Ambrisentan: Complete Drug Monograph

Pharmacokinetic Profile

Half-Life

~15 h (steady-state)

Metabolism

Glucuronidation (UGTs); minor CYP3A4/2C19

Protein Binding

99%

Bioavailability

High (absolute not determined)

Tmax

~2 h

Clinical Information

Drug Class

Selective ET_A Receptor Antagonist

Available Doses

5 mg, 10 mg tablets

Route

Oral

Renal Adjustment

None required

Hepatic Adjustment

Not recommended in moderate-severe impairment

Pregnancy

Contraindicated (Teratogenic)

Lactation

Not recommended

Schedule

Prescription only (REMS removed April 2025)

Generic Available

Yes

Black Box Warning

Embryo-Fetal Toxicity

Indications

Indication	Approved Population	Therapy Type	Status
Pulmonary arterial hypertension (WHO Group 1) — to improve exercise ability and delay clinical worsening	Adults (WHO FC II-III)	Monotherapy; also studied in combination with tadalafil (AMBITION)	FDA Approved

Ambrisentan is indicated for the treatment of pulmonary arterial hypertension in adult patients with WHO functional class II or III symptoms. The pivotal ARIES-1 and ARIES-2 trials enrolled predominantly patients with idiopathic or heritable PAH (60%) and connective tissue disease-associated PAH (34%). The AMBITION trial subsequently established initial combination therapy with ambrisentan plus tadalafil as a preferred first-line strategy, demonstrating a 50% reduction in clinical failure events compared with either agent alone (FDA PI; NEJM 2015).

Off-Label Uses

Chronic thromboembolic pulmonary hypertension (CTEPH, WHO Group 4): Limited data from the ARIES-3 open-label study included a small subset of CTEPH patients. Evidence quality: Low. Not a substitute for surgical pulmonary endarterectomy in operable disease.

Pediatric PAH: Small pharmacokinetic and safety studies suggest ambrisentan may be tolerated in children, but safety and efficacy have not been established by the FDA. Evidence quality: Low.

Dose

Dosing

Adult Dosing — By Clinical Scenario

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
PAH monotherapy — new diagnosis, WHO FC II-III	5 mg once daily	5-10 mg once daily	10 mg/day	Titrate at 4-week intervals based on tolerability Do not split, crush, or chew tablets; food does not affect absorption
PAH — initial combination with tadalafil (AMBITION regimen)	5 mg once daily + tadalafil 20 mg once daily	10 mg once daily + tadalafil 40 mg once daily	10 mg/day	Uptitrate ambrisentan at 8 weeks; tadalafil at 4 weeks ESC/ERS 2022 Class I recommendation for initial combination in iPAH/hPAH
PAH with concurrent cyclosporine use	5 mg once daily	5 mg once daily	5 mg/day	Cyclosporine approximately doubles ambrisentan exposure; do not exceed 5 mg FDA PI mandates dose cap
PAH in elderly patients (age 65 and older)	5 mg once daily	5-10 mg once daily	10 mg/day	Higher incidence of peripheral edema (29% vs 14% in younger adults) Smaller improvement in 6MWD observed in subgroup analyses
Transition from bosentan due to hepatotoxicity	5 mg once daily	5-10 mg once daily	10 mg/day	Ensure aminotransferases have normalized before switching Lower risk of hepatic enzyme elevations compared with bosentan

Clinical Pearl: Dosing Considerations

Unlike bosentan, ambrisentan does not require dose-dependent titration through a mandatory initial period. However, starting at 5 mg with optional uptitration at 4 weeks allows assessment of tolerability, particularly regarding peripheral edema. Doses above 10 mg daily have not been studied in PAH patients. No dose adjustment is needed for renal impairment, including severe renal impairment, although hemodialysis clearance has not been characterized.

Pharmacology

Mechanism of Action

Ambrisentan is a propanoic acid-derived, non-sulfonamide endothelin receptor antagonist with high selectivity for the endothelin type-A (ET_A) receptor over the ET_B receptor (selectivity ratio exceeding 4,000:1). In pulmonary arterial hypertension, endothelin-1 (ET-1) concentrations are elevated up to 10-fold in plasma and 9-fold in pulmonary vascular endothelium, driving pathological vasoconstriction and smooth muscle proliferation through ET_A receptor activation. By selectively blocking ET_A, ambrisentan inhibits vasoconstriction and cell proliferation while preserving ET_B-mediated vasodilation, nitric oxide release, and endothelin clearance. This selectivity profile distinguishes ambrisentan from dual-receptor antagonists like bosentan. The clinical significance of this selectivity difference, however, has not been established in comparative outcome trials.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Rapidly absorbed; Tmax ~2 h; food does not affect bioavailability; dose-linear PK over 1-100 mg	Can be taken with or without food; predictable exposure across dose range
Distribution	99% protein bound; substrate of P-glycoprotein (P-gp) and OATP	Highly protein-bound; P-gp and OATP substrate status relevant to cyclosporine interaction
Metabolism	Primarily hepatic glucuronidation (phase II UGTs); minor oxidative metabolism via CYP3A4 and CYP2C19; active metabolite (4-hydroxymethyl) ~4% of parent AUC	Minimal CYP-mediated metabolism explains low drug interaction potential compared with bosentan; not a CYP inducer or clinically significant inhibitor
Elimination	Predominantly non-renal (hepatic/biliary); t_1/2 ~15 h at steady state; steady state reached in 3-4 days	Once-daily dosing supported by 15 h half-life; no renal dose adjustment required; not studied in hemodialysis

