Esmolol (Brevibloc®)

Esmolol
Brand Name	Brevibloc®
Drug Class	β-Blocker (β1-selective)
Primary Indication	Acute Rate Control
β1 Selectivity	High
Intrinsic Sympathomimetic Activity	No
Half-Life	~9 minutes
Route	IV only
Metabolism	Plasma esterases
FDA Approval	1986

Overview

Esmolol is a short-acting, β1-selective adrenergic receptor antagonist used for rapid, titratable heart rate control in acute settings.

Its ultra-short half-life (~9 minutes) allows for precise titration and rapid discontinuation if adverse effects occur.

It is commonly used in ICU and perioperative settings.

Mechanism of Action

Receptor Activity

Selective β1-adrenergic receptor antagonist

Cardiac Effects

↓ Heart rate
↓ Myocardial contractility
↓ AV nodal conduction

Net Effect

Reduced cardiac output
Rate control in tachyarrhythmias

Minimal β2 activity at therapeutic doses.

Indications

Acute atrial fibrillation with rapid ventricular response
Supraventricular tachycardia
Intraoperative or postoperative tachycardia
Acute hypertension (short-term control)
Thyroid storm (adjunct therapy)

Used when rapid onset and rapid offset are desired.

Contraindications

Absolute:

Severe bradycardia
Second- or third-degree AV block (without pacemaker)
Cardiogenic shock
Decompensated heart failure

Relative / Caution:

Asthma or severe COPD
Hypotension
Peripheral vascular disease

Dosing

IV bolus:

500 mcg/kg over 1 minute

Continuous infusion:

50–200 mcg/kg/min

Titrated based on heart rate and blood pressure.

Effects dissipate within 10–20 minutes after discontinuation.

Pharmacokinetics

Route:

Intravenous only

Metabolism:

Rapid hydrolysis by plasma esterases

Half-life:

~9 minutes

Elimination:

Renal excretion of inactive metabolites

Short half-life allows rapid reversal of effect.

Adverse Effects

Common:

Hypotension
Bradycardia

Serious:

AV block
Acute heart failure exacerbation
Cardiogenic shock

Rapid offset reduces prolonged toxicity risk.

Drug Interactions

Additive AV nodal suppression:

Non-DHP Calcium Channel Blockers (verapamil, diltiazem)
Digoxin

Other antihypertensives:

Increased hypotension risk

Monitoring

Continuous cardiac monitoring
Blood pressure
Heart rate

Used in monitored settings (ICU, OR, ED).

Clinical Pearls

Ultra-short acting β1-selective blocker.
Ideal for unstable or dynamic clinical situations.
Effects disappear quickly after discontinuation.
Metabolized by plasma esterases — not dependent on hepatic metabolism.
Useful in thyroid storm for rapid rate control.

Comparison Within Class

Compared to Metoprolol:

Much shorter half-life
IV only
More titratable

Compared to Propranolol:

β1-selective
Less bronchospasm risk

Compared to Sotalol:

No potassium channel blockade
Not used for rhythm control