Atenolol: Comprehensive Drug Monograph

Pharmacokinetic Profile

Half-Life

6–7 h

Metabolism

Minimal hepatic; renal excretion

Protein Binding

6–16%

Bioavailability

~50% (oral)

Volume of Distribution

Hydrophilic; limited tissue distribution

Clinical Information

Drug Class

Cardioselective beta-1 blocker

Available Doses

25, 50, 100 mg tabs; 5 mg/10 mL IV

Route

Oral, IV

Renal Adjustment

CrCl <35: max 25 mg/day; give post-dialysis

Hepatic Adjustment

Not required (minimal hepatic metabolism)

Pregnancy

Associated with IUGR; use with caution

Lactation

Excreted in breast milk; AAP advises against

Schedule / Legal Status

Rx only (not scheduled)

Generic Available

Yes

Approved Indications & Off-Label Uses

Indication	Approved Population	Therapy Type	Status
Hypertension	Adults	Monotherapy or combination	FDA Approved
Angina pectoris (chronic stable)	Adults	Monotherapy or combination	FDA Approved
Acute myocardial infarction (hemodynamically stable)	Adults	IV then oral (early intervention)	FDA Approved

Atenolol is a hydrophilic, cardioselective beta-1 blocker with no intrinsic sympathomimetic activity and no membrane-stabilizing properties. It was one of the most widely prescribed antihypertensives for decades; however, since the 2002 LIFE trial demonstrated inferior stroke prevention compared with losartan, and subsequent meta-analyses raised concerns about cardiovascular outcomes, current guidelines (2017 ACC/AHA) no longer recommend atenolol as first-line monotherapy for uncomplicated hypertension. It retains important roles in angina, rate control, and secondary prevention post-MI. Notably, atenolol is not one of the three evidence-based beta-blockers recommended for heart failure with reduced ejection fraction.

Off-Label Uses

Rate control in atrial fibrillation/flutter — Once-daily dosing and 24-hour beta-blocking effect support sustained rate control; recommended by AHA/ACC/HRS guidelines as a class option. Evidence quality: High.

Supraventricular tachycardia (SVT) — Used for acute management and prophylaxis of recurrent SVT. Evidence quality: Moderate.

Migraine prophylaxis — Supported by some evidence but less studied than propranolol or metoprolol for this indication. Evidence quality: Low–Moderate.

Thyrotoxicosis symptom control — Controls adrenergic symptoms (tachycardia, tremor); hydrophilic nature means less CNS penetration. Evidence quality: Moderate.

Dose

Dosing by Clinical Scenario

Adult Dosing

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Essential hypertension	50 mg once daily	50–100 mg once daily	100 mg/day	Full effect within 1–2 weeks; doses >100 mg/day unlikely to provide additional benefit Measure trough BP to confirm 24-hour coverage; may use with thiazide diuretics for additive effect
Chronic stable angina	50 mg once daily	100 mg once daily	200 mg/day	Increase after 1 week if response is inadequate; taper gradually over 1–2 weeks if discontinuing Doses of 50–100 mg provide maximum exercise tolerance effect; 200 mg may be needed in some patients
Acute MI — early intervention (hemodynamically stable)	5 mg IV over 5 min x 2 doses	50 mg PO 10 min after last IV dose, then 50 mg 12 h later, then 100 mg QD	100 mg/day (oral maintenance)	Give second IV dose 10 min after first; monitor HR, BP, ECG during IV dosing Continue oral therapy for at least 7 days; data suggest benefit may extend to 1–3 years
Rate control — atrial fibrillation (off-label)	25–50 mg once daily	50–100 mg once daily	200 mg/day	Hydrophilic nature means fewer CNS side effects; target resting ventricular rate per guidelines