Side Effects

≥10% Very Common

Adverse Effect	Incidence	Clinical Note
Peripheral edema	17% (vs 11% placebo)	Class effect of ERAs; higher in elderly (29%); may require diuretics; distinguish from worsening right heart failure

1-10% Common

Adverse Effect	Incidence	Clinical Note
Nasal congestion	6% (vs 2% placebo)	Dose-dependent; related to vasodilatory effects; usually mild
Flushing	4% (vs 1% placebo)	Vasodilatory mechanism; tends to diminish over time
Sinusitis	3% (vs 0% placebo)	May overlap with nasal congestion; treat symptomatically
Headache	Common (higher with 10 mg; EMA SmPC)	Not in FDA PI Table 1 (>3% placebo-adjusted); classified as common (1-10%) in EMA SmPC; dose-related; generally self-limiting
Hemoglobin decrease	7% marked decrease (>15% from baseline)	Mean decrease 0.8 g/dL over 12 weeks; onset within first few weeks, then stabilizes; not from hemorrhage or hemolysis; 10% incidence at 10 mg dose
Palpitations	Common (EMA SmPC)	Classified as common (1-10%) in EMA SmPC; likely secondary to vasodilation; not listed in FDA PI Table 1

Serious Serious (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Embryo-fetal toxicity	Expected if exposed	First trimester	Absolute contraindication; pregnancy test before start, monthly during, and 1 month after; discontinue immediately if pregnancy detected
Heart failure / fluid retention requiring hospitalization	Rare (postmarketing)	Weeks after initiation	Assess volume status; initiate diuretics; evaluate for decompensated right heart failure; consider discontinuation
Anemia requiring transfusion	Rare (postmarketing)	First weeks to months	Exclude other causes; consider discontinuation if clinically significant and unexplained
Hepatotoxicity (aminotransferase elevation >3x ULN)	0% in ARIES trials (vs 2.3% placebo); rare postmarketing	Variable	Discontinue if ALT/AST >5x ULN or elevated with bilirubin >2x ULN; investigate cause fully
Hypersensitivity (angioedema, rash)	Rare (postmarketing)	Any time	Discontinue permanently; standard allergy management
Pulmonary edema (PVOD-related)	Very rare	Early in therapy	Consider pulmonary veno-occlusive disease; discontinue if confirmed
Decreased sperm count	Frequency unknown (class effect)	With prolonged use	Counsel male patients about potential fertility effects before initiation

Discontinuation Discontinuation Rates

ARIES-1 and ARIES-2 (Monotherapy)

2% vs 2% placebo

Top reasons: Adverse events related to PAH progression rather than drug toxicity

AMBITION (Combination Therapy)

Similar across arms

Top reasons: Peripheral edema and dyspnea were the most common reasons for stopping therapy

Reason for Discontinuation	Incidence	Context
Peripheral edema	<1%	Most common non-PAH-related cause in both monotherapy and combination arms
Dyspnea	<1%	Often difficult to distinguish from disease progression

Managing Peripheral Edema

Peripheral edema is the most frequently encountered adverse effect of ambrisentan. It is important to distinguish ERA-related fluid retention from worsening right ventricular failure. If weight gain exceeds 2-3 kg over days, assess jugular venous pressure, hepatic congestion markers, and BNP levels. Mild edema can generally be managed with loop diuretics. Hospitalization for fluid management has been reported in postmarketing surveillance, particularly in patients with advanced right heart disease.

Int

Drug Interactions

Ambrisentan has a notably favorable drug interaction profile compared with other ERAs. It is primarily cleared by glucuronidation rather than CYP-mediated oxidation, does not induce or significantly inhibit CYP enzymes, and does not alter warfarin pharmacokinetics. It is, however, a substrate of P-glycoprotein (P-gp), organic anion transporting polypeptide (OATP), and CYP3A4, making it susceptible to inhibitors of these transporters and enzymes.

Major Cyclosporine

MechanismInhibition of P-gp, OATP, and CYP3A4; approximately 2-fold increase in ambrisentan exposure

EffectDoubled ambrisentan plasma levels; increased risk of adverse effects including edema and hemoglobin drop

ManagementLimit ambrisentan to 5 mg once daily when co-administered; monitor closely for fluid retention

FDA PI

Moderate Strong CYP3A4 Inhibitors (e.g., ketoconazole, ritonavir)

MechanismCYP3A4 contributes to minor oxidative metabolism; strong inhibitors may modestly increase ambrisentan levels

EffectPotential for increased exposure, though effect is expected to be less than with cyclosporine

ManagementMonitor for edema, headache, and flushing; consider maintaining 5 mg dose

FDA PI / Lexicomp

Moderate Rifampin

MechanismPