Ipratropium Bromide: Comprehensive Drug Monograph

Pharmacokinetic Profile

Half-Life

~2 hours (inhalation and IV)

Onset of Action

15–30 min; peak 1–2 hours

Duration

3–5 hours (up to 2–4 h per FDA PI)

Metabolism

Partial ester hydrolysis to inactive metabolites

Systemic Absorption

Minimal (quaternary amine)

Clinical Information

Drug Class

Short-acting muscarinic antagonist (SAMA)

Available Forms

MDI (17 mcg/puff); neb solution (0.5 mg/2.5 mL, 0.02%); nasal spray 0.03%, 0.06%

Route

Inhaled (MDI), nebulized, intranasal

Renal Adjustment

Not studied; caution advised (renally excreted)

Hepatic Adjustment

Not studied

Pregnancy

No drug-associated risk identified in published data

Lactation

Unknown excretion; low systemic levels expected

Pediatric (MDI)

Safety/efficacy not established

Generic Available

Yes

Indications for Ipratropium

Indication	Approved Population	Therapy Type	Status
Maintenance treatment of bronchospasm associated with COPD (chronic bronchitis and emphysema)	Adults	Scheduled maintenance bronchodilator	FDA Approved
Rhinorrhea associated with allergic and nonallergic perennial rhinitis (nasal spray 0.03%)	≥6 years	Symptomatic relief	FDA Approved
Rhinorrhea associated with the common cold (nasal spray 0.06%)	≥5 years	Symptomatic relief	FDA Approved

Ipratropium bromide is a short-acting muscarinic antagonist (SAMA) and the most widely used inhaled anticholinergic bronchodilator. In COPD, it provides consistent bronchodilation by blocking vagal cholinergic tone in airway smooth muscle. GOLD guidelines position short-acting bronchodilators (SABA or SAMA) for initial symptomatic relief, with long-acting agents (LAMA such as tiotropium) preferred for maintenance in patients with persistent symptoms.

Off-Label Uses

Acute asthma exacerbation (adjunctive with SABA): Nebulized ipratropium 0.5 mg combined with albuterol every 20 minutes for 3 doses is recommended by GINA and NAEPP for moderate-to-severe acute asthma in the emergency department. The addition of ipratropium to SABA reduces hospitalization rates. Benefit is not sustained once the patient is admitted. Evidence quality: High

Acute COPD exacerbation: Nebulized ipratropium 0.5 mg with albuterol is standard practice for acute COPD exacerbations in the ED. Evidence quality: Moderate

FDA Label Warning Not for Acute Rescue

Atrovent HFA is indicated for the maintenance treatment of bronchospasm associated with COPD and is NOT indicated for the initial treatment of acute episodes of bronchospasm where rescue therapy is required for rapid response. A SABA (albuterol) should always be available as rescue therapy (FDA PI).

Dose

Dosing of Ipratropium

Inhaled Dosing (Atrovent HFA MDI)

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
COPD maintenance — adults (MDI)	2 puffs (34 mcg) QID	2 puffs QID	12 puffs/24 h	Each actuation delivers 17 mcg from mouthpiece (21 mcg from valve) Solution aerosol — does NOT require shaking before use. Prime 2 sprays before first use or after >3 days of non-use (FDA PI)

Nebulizer Dosing

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
COPD maintenance — adults ≥12 years (nebulizer 0.02%)	500 mcg (0.5 mg) nebulized TID–QID	500 mcg q6–8h	2 mg/day (4 doses)	Deliver via jet nebulizer over 5–15 min May be mixed with albuterol in the same nebulizer; do not mix with cromolyn (incompatible)
Acute asthma exacerbation — adults (off-label, NAEPP/GINA)	0.5 mg nebulized q20min ×3 doses	0.5 mg q4–6h PRN	Per clinical judgment	Always co-administer with SABA (albuterol 2.5–5 mg); do not use as monotherapy Benefit not sustained after admission; primary value is in the first 3 hours of ED management
Acute asthma exacerbation — pediatric (off-label, NAEPP)	0.25–0.5 mg nebulized q20min ×3 doses	0.25–0.5 mg q4–6h PRN	Per clinical judgment	Use 0.25 mg for children <5 years; 0.5 mg for ≥5 years; always combine with albuterol

Clinical Pearl: Ipratropium Does Not Replace Albuterol

Ipratropium has a slower onset (15–30 minutes) than albuterol (5–15 minutes) and provides complementary bronchodilation via a different mechanism. In acute exacerbations, it should always be co-administered with a SABA — never as sole bronchodilator therapy. The fixed combination of ipratropium 0.5 mg plus albuterol 2.5 mg (Combivent/DuoNeb) is commercially available for convenience.

Nasal Spray Dosing

Allergic/nonallergic perennial rhinitis (0.03%): 2 sprays (42 mcg) per nostril BID–TID; ages ≥6 years. Common cold rhinorrhea (0.06%): 2 sprays (84 mcg) per nostril TID–QID; ages ≥5 years; use for up to 4 days. Prime with 7 sprays before first use.

Pharmacology of Ipratropium

Mechanism of Action

Ipratropium bromide is an anticholinergic (parasympatholytic) agent that inhibits vagally-mediated reflexes by antagonizing the action of acetylcholine at muscarinic receptors (M1, M2, M3) on bronchial smooth muscle. It is a nonselective muscarinic antagonist. By blocking acetylcholine-induced increases in intracellular calcium, ipratropium prevents bronchoconstriction and reduces mucus secretion from submucosal glands. Unlike beta-agonists, ipratropium does not inhibit mast cell mediator release or enhance mucociliary clearance. Its bronchodilatory effect is most pronounced in COPD, where vagal cholinergic tone is a major contributor to airflow limitation, and relatively less prominent in asthma where inflammation-mediated bronchoconstriction predominates.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Quaternary amine — poorly absorbed from lung and GI tract; Cmax 59±20 pg/mL after single 84 mcg dose (4 puffs); steady-state peak 82±39 pg/mL with QID dosing	Very low systemic bioavailability minimizes systemic anticholinergic side effects (dry mouth, urinary retention, constipation); does not cross blood-brain barrier
Distribution	Minimally bound to plasma proteins (0–9% in vitro to albumin and α1-acid glycoprotein)	Low protein binding means drug-displacement interactions are not clinically significant
Metabolism	Partially metabolized to inactive ester hydrolysis products; not a CYP substrate	No CYP-mediated drug interactions; metabolism is primarily non-enzymatic hydrolysis
Elimination	t½ ~2 h (inhalation and IV); ~50% excreted unchanged in urine after IV dosing; after nebulization, ~4% excreted unchanged in urine (reflecting low systemic absorption)	Short half-life supports QID dosing; renal clearance exceeds GFR, indicating active tubular secretion

Side Effects of Ipratropium

Adverse event data for Atrovent HFA are derived from two 12-week, double-blind, placebo-controlled studies and one 1-year open-label study in 1,010 COPD patients (Atrovent HFA N=243, placebo N=128 in the 12-week study; Atrovent HFA N=305 in the 1-year study). Drug-related adverse events occurred in 9.3% of Atrovent HFA patients; the most common were dry mouth (1.6%) and taste perversion (0.9%) (FDA PI).

≥5%Most Common (≥5% and > Placebo)

Adverse Effect	12-Week Study	Placebo	1-Year Study	Clinical Note
Bronchitis	10%	6%	23%	May reflect COPD-related intercurrent infections rather than drug effect; higher 1-year rate consistent with chronic disease course
COPD exacerbation	8%	13%	23%	Placebo rate was actually higher in the 12-week study (13% vs 8%), suggesting ipratropium may reduce exacerbation risk
Dyspnea	8%	4%	7%	Assess for paradoxical bronchospasm vs underlying disease progression
Headache	6%	8%	7%	Comparable to placebo; likely disease or population-related

1–5%Common (1–5% and > Placebo)

Adverse Effect	12-Week Study	Placebo	1-Year Study	Clinical Note
Dry mouth	4%	2%	2%	Classic anticholinergic effect; most common drug-related AE (1.6% investigator-attributed); usually mild; good oral hygiene important
Nausea	4%	2%	4%	May relate to swallowed drug fraction with bitter taste
Influenza-like symptoms	4%	2%	8%	Likely intercurrent infection rather than drug effect
Dizziness	3%	2%	3%	Advise caution with driving and operating machinery
Back pain	2%	2%	7%	Comparable to placebo in short-term; higher in 1-year study
UTI	2%	1%	10%	Consider relationship to anticholinergic urinary retention effects in elderly COPD patients

SeriousSerious Adverse Effects

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Paradoxical bronchospasm	Rare	During or shortly after inhalation	Discontinue immediately; institute alternative bronchodilator; may be life-threatening
Narrow-angle glaucoma / increased IOP	Uncommon	Minutes to hours; especially if sprayed into eyes or nebulized with face mask	Eye pain, blurred vision, mydriasis, visual halos, conjunctival congestion; consult ophthalmology urgently; avoid spraying into eyes
Urinary retention	Uncommon (post-marketing)	Hours to days; more common in males with BPH	Caution in patients with prostatic hyperplasia or bladder-neck obstruction; may require catheterization
Anaphylaxis / angioedema	Rare (post-marketing)	During or shortly after administration; positive rechallenge reported	Discontinue at once; treat with epinephrine; do not rechallenge; note cross-reactivity with atropine derivatives
SVT / atrial fibrillation	0.5% (5-year placebo-controlled trial, post-marketing)	Variable	ECG monitoring if symptoms develop; evaluate cardiac status

TolerabilityOverall Tolerability

Drug-Related AEs

9.3% Atrovent HFA

Comparable to Atrovent CFC (8.7%). Most common drug-related events: dry mouth (1.6%) and taste perversion / bitter taste (0.9%). Ipratropium is generally well tolerated with a favorable safety profile compared to systemic anticholinergics due to minimal systemic absorption.

Cardiovascular Safety

No clinically significant HR/BP changes

At recommended doses, ipratropium does not produce clinically significant changes in pulse rate or blood pressure (FDA PI section 12.2). This makes it suitable for COPD patients with cardiovascular comorbidities where beta-agonist tachycardia is a concern.

Eye Safety: Nebulizer Mask Considerations

When ipratropium is delivered via nebulizer with a face mask, inadvertent ocular exposure to the aerosol can precipitate or worsen narrow-angle glaucoma. Clinicians should use a mouthpiece rather than a face mask whenever possible. If a face mask is necessary (e.g., in young children or debilitated patients), ensure it fits snugly to minimize eye exposure, and monitor for eye pain or visual disturbance.

Int

Drug Interactions with Ipratropium

Ipratropium has a minimal systemic drug interaction profile because it is a quaternary amine with negligible systemic absorption. Its primary interaction concern is pharmacodynamic: additive anticholinergic effects when combined with other anticholinergic agents. It is not a CYP substrate and does not alter hepatic drug metabolism.

MajorOther Anticholinergic Agents (tiotropium, umeclidinium, glycopyrrolate, oxybutynin, etc.)

MechanismAdditive muscarinic receptor blockade at systemic and local level

EffectIncreased risk of anticholinergic toxicity: dry mouth, constipation, urinary retention, mydriasis, tachycardia, confusion (especially in elderly)

ManagementAvoid co-administration with other inhaled anticholinergics (LAMAs). Assess anticholinergic burden when combining with systemic agents

FDA PI

MinorAlbuterol (Salbutamol)

MechanismComplementary bronchodilation via different pathways (muscarinic antagonism + beta-2 agonism)

EffectAdditive and potentially synergistic bronchodilation with no significant adverse interaction

ManagementSafe and commonly co-administered; available as fixed combination (Combivent Respimat, DuoNeb). May be mixed in the same nebulizer.

Clinical Practice / FDA

ModerateTricyclic Antidepressants / Antihistamines / Antipsychotics with Anticholinergic Properties

MechanismAdditive anticholinergic effects (systemic agents plus local airway effects)

EffectIncreased risk of dry mouth, constipation, urinary retention, cognitive impairment in elderly

ManagementDue to poor systemic absorption of inhaled ipratropium, clinically significant interaction unlikely at recommended doses; assess total anticholinergic burden

Clinical Practice

ModeratePotassium Chloride Oral Formulations

MechanismAnticholinergics reduce GI motility, potentially increasing contact time and risk of GI mucosal injury from solid KCl formulations

EffectIncreased risk of GI ulceration from solid oral potassium supplements

ManagementUse liquid potassium formulations or wax-matrix extended-release tablets if concurrent anticholinergic use

Clinical Practice

Mon

Monitoring for Ipratropium

Pulmonary FunctionPeriodic spirometry
RoutineAssess FEV1 response to ipratropium maintenance therapy. If bronchodilator response is inadequate, consider switching to a LAMA (tiotropium) or adding LABA therapy per GOLD guidelines.
Ocular SymptomsEach visit; urgently if symptomatic
Trigger-basedAsk about eye pain, blurred vision, visual halos, or red eyes. Particularly important in patients with narrow-angle glaucoma or when using nebulizer with face mask. Refer urgently to ophthalmology if symptoms develop.
Urinary SymptomsAt initiation and periodically
Trigger-basedAssess for urinary retention symptoms (difficulty starting stream, incomplete emptying, straining) especially in males with BPH or bladder-neck obstruction.
Anticholinergic BurdenMedication review
RoutineReview concurrent anticholinergic medications (bladder agents, antihistamines, TCAs, antipsychotics). Cumulative anticholinergic burden increases risk of cognitive impairment, falls, and constipation in elderly patients.
Treatment Response4–8 weeks after initiation
RoutineEvaluate symptom control, inhaler technique, and adherence to QID regimen. COPD patients with persistent symptoms despite SAMA therapy may benefit from stepping up to a LAMA which requires only once-daily dosing.

Contraindications & Cautions for Ipratropium

Absolute Contraindications

Hypersensitivity to ipratropium bromide or other Atrovent HFA components — reactions include urticaria, angioedema, rash, bronchospasm, anaphylaxis, and oropharyngeal edema (FDA PI)
Hypersensitivity to atropine or any of its derivatives — ipratropium is a synthetic quaternary ammonium derivative of atropine (FDA PI)

Use with Caution

Narrow-angle glaucoma: Ipratropium may increase intraocular pressure, precipitating or worsening narrow-angle glaucoma. Patients should avoid spraying into eyes. If using nebulizer, prefer mouthpiece over face mask.
Prostatic hyperplasia / bladder-neck obstruction: Anticholinergic effects may worsen urinary retention. Instruct patients to report difficulty with urination.
Pregnancy: Published literature (cohort studies, case-control studies, case series) has not identified a drug-associated risk of major birth defects or miscarriage. No teratogenicity in animal studies at up to 200–40,000 times MRHDID. Negligible systemic absorption makes fetal exposure unlikely (FDA PI 2025).
Lactation: Unknown whether excreted in human milk. Quaternary cations may pass into breast milk; however, plasma levels after inhaled therapeutic doses are very low, so milk levels are expected to be minimal.
Pediatric (MDI): Safety and efficacy not established for Atrovent HFA in the pediatric population. Nasal spray formulations are approved from age 5–6 years. Off-label nebulized use in acute asthma exacerbations is supported by NAEPP/GINA guidelines.
Elderly: 57% of clinical trial subjects were ≥65 years. No overall differences in safety or efficacy observed compared to younger patients. Pharmacokinetics were consistent between older and younger COPD patients.

Patient Counselling for Ipratropium

Purpose of Therapy

Ipratropium (Atrovent HFA) is a maintenance bronchodilator used to keep the airways in your lungs open on a regular basis. It works differently from albuterol — it blocks nerve signals that cause the airways to tighten. It is NOT a rescue inhaler and should not be used to treat sudden breathing emergencies. You should always carry a separate rescue inhaler (such as albuterol) for acute shortness of breath.

How to Use

You do NOT need to shake the Atrovent HFA canister before use. Prime the inhaler with 2 test sprays before the first use or after more than 3 days of non-use. Place your lips firmly around the mouthpiece, press the canister while breathing in slowly and deeply, then hold your breath for up to 10 seconds. Avoid spraying the medication into your eyes. Discard the inhaler when the dose indicator shows zero (200 actuations).

Not a Rescue Inhaler

Tell patientAtrovent HFA takes 15–30 minutes to start working and lasts 2–4 hours. It is designed for regular, scheduled use — not for sudden breathing emergencies. Always have your rescue inhaler (albuterol) available for acute episodes.

Call prescriberIf symptoms are not adequately controlled with regular Atrovent HFA use, or if you are needing your rescue inhaler more frequently than usual.

Eye Safety

Tell patientBe very careful not to spray this medication into your eyes. If it gets into your eyes, it can cause pain, blurred vision, dilated pupils, and worsening of glaucoma. If you use a nebulizer, use a mouthpiece instead of a face mask whenever possible.

Call prescriberImmediately if you experience eye pain, blurred vision, seeing halos around lights, or red eyes after using the inhaler.

Dry Mouth

Tell patientDry mouth is the most common side effect of this medication. Sipping water, chewing sugar-free gum, or using mouth rinse can help. Maintaining good oral hygiene is important to prevent dental problems from chronic dry mouth.

Call prescriberIf dry mouth is severe or persistent, or if you have trouble swallowing.

Urinary Difficulties

Tell patientThis medication may make it harder to urinate, especially if you have an enlarged prostate. Report any difficulty starting your stream, needing to strain, or feeling like your bladder does not empty completely.

Call prescriberIf you are unable to urinate or have significant discomfort.

Inhaler Maintenance

Tell patientWash the mouthpiece with warm water at least once a week and air-dry completely. When the dose indicator background turns red (approximately 40 puffs remaining), contact your pharmacy for a refill. Discard at zero even if the canister feels like it has medication left.

Call prescriberIf the inhaler stops delivering medication despite regular cleaning.

Ref

Sources

Regulatory (PI / SmPC)

ATROVENT HFA (ipratropium bromide HFA inhalation aerosol). Full Prescribing Information. Boehringer Ingelheim Pharmaceuticals, Inc. 2025 Label. FDA Label (PDF)Primary source for all dosing, adverse event Table 1, pharmacokinetic data (Cmax, t½, protein binding), and contraindications/warnings.
Ipratropium Bromide Inhalation Solution 0.02% (500 mcg/2.5 mL). Full Prescribing Information. DailyMedSource for nebulizer solution dosing, pharmacokinetics after nebulization (~4% urinary excretion), and combination data with albuterol.
ATROVENT Nasal Spray 0.03% and 0.06% (ipratropium bromide). Full Prescribing Information. FDA Label (PDF)Source for nasal spray indications (rhinorrhea), dosing, and pediatric safety data.

Guidelines

Global Initiative for Chronic Obstructive Lung Disease (GOLD). Global Strategy for the Diagnosis, Management, and Prevention of COPD, 2024 Report. goldcopd.orgPositions SAMA (ipratropium) and SABA as initial therapy for mild COPD, with LAMAs preferred for maintenance in persistent disease.
Global Initiative for Asthma (GINA). Global Strategy for Asthma Management and Prevention, 2024 Update. ginasthma.orgRecommends nebulized ipratropium + SABA in the first hour of moderate-to-severe asthma exacerbation management.
National Asthma Education and Prevention Program (NAEPP). Expert Panel Report 4 (EPR-4), 2020. doi:10.1016/j.jaci.2020.10.003US guideline recommending ipratropium + SABA for severe acute asthma exacerbations; documents doses for adults and children.

Key Clinical Evidence

Rodrigo GJ, Rodrigo C. The role of anticholinergics in acute asthma treatment: an evidence-based evaluation. Chest. 2002;121(6):1977–1987. doi:10.1378/chest.121.6.1977Meta-analysis demonstrating that adding ipratropium to SABA in acute severe asthma reduces hospitalization rates.
Plotnick LH, Ducharme FM. Combined inhaled anticholinergics and short-acting beta2-agonists for initial treatment of acute asthma in children. Cochrane Database Syst Rev. 2000;(4):CD000060. doi:10.1002/14651858.CD000060Cochrane review supporting ipratropium + SABA in pediatric acute asthma to reduce hospitalization.
Anthonisen NR, Connett JE, Kiley JP, et al. Effects of smoking intervention and the use of an inhaled anticholinergic bronchodilator on the rate of decline of FEV1: the Lung Health Study. JAMA. 1994;272(19):1497–1505. doi:10.1001/jama.1994.03520190043033Landmark Lung Health Study; ipratropium improved FEV1 short-term but did not significantly alter long-term decline in COPD.

Mechanistic / Pharmacology

Gross NJ. Ipratropium bromide. N Engl J Med. 1988;319(8):486–494. doi:10.1056/NEJM198808253190806Comprehensive review of ipratropium pharmacology, clinical efficacy in COPD, and comparison with beta-agonists.
Barnes PJ. The role of anticholinergics in chronic obstructive pulmonary disease. Am J Med. 2004;117 Suppl 12A:24S–32S. doi:10.1016/j.amjmed.2004.10.018Reviews muscarinic receptor subtypes in the lung and the rationale for anticholinergic bronchodilation in COPD vs asthma.
Tashkin DP, Celli B, Senn S, et al. A 4-year trial of tiotropium in chronic obstructive pulmonary disease (UPLIFT). N Engl J Med. 2008;359(15):1543–1554. doi:10.1056/NEJMoa0805800UPLIFT trial establishing tiotropium (LAMA) superiority over ipratropium for COPD maintenance, contextualizing ipratropium in modern COPD management.

Ipratropium Bromide (Atrovent HFA)