriction concern seen with pure beta-blockers

EffectPer the FDA PI, patients on beta-blockers may be unresponsive to usual doses of epinephrine for anaphylaxis

ManagementPer the FDA PI, avoid labetalol in patients at high risk of anaphylactic reactions. If adrenaline is needed, higher doses may be required; have IV glucagon available

FDA PI

Moderate Negative chronotropes (digitalis glycosides)

MechanismAdditive AV nodal slowing

EffectIncreased risk of bradycardia and high-degree AV block per the FDA PI

ManagementMonitor heart rate and rhythm; ECG before initiation if conduction concerns

FDA PI

Moderate Bronchodilators (β2-agonists)

MechanismPer the FDA PI, labetalol antagonises the bronchodilator effect of beta-receptor agonists

EffectReduced efficacy of beta-agonist bronchodilators; doses greater than the normal anti-asthmatic dose may be required

ManagementLabetalol is contraindicated in bronchial asthma. In other patients with reactive airways disease, use lowest effective labetalol dose; β2-agonist may need uptitration

FDA PI

Moderate Nitroglycerin and other nitrates

MechanismAdditive blood-pressure lowering; labetalol blunts the reflex tachycardia produced by nitroglycerin

EffectExcessive hypotension per the FDA PI

ManagementPer the FDA PI, monitor BP and adjust labetalol dose as needed; avoid initiating labetalol in patients on nitroglycerin

FDA PI

Moderate Cimetidine

MechanismPer the FDA PI, cimetidine increases the bioavailability of labetalol — possibly via enhanced absorption or altered hepatic metabolism

EffectIncreased labetalol exposure and risk of hypotension/bradycardia

ManagementSubstitute famotidine or a PPI; monitor BP and HR if combination cannot be avoided

FDA PI

Moderate Tricyclic antidepressants (TCAs)

MechanismMechanism uncertain; possible additive central effect

EffectPer the FDA PI, 2.3% of patients on labetalol + TCA experienced tremor compared with 0.7% on labetalol alone

ManagementCounsel patients about possible tremor; consider alternative antidepressant (SSRI) where clinically appropriate

FDA PI

Moderate Insulin and oral hypoglycaemics

MechanismPer the Trandate Injection PI, beta-blockade may prevent appearance of premonitory signs of acute hypoglycaemia (e.g., tachycardia) and may reduce insulin release in response to hyperglycaemia

EffectPer the 2024 FDA oral PI, increased risk for severe or prolonged hypoglycaemia at any time during treatment, especially in diabetics, children, and fasting patients

ManagementIncrease glucose monitoring; consider cardioselective beta-blocker if a labetalol-specific indication is not present

FDA PI

Moderate Iodinated contrast media

MechanismBeta-blockade lowers threshold for and increases severity of contrast hypersensitivity reactions; reduces responsiveness to adrenaline used to treat them

EffectIncreased risk of severe contrast reactions

ManagementCommunicate beta-blocker therapy to radiology team; have IV glucagon available for treatment of refractory anaphylactoid reactions

Class effect

Moderate Iobenguane (MIBG) imaging

MechanismLabetalol (and other agents that decrease neuronal uptake of norepinephrine) interfere with iobenguane uptake

EffectRisk of false-negative MIBG scans (used in pheochromocytoma/paraganglioma evaluation)

ManagementDiscontinue labetalol for at least 5 half-lives (approximately 2 days) before MIBG scintigraphy if clinically appropriate

Iobenguane FDA labelling

Minor (Diagnostic) Urinary catecholamine and amphetamine assays

MechanismPer the FDA PI, labetalol metabolites in urine cause falsely elevated levels of urinary catecholamines, metanephrine, normetanephrine, and VMA when measured by fluorimetric or photometric methods. Labetalol can also cause false-positive amphetamine screens (e.g., Toxi-Lab A and EMIT-d.a.u. assays per the Trandate Injection PI)

EffectMisleading laboratory results during pheochromocytoma evaluation or drug screening

ManagementUse HPLC with solid-phase extraction for urinary catecholamines per the FDA PI; confirm positive amphetamine screens by gas chromatography mass spectrometry

FDA PI

Practical Take-Home — Three Interactions That Matter Most

(1) Non-DHP CCB combination is contraindicated per the 2024 FDA oral PI — a uniquely strong restriction for labetalol (most beta-blockers carry only a “use caution” warning for this combination). Use amlodipine instead. (2) Halothane anaesthesia synergism — communicate labetalol therapy to the anaesthesia team; high-concentration halothane (≥3%) is contraindicated. (3) Falsely elevated urinary catecholamines — important to remember when evaluating possible pheochromocytoma in a patient already taking labetalol; insist on HPLC-based assay or hold labetalol and use plasma-free metanephrines.

Mon

Monitoring

Blood Pressure (Supine and Standing) Baseline, at each titration step, then routinely
Routine Per the FDA PI, monitor for symptomatic postural hypotension and syncope after initial dosing or dose increments. Symptomatic postural hypotension is most likely 2–4 hours after a dose. For IV labetalol, supine BP measured immediately before injection and at 5 and 10 minutes after; supine positioning during and for up to 3 hours after IV administration.
Heart Rate Baseline, at each titration step, then routinely
Routine Per the FDA PI, monitor heart rate and rhythm in patients receiving labetalol. Bradycardia, sinus pause, heart block, severe bradycardia, and cardiac arrest have occurred with beta-blockers.
Liver Function Tests (LFTs) If symptoms develop; baseline reasonable; periodic determination considered appropriate per the Trandate Injection PI
Trigger-based Per the FDA PI, severe hepatocellular injury occurs rarely with labetalol therapy. Hepatic injury is usually reversible, but hepatic necrosis and death have been reported. Investigate the probable cause of any signs/symptoms of liver injury (pruritus, dark urine, persistent anorexia, jaundice, right-upper-quadrant tenderness, unexplained “flu-like” symptoms). Do not restart labetalol without another explanation.
ECG Baseline if conduction concerns; for symptomatic bradycardia
Trigger-based Particularly important in patients with pre-existing first-degree AV block (a relative contraindication unless paced) or sinus node dysfunction.
Respiratory Symptoms At each visit; particularly if any history of reactive airways disease
Routine Bronchial asthma is an absolute contraindication. New wheezing or dyspnoea warrants urgent reassessment; per the FDA PI, avoid labetalol in patients with reactive airways disease.
Glycaemic Status (in diabetics) Routine in diabetics
Routine Per the FDA PI, beta-blockers may prevent early warning signs of hypoglycaemia (tachycardia) and increase risk for severe or prolonged hypoglycaemia, especially in diabetics, children, and fasting patients.
Maternal/Fetal Surveillance (in Pregnancy) Per obstetric protocol
Routine Routine BP, HR, and LFT monitoring; serial fetal growth assessment given association of maternal hypertension with intrauterine growth restriction. At delivery, neonatal monitoring for hypotension, bradycardia, hypoglycaemia, and respiratory depression per the FDA PI.
Pre-Cataract Surgery Communication Before any planned cataract surgery
Trigger-based Per the FDA PI, intraoperative floppy iris syndrome has been observed during cataract surgery in patients treated with α1-blockers. Inform the patient’s ophthalmologist preoperatively. Per the Trandate Injection PI, no benefit demonstrated for stopping alpha-1 blocker therapy prior to cataract surgery.
Pre-Surgery Communication Before any planned surgery
Trigger-based Per the FDA PI, do not routinely withdraw chronic beta-blocker therapy prior to surgery. The effect of labetalol’s alpha-adrenergic activity has not been fully evaluated in this setting. Communicate beta-blocker use and recent dose to anaesthetist; halothane synergism may warrant alternative anaesthetic agent.
Adherence and Withdrawal Risk At each follow-up
Routine Per the FDA PI, abrupt cessation of therapy with beta-blockers in patients with coronary artery disease can cause exacerbations of angina pectoris and, in some cases, MI. Counsel patients to refill in advance and never run out.

The Vitals That Matter Most

For routine outpatient labetalol monitoring, BP (both supine and standing) and HR are the primary parameters at every visit. For inpatient IV use, continuous BP and HR monitoring with supine positioning during and for 3 hours after administration is mandatory per the FDA PI. LFTs are not strictly required but should be checked at the first sign of symptoms suggesting liver injury — labetalol’s hepatotoxicity is rare but recognised and potentially serious. Per the Trandate Injection PI, periodic LFT determination is considered appropriate for chronic therapy.

Contraindications & Cautions

Absolute Contraindications (per the 2024 FDA Labetalol Tablets PI)

Bronchial asthma or obstructive airway disease — non-selective β-blockade can provoke severe bronchospasm
Decompensated heart failure — beta-blockade may further depress myocardial contractility and precipitate more severe failure
Greater than first-degree heart block
Cardiogenic shock
Severe bradycardia
Hypersensitivity reactions, including anaphylaxis, to labetalol
Concomitant non-dihydropyridine calcium-channel antagonists (verapamil, diltiazem) — additive AV nodal slowing risk

Relative Contraindications (Specialist Input Recommended)

Reactive airways disease (non-asthmatic) — avoid use; if essential, use the smallest effective dose to minimise inhibition of endogenous or exogenous beta-agonists
Overt congestive heart failure — avoid use; if HF develops during therapy, discontinue
Active untreated pheochromocytoma — alpha-blockade should be established first; per the FDA PI, paradoxical hypertensive responses have been reported in a few patients
Severe hepatic impairment — bioavailability is increased; rare but potentially fatal hepatotoxicity
History of severe acute hypersensitivity reactions — beta-blocker may blunt response to adrenaline used for treatment; avoid in patients at high risk per the FDA PI
Impending iobenguane (MIBG) imaging — discontinue for at least 5 half-lives before scan
Following coronary artery bypass surgery with low cardiac index and elevated systemic vascular resistance — per the Trandate Injection PI, IV labetalol use should be avoided in this specific subset

Use with Caution

First-degree AV block, sinus node dysfunction — risk of progression with beta-blockade
Diabetes mellitus, especially insulin-treated — masking of hypoglycaemic warning signs; per the FDA PI, increased risk of severe/prolonged hypoglycaemia, especially in fasting patients
Major surgery — per the FDA PI, do not routinely withdraw chronic beta-blocker therapy prior to surgery; the effect of labetalol’s alpha-adrenergic activity has not been fully evaluated in this setting. Per the Trandate Injection PI, several deaths have occurred when Trandate Injection was used during surgery
Coronary artery disease — do not abruptly discontinue (rebound angina, MI risk)
Active hepatobiliary disease — increased exposure due to reduced first-pass; monitor for symptoms of hepatotoxicity
Concurrent non-DHP CCB therapy — contraindicated per the FDA PI; if any beta-blocker is required with verapamil/diltiazem, choose a different agent
Concurrent halothane anaesthesia — avoid concentrations ≥3% with IV labetalol
Patients undergoing or scheduled for cataract surgery — IFIS risk; pre-operative ophthalmology communication

FDA Regulatory Note No Boxed Warning, but Several Key Cautions

Labetalol does not carry an FDA boxed warning. The FDA prescribing information emphasises several distinctive cautions: (1) Concomitant use with non-DHP calcium-channel blockers is contraindicated — a stronger restriction than for most beta-blockers. (2) Bronchial asthma and obstructive airway disease are absolute contraindications because of non-selective β-blockade. (3) Severe hepatocellular injury, although rare, may be fatal — the PI specifies that labetalol should not be restarted in patients without another explanation for observed liver injury. (4) Halothane synergism mandates that high-concentration halothane (≥3%) not be used with IV labetalol, and per the Trandate Injection PI, several deaths have occurred when the injection was used during surgery. (5) Intraoperative floppy iris syndrome (a known α1-blocker effect) requires preoperative communication with ophthalmologists planning cataract surgery. (6) Strict supine positioning is required during and for 3 hours after IV administration to prevent symptomatic orthostatic hypotension (incidence 58% if patients are tilted within this window).

Patient Counselling

Purpose of Therapy

Explain that labetalol is a blood-pressure medicine that works in two ways at once: it relaxes the blood vessels (the “alpha” part) and slows the heart slightly (the “beta” part). This combination gives smooth blood-pressure control without the racing heartbeat that can happen with vessel-relaxing medicines alone. It is widely used for everyday high blood pressure, in pregnancy, and in hospital settings to bring dangerously high blood pressure down quickly.

How to Take

Take labetalol exactly as prescribed, usually twice a day. Take it with food — meals actually help the medicine absorb better. Take it consistently, the same way each time. Do not crush, chew, or split the tablets unless your prescriber tells you to. Do not stop suddenly. If you stop labetalol abruptly, your blood pressure can rebound, your heart rate can speed up, and in people with heart disease, this can trigger chest pain or even a heart attack. If you need to stop the medicine, your prescriber will guide you through a gradual taper.

Dizziness Standing Up — The Main First-Dose Effect

Tell patient Dizziness, especially when standing up quickly, is the most common side effect of labetalol — about 1 in 9 patients in the original studies. It usually happens 2–4 hours after a dose and is most pronounced with the first dose or after a dose increase. Stand up slowly. Sit on the edge of the bed for a minute before standing in the morning. If you feel light-headed, sit or lie down with your legs raised.

Call prescriber If dizziness causes a fall, fainting, or near-fainting; if it does not improve over the first 1–2 weeks; if you become consistently light-headed even when sitting still.

Tiredness, Nausea, and Tingling

Tell patient Mild tiredness and queasiness are common in the first 2–4 weeks and usually improve. Taking the dose with food helps. Headache and stuffy nose can also occur — the stuffy nose comes from the alpha-blocking effect on small blood vessels in the nose. Some patients notice a transient tingling or “pins and needles” sensation on the scalp or skin when starting therapy — this is recognised in the labelling and usually fades.

Call prescriber If tiredness is severe enough to interfere with daily activities; if nausea persists past a few weeks; if tingling becomes painful or persistent.

Breathing Symptoms — Particularly Important

Tell patient Labetalol must NOT be used if you have asthma — it is specifically contraindicated. If you have any history of wheezing, breathlessness, or use of a rescue inhaler, tell your prescriber before starting. Mild shortness of breath with exertion can occur as the medicine slows your heart slightly; this often improves.

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

Liver Symptoms — Rare but Important

Tell patient Very rarely, labetalol can affect the liver. Watch for warning signs: yellowing of the skin or eyes (jaundice), dark or “tea-coloured” urine, persistent loss of appetite, pain in the upper right side of your abdomen, itching, or unexplained “flu-like” feeling.

Call prescriber Immediately if you notice any of these signs. Stop taking the medicine and contact your prescriber the same day.

Pregnancy and Breastfeeding

Tell patient Labetalol is one of the most commonly used and best-studied blood-pressure medicines in pregnancy. Major medical bodies including the American College of Obstetricians and Gynecologists recommend it as a preferred agent. It can be used during breastfeeding — only tiny amounts (around 0.004% of your dose) reach breast milk.

Call prescriber If you are pregnant, planning to become pregnant, or breastfeeding. Your dose may need adjustment; your baby will be monitored at delivery for low heart rate, low blood pressure, low blood sugar, and breathing changes.

Diabetes — Watch for Hidden Hypoglycaemia

Tell patient If you have diabetes — particularly if you take insulin or sulfonylureas — labetalol may hide the early warning signs of low blood sugar (the racing heartbeat). You may go more quickly to feeling sweaty, weak, or confused. Check your blood sugar more often, especially in the early weeks of treatment.

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

Eye Surgery and Anaesthesia Awareness

Tell patient If you are scheduled for cataract surgery, tell your eye surgeon you are taking labetalol — it can occasionally make the iris of the eye more “floppy” during surgery, and the surgeon will adjust their technique. If you need any operation under anaesthesia, tell the anaesthesia team about your labetalol — there are some specific anaesthetic gases (halothane in particular) that need to be used carefully alongside it.

Call prescriber Before any planned surgery — usually labetalol should be continued through surgery rather than stopped, but the team should know.

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 labetalol. 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, contrast-imaging study, or new medication that has caused you an allergic reaction in the past.

Never Stop Suddenly

Tell patient Stopping labetalol abruptly — including missing several doses or running out — 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. 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.

Other Medicines and Lab Tests

Tell patient Two heart-rhythm medicines — verapamil and diltiazem — must NOT be used together with labetalol because the combination can cause a dangerously slow heart rate. Tell your prescriber about every medicine you take, including over-the-counter products. Labetalol can also cause some lab tests to look abnormal — particularly urine tests for adrenaline-related substances (used to look for a rare tumour called pheochromocytoma) and urine drug screens for amphetamines. Always tell the lab and the doctor ordering the test that you take labetalol.

Call prescriber If you start any new prescription, OTC product, or herbal supplement and want to confirm compatibility; before any blood-pressure-related work-up that includes urine adrenaline testing.

Ref

Sources

Regulatory (PI / SmPC)

U.S. Food and Drug Administration. Labetalol Hydrochloride Tablets prescribing information. Alvogen, Inc. Revised April 2024. FDA label PDF Primary source for the 2024 oral labetalol indication, dosing, contraindications (including the unusual contraindication of concomitant non-DHP CCBs), pharmacokinetics, and adverse-event Table 1 with placebo-controlled incidence rates. Confirms Initial U.S. Approval date of 1984.
U.S. Food and Drug Administration. Trandate (labetalol hydrochloride) Tablets prescribing information. FDA label PDF Brand-name reference label with detailed lactation data (~0.004% of maternal dose excreted in human milk) and elderly-population information.
U.S. Food and Drug Administration. Trandate (labetalol hydrochloride) Injection prescribing information. FDA label PDF Source for IV bolus and continuous-infusion dosing, IV-specific α:β ratio of 1:7, supine positioning requirement, dose-stratified AE table across daily doses 200–2,400 mg, IV-specific AE rates per 100 patients (including 58% postural hypotension if tilted within 3 hours), the dilevalol hepatotoxicity historical context, and overdose management with glucagon 5–10 mg over 30 seconds followed by 5 mg/h infusion.

Key Clinical Trials

Magee LA, von Dadelszen P, Rey E, et al. Less-tight versus tight control of hypertension in pregnancy. N Engl J Med. 2015;372(5):407-417. DOI: 10.1056/NEJMoa1404595 CHIPS (Control of Hypertension In Pregnancy Study) trial — randomised non-inferiority trial comparing less-tight versus tight control of non-severe maternal hypertension; labetalol was the most commonly used antihypertensive. Tight control reduced severe hypertension without adverse perinatal outcomes.
Tita AT, Szychowski JM, Boggess K, et al. Treatment for Mild Chronic Hypertension during Pregnancy. N Engl J Med. 2022;386(19):1781-1792. DOI: 10.1056/NEJMoa2201295 CHAP (Chronic Hypertension and Pregnancy) trial — randomised trial demonstrating that targeting BP <140/90 mmHg in chronic hypertension during pregnancy reduces adverse pregnancy outcomes without compromising fetal growth; labetalol and extended-release nifedipine were the predominant agents.

Guidelines

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 ACC/AHA hypertension guideline; defines BP thresholds and treatment goals. Beta-blockers (including labetalol) are not first-line for uncomplicated hypertension but appropriate when there is a compelling indication.
American College of Obstetricians and Gynecologists’ Committee on Practice Bulletins—Obstetrics. ACOG Practice Bulletin No. 203: Chronic Hypertension in Pregnancy. Obstet Gynecol. 2019;133(1):e26-e50. DOI: 10.1097/AOG.0000000000003020 ACOG guidance establishing labetalol as one of the preferred first-line oral antihypertensives in chronic hypertension during pregnancy (alongside extended-release nifedipine; methyldopa and hydrochlorothiazide are secondary options).
ACOG Committee Opinion No. 767: Emergent Therapy for Acute-Onset, Severe Hypertension During Pregnancy and the Postpartum Period. Obstet Gynecol. 2019;133(2):e174-e180. DOI: 10.1097/AOG.0000000000003075 ACOG protocol for emergent antihypertensive therapy in pregnancy; identifies IV labetalol, IV hydralazine, and immediate-release oral nifedipine as first-line agents for acute severe-range BP.
Powers WJ, Rabinstein AA, Ackerson T, et al. Guidelines for the Early Management of Patients With Acute Ischemic Stroke: 2019 Update to the 2018 Guidelines for the Early Management of Acute Ischemic Stroke. Stroke. 2019;50(12):e344-e418. DOI: 10.1161/STR.0000000000000211 AHA/ASA acute ischaemic stroke guidelines; identifies IV labetalol as one of the preferred agents for blood-pressure lowering before and during thrombolytic therapy.
van den Born BH, Lip GYH, Brguljan-Hitij J, et al. ESC Council on hypertension position document on the management of hypertensive emergencies. Eur Heart J Cardiovasc Pharmacother. 2019;5(1):37-46. DOI: 10.1093/ehjcvp/pvy032 European Society of Cardiology position paper defining the role of IV labetalol across hypertensive emergency scenarios including aortic dissection, intracerebral haemorrhage, and pre-eclampsia/eclampsia.
Lenders JWM, Duh QY, Eisenhofer G, et al. Pheochromocytoma and Paraganglioma: An Endocrine Society Clinical Practice Guideline. J Clin Endocrinol Metab. 2014;99(6):1915-1942. DOI: 10.1210/jc.2014-1498 Endocrine Society guidance on perioperative management of pheochromocytoma; emphasises adequate alpha-blockade before any beta-blocker initiation.

Pharmacokinetics / Special Populations

MacCarthy EP, Bloomfield SS. Labetalol: a review of its pharmacology, pharmacokinetics, clinical uses and adverse effects. Pharmacotherapy. 1983;3(4):193-219. DOI: 10.1002/j.1875-9114.1983.tb03252.x Foundational review of labetalol pharmacology published shortly before its 1984 U.S. approval — describes the combined α/β-blockade profile, the four-stereoisomer composition, and the predominantly glucuronide metabolism.
Goa KL, Benfield P, Sorkin EM. Labetalol. A reappraisal of its pharmacology, pharmacokinetics and therapeutic use in hypertension and ischaemic heart disease. Drugs. 1989;37(5):583-627. DOI: 10.2165/00003495-198937050-00002 Comprehensive Drugs review covering labetalol’s stereochemistry, ADME, comparative efficacy versus other antihypertensives, and adverse-effect profile.