Special Populations

Population	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Renal impairment (CrCl 15–35 mL/min)	25 mg once daily	25–50 mg once daily	50 mg/day	No significant accumulation until CrCl <35; half-life markedly prolonged in severe renal impairment
Hemodialysis patients	25–50 mg after each session	25–50 mg post-dialysis	50 mg post-dialysis	Atenolol IS dialyzable (unlike most beta-blockers); give dose after each dialysis session under hospital supervision; marked BP drops can occur
Hepatic impairment	No dose adjustment required. Atenolol undergoes little or no hepatic metabolism; the absorbed portion is eliminated primarily by renal excretion.
Elderly (≥65 years)	25 mg once daily	Titrate cautiously	Standard max	Plasma levels ~50% higher and clearance ~50% lower than younger patients; assess renal function before starting

Clinical Pearl: Hydrophilic Advantage and Limitation

Atenolol’s hydrophilic nature is a double-edged sword. On the positive side, it crosses the blood-brain barrier minimally, leading to fewer CNS side effects (depression, nightmares, insomnia) compared with lipophilic agents like metoprolol or propranolol. This makes it particularly suitable for patients troubled by central side effects on other beta-blockers. On the negative side, its renal-dependent elimination means dose adjustments are critical in patients with impaired kidney function, and the drug is removed by hemodialysis, requiring post-dialysis dosing.

Pharmacology

Mechanism of Action

Atenolol is a second-generation, cardioselective beta-1 adrenergic receptor antagonist. It competitively blocks beta-1 receptors in the heart, reducing heart rate, contractility, and AV conduction velocity. These effects lower cardiac output and myocardial oxygen demand. Like other cardioselective agents, atenolol’s beta-1 selectivity is relative, and at higher doses it may also block beta-2 receptors in bronchial and vascular smooth muscle. Atenolol lacks intrinsic sympathomimetic activity, meaning it does not partially activate the receptors it blocks. It is also devoid of membrane-stabilizing activity, and increasing the dose beyond that required for beta-blockade does not further depress myocardial contractility. Notably, atenolol produces a moderate (~10%) increase in stroke volume at rest and during exercise, distinguishing it from some other beta-blockers.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Rapid but incomplete; ~50% absorbed from GI tract; Tmax 2–4 h; remainder excreted unchanged in feces; food does not significantly affect absorption	50% oral bioavailability is lower than bisoprolol (80%) but higher than carvedilol (25–35%); once-daily dosing effective despite moderate bioavailability
Distribution	Hydrophilic (log P = 0.23); protein binding 6–16%; minimal CNS penetration	Very low protein binding virtually eliminates displacement interactions; hydrophilicity limits blood-brain barrier crossing, reducing CNS side effects (nightmares, depression)
Metabolism	Little or no hepatic metabolism; NOT metabolized by CYP enzymes; no active metabolites	No hepatic dose adjustment needed; no CYP-mediated drug interactions; pharmacokinetically simpler than metoprolol or carvedilol
Elimination	t½ 6–7 h; absorbed portion excreted primarily unchanged by kidneys; renal excretion closely tracks GFR; half-life markedly prolonged in CrCl <35; atenolol IS dialyzable	Renal-dependent elimination makes dose adjustment essential in kidney disease; dialyzability (unlike most beta-blockers) requires post-dialysis dosing; 24-hour beta-blocking effect despite 6–7 h half-life

Atenolol Side Effects

≥10% Very Common (Elicited Data, Foreign + US Studies)

Adverse Effect	Incidence	Clinical Note
Tiredness	26% vs 13% placebo	Most commonly elicited complaint; true drug-attributable rate is approximately half the reported figure when placebo rate is subtracted; may improve over weeks
Cold extremities	12% vs 5% placebo	Peripheral vasoconstriction from beta-2 blockade at higher plasma levels; more troublesome in patients with Raynaud phenomenon or peripheral vascular disease
Dizziness	13% vs 6% placebo	Multifactorial: blood pressure reduction and heart rate slowing; counsel patients to change positions slowly
Depression	12% vs 9% placebo	When elicited by checklist, rates appear high, but placebo-subtracted difference is modest (~3%); recent meta-analyses suggest beta-blockers may contribute more to sleep disturbances than overt depression

1–10% Common (Controlled Hypertension Trials)

Adverse Effect	Incidence	Clinical Note
Dizziness (volunteered)	4% vs 1% placebo	When voluntarily reported (US data), rate is substantially lower than when elicited by checklist; more clinically representative
Fatigue (volunteered)	3% vs 1% placebo	Distinct from “tiredness”; both volunteered at lower rates than elicited; dose-related in longer trials
Bradycardia	3% vs 0% placebo	Expected pharmacologic effect; clinically significant if HR <50 bpm with symptoms; reduce dose or hold
Nausea	3% vs 1% placebo	Usually mild; taking with food may reduce symptoms; persistent nausea warrants evaluation
Postural hypotension	2% vs 1% placebo	Less pronounced than with alpha-blocking agents (carvedilol); counsel slow position changes
Vertigo	2% vs 0.5% placebo	Distinguish from lightheadedness; evaluate for other causes if persistent
Diarrhea	2% vs 0% placebo	Usually self-limiting; maintain hydration
Leg pain	3% vs 1% placebo (elicited)	May reflect peripheral vasoconstriction or underlying vascular disease; assess for claudication

Serious Serious (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Severe bradycardia	1–3%	Days to weeks	Reduce dose or hold; atropine 1–2 mg IV; isoproterenol cautiously; transvenous pacing for refractory cases
Worsening heart failure	Uncommon	Days to weeks	Increase diuretics; consider dose reduction or discontinuation; atenolol is NOT recommended for HFrEF treatment
AV block (2nd/3rd degree)	Rare	Days to weeks	Discontinue atenolol; atropine or isoproterenol; evaluate need for pacing
Bronchospasm	Rare at therapeutic doses	Any time	Administer beta-2 agonist; selectivity is dose-dependent; atenolol produces less FEV1 decline than non-selective agents
Rebound angina/MI on abrupt withdrawal	Rare (if tapered properly)	1–14 days post-discontinuation	Taper gradually; reinstate promptly if rebound symptoms occur; limit physical activity during taper
IUGR in pregnancy	Documented risk	Chronic gestational exposure	Atenolol crosses the placenta; associated with intrauterine growth restriction; consider labetalol as preferred alternative per ACOG

Discontinuation Discontinuation Data

Hypertension Trials

Well tolerated

Key finding: Most adverse effects were mild and transient. Discontinuation rates comparable to placebo in controlled studies.

ISIS-1 (Acute MI)

Dose reduced or stopped in minority

Top reasons: Bradycardia, hypotension, cardiac failure, bronchospasm; events usually responded to atropine or dose withholding

Reason for Discontinuation	Incidence	Context
Bradycardia	Most common in acute MI setting	Usually responded to atropine or dose reduction; less frequent in hypertension trials
Hypotension	More common in acute MI	Resolved with dose withholding in most cases
Cardiac failure	Infrequent	Incidence of heart failure was not increased by atenolol in MI trials overall

Understanding the Side Effect Data: Volunteered vs. Elicited

The Tenormin PI presents adverse event rates from two distinct methodologies. US studies used volunteered reporting (patients spontaneously mentioned symptoms), while foreign studies used a symptom checklist (elicited). Elicited rates are consistently higher for both atenolol and placebo groups. For clinical decision-making, the volunteered US data is more representative of what patients will spontaneously report in practice, while the elicited data captures subclinical effects that may affect quality of life if specifically asked about.

Int

Drug Interactions

Atenolol undergoes minimal hepatic metabolism and is not a CYP enzyme substrate, which eliminates most pharmacokinetic drug interactions that affect lipophilic beta-blockers. Its interaction profile is primarily pharmacodynamic, involving other negative chronotropes, agents with additive hypotensive effects, and drugs that mask hypoglycemia. No clinically relevant pharmacokinetic interactions have been documented with warfarin or common antihypertensives.

MajorVerapamil / Diltiazem

MechanismAdditive AV node depression and negative inotropy (pharmacodynamic)

EffectSevere bradycardia, AV block, heart failure

ManagementAvoid concurrent use, especially IV; if oral co-use essential, monitor ECG and cardiac function closely

FDA PI

MajorClonidine (on withdrawal)

MechanismUnopposed alpha stimulation when clonidine discontinued while beta-blocker continues

EffectSevere rebound hypertension

ManagementDiscontinue atenolol several days before tapering clonidine; close BP monitoring during transition

FDA PI

MajorDisopyramide

MechanismPotent negative inotropic and chronotropic effects of disopyramide compound beta-blockade

EffectSevere bradycardia, asystole, and heart failure

ManagementAvoid combination; if essential, continuous ECG monitoring required

FDA PI

ModerateAmiodarone

MechanismAdditive negative chronotropic and dromotropic effects

EffectEnhanced bradycardia, heart block, left ventricular dysfunction

ManagementMonitor HR and ECG closely; may need atenolol dose reduction

FDA PI

ModerateDigoxin

MechanismAdditive slowing of AV conduction (pharmacodynamic)

EffectIncreased risk of bradycardia and AV block

ManagementMonitor heart rate and ECG periodically; adjust doses based on rate response

FDA PI

ModerateReserpine / Catecholamine-depleting agents

MechanismAdditive reduction in sympathetic activity

EffectExcessive hypotension and/or marked bradycardia causing vertigo, syncope, or postural hypotension

ManagementClose monitoring of HR and BP; may need dose reduction of either agent

FDA PI

ModerateInsulin / Oral hypoglycemics

MechanismBeta-blockade masks adrenergic hypoglycemia signs (tachycardia); beta-1 selective agents are less problematic than non-selective agents

EffectDelayed hypoglycemia recognition

ManagementMonitor blood glucose; educate patients that sweating remains a preserved sign; beta-1 selectivity offers relative advantage

FDA PI

MinorNSAIDs

MechanismProstaglandin inhibition opposes antihypertensive effect

EffectBlunted blood pressure reduction

ManagementMonitor BP; use lowest effective NSAID dose for shortest duration

Lexicomp

Notable Non-Interactions

Because atenolol undergoes minimal hepatic metabolism and is not a CYP substrate, it has no pharmacokinetic interactions with CYP2D6 inhibitors (fluoxetine, paroxetine, quinidine) or CYP3A4 inhibitors/inducers. This is a meaningful clinical advantage over metoprolol and carvedilol in patients requiring complex medication regimens. Similarly, no clinically relevant interaction exists with warfarin or thiazide diuretics.

Mon

Monitoring Parameters

Heart RateEvery visit
RoutineBeta-blocking effect is apparent within 1 hour and persists for 24 hours. Hold or reduce dose if HR <50 bpm with symptoms. During IV dosing for acute MI, monitor continuously.
Blood PressureEvery visit; trough measurement
RoutineMeasure trough BP (just before next dose) to confirm 24-hour coverage, especially at lower doses where end-of-dose BP control may attenuate.
Renal FunctionBaseline; periodically
RoutineAtenolol is renally excreted; no significant accumulation until CrCl <35. Assess CrCl before starting and regularly in patients with known or suspected renal impairment. Age-related renal decline must be factored in.
ECGBaseline; if symptomatic
Trigger-basedAssess for pre-existing conduction abnormalities. Repeat if syncope, presyncope, or palpitations develop. Continuous monitoring required during IV dosing.
Blood GlucosePeriodically in diabetics
RoutineBeta-1 selectivity makes atenolol less likely than non-selective agents to mask hypoglycemia or impair glucose recovery, but caution is still warranted.
Signs of Heart FailureEach visit
Trigger-basedWatch for dyspnea, edema, weight gain. Atenolol can precipitate heart failure in susceptible patients. It is NOT one of the three evidence-based beta-blockers for HFrEF.

Contraindications & Cautions

Absolute Contraindications

Sinus bradycardia
Heart block greater than first degree (without a functioning pacemaker)
Cardiogenic shock
Overt cardiac failure
Untreated pheochromocytoma
Known hypersensitivity to atenolol or its excipients

Relative Contraindications (Specialist Input Recommended)

Bronchospastic disease (asthma, COPD) — atenolol produces significantly less FEV1 decline than non-selective agents, but should be avoided in asthma unless no alternative exists; if used, start at the lowest dose with a beta-2 agonist available
Severe peripheral arterial disease — beta-blockade may aggravate claudication; metabolic acidosis is a contraindication
Pregnancy — associated with intrauterine growth restriction; ACOG recommends labetalol as the preferred beta-blocker for gestational hypertension

Use with Caution

Diabetes mellitus — may mask tachycardia of hypoglycemia; beta-1 selectivity reduces but does not eliminate this risk
Thyrotoxicosis — may mask tachycardia; abrupt withdrawal can precipitate thyroid storm
Renal impairment — dose reduction critical when CrCl <35; atenolol accumulates
Elderly — clearance ~50% lower; start at lower doses and assess renal function
Breastfeeding — excreted in breast milk at ratio 1.5–6.8 to plasma; clinically significant bradycardia reported in breastfed infants; AAP advises against
Major surgery — do not routinely withdraw chronic beta-blocker therapy preoperatively
History of anaphylaxis — patients on beta-blockers may have more severe reactions and be less responsive to epinephrine

FDA Class-Wide Regulatory Warning Abrupt Cessation of Beta-Blocker Therapy

Patients should not abruptly discontinue atenolol. Severe exacerbation of angina pectoris, myocardial infarction, and ventricular arrhythmias have been reported following sudden withdrawal. Taper the dose gradually and advise patients to limit physical activity during the withdrawal period. If angina worsens or acute coronary insufficiency develops, reinstate atenolol promptly.

Patient Counselling

Purpose of Therapy

Atenolol slows your heart rate and lowers your blood pressure, reducing the workload on your heart. Depending on your condition, it may be used to manage high blood pressure, prevent chest pain (angina), or protect your heart after a heart attack.

How to Take

Take atenolol once daily at the same time each day. It can be taken with or without food. Do not stop taking this medication suddenly without consulting your doctor, as this can cause serious heart problems. Your doctor will gradually reduce your dose if the medication needs to be stopped.

Tiredness & Fatigue

Tell patientYou may feel more tired than usual, especially when you first start taking atenolol. This often improves as your body adjusts over the first few weeks. Get adequate rest and avoid driving or operating machinery until you know how the medication affects you.

Call prescriberIf fatigue is severe, persistent, or significantly interferes with daily activities after 2–3 weeks.

Dizziness & Lightheadedness

Tell patientYou may feel dizzy when standing up quickly. Rise slowly from sitting or lying positions. Sit or lie down if you feel dizzy until it passes.

Call prescriberIf dizziness is frequent, causes falls, or is accompanied by fainting.

Never Stop Suddenly

Tell patientStopping atenolol abruptly can cause dangerous effects including worsening chest pain, heart attack, or fast irregular heartbeat. Always consult your doctor before making any changes. If you run out, get a refill immediately.

Call prescriberIf you have missed several doses, or if you develop chest pain or a racing heartbeat after missing doses.

Cold Hands & Feet

Tell patientSome patients notice their hands and feet feel colder than usual. This is caused by reduced blood flow to the extremities. Wear warm clothing in cold weather.

Call prescriberIf fingers or toes change color (white, blue, then red), become painful, or develop sores.

Blood Sugar (Diabetic Patients)

Tell patientThis medication may mask some warning signs of low blood sugar, particularly a fast heartbeat. Sweating and hunger will still occur as warning signs. Monitor your blood sugar more frequently when starting or changing doses.

Call prescriberIf you experience more frequent or severe low blood sugar episodes, or if diabetes becomes harder to manage.

Ref

Sources

Regulatory (PI / SmPC)

Tenormin (atenolol) tablets — FDA-approved prescribing information (revised 2023). accessdata.fda.govPrimary regulatory source for all three approved indications, dosing, adverse reaction table (volunteered vs. elicited), PK parameters, and renal adjustment guidance.
Tenormin (atenolol) tablets — FDA prescribing information (2011 revision). accessdata.fda.govCross-reference for the full adverse event table, ISIS-1 trial data, and contraindications including pregnancy warnings.

Key Clinical Trials

ISIS-1 (First International Study of Infarct Survival) Collaborative Group. Randomised trial of intravenous atenolol among 16,027 cases of suspected acute myocardial infarction. Lancet. 1986;2(8498):57–66. doi:10.1016/S0140-6736(86)90468-6Landmark trial demonstrating 15% relative reduction in mortality with early atenolol in acute MI (n=16,027); basis for the acute MI indication.
Dahlof B, Devereux RB, Kjeldsen SE, et al. Cardiovascular morbidity and mortality in the Losartan Intervention For Endpoint reduction in hypertension study (LIFE). Lancet. 2002;359(9311):995–1003. doi:10.1016/S0140-6736(02)08089-3LIFE trial showing losartan superiority over atenolol for stroke prevention in hypertensive patients with LVH; contributed to atenolol’s decline as first-line antihypertensive.
Carlberg B, Samuelsson O, Lindholm LH. Atenolol in hypertension: is it a wise choice? Lancet. 2004;364(9446):1684–1689. doi:10.1016/S0140-6736(04)17355-8Influential meta-analysis questioning atenolol’s effectiveness as first-line antihypertensive; found no outcome benefit over placebo and inferior results vs. other agents for stroke and mortality.

Guidelines

Whelton PK, Carey RM, Aronow WS, et al. 2017 ACC/AHA Guideline for the Management of High Blood Pressure in Adults. J Am Coll Cardiol. 2018;71(19):e127–e248. doi:10.1016/j.jacc.2017.11.006Current US hypertension guideline; beta-blockers are no longer first-line for uncomplicated hypertension, partly based on atenolol outcome data (LIFE, Carlberg meta-analysis).
Heidenreich PA, Bozkurt B, Aguilar D, et al. 2022 AHA/ACC/HFSA Guideline for the Management of Heart Failure. J Am Coll Cardiol. 2022;79(17):e263–e421. doi:10.1016/j.jacc.2021.12.012Current US HF guideline specifying carvedilol, bisoprolol, and metoprolol succinate as the 3 evidence-based beta-blockers for HFrEF; atenolol is NOT included in this list.
January CT, Wann LS, Calkins H, et al. 2019 AHA/ACC/HRS Focused Update on Atrial Fibrillation. J Am Coll Cardiol. 2019;74(1):104–132. doi:10.1016/j.jacc.2019.01.011Supports beta-blockers including atenolol as an option for ventricular rate control in atrial fibrillation.

Mechanistic / Basic Science

Barrett AM, Cullum VA. The biological properties of the optical isomers of propranolol and their effects on cardiac arrhythmias. Br J Pharmacol. 1968;34(1):43–55. doi:10.1111/j.1476-5381.1968.tb07949.xEarly pharmacology establishing the beta-adrenergic receptor blocking properties relevant to atenolol’s class; foundational work for cardioselective beta-blocker development.

Pharmacokinetics / Special Populations

Mason WD, Winer N, Kochak G, et al. Kinetics and absolute bioavailability of atenolol. Clin Pharmacol Ther. 1979;25(4):408–415. doi:10.1002/cpt1979254408Established the ~50% oral bioavailability, renal-dependent elimination, and 6–7 hour half-life of atenolol in healthy subjects.
Kirch W, Görg KG. Clinical pharmacokinetics of atenolol — a review. Eur J Drug Metab Pharmacokinet. 1982;7(2):81–91. doi:10.1007/BF03188723Comprehensive PK review confirming minimal hepatic metabolism, renal excretion, hydrophilicity, and impact of renal impairment and aging on atenolol disposition.
McAinsh J, Holmes BF, Smith S, Hood D, Warren D. Atenolol kinetics in renal failure. Clin Pharmacol Ther. 1980;28(3):302–309. PubMed: 7408390Quantified the relationship between GFR and atenolol clearance, establishing the CrCl <35 threshold for dose reduction and confirming dialyzability of atenolol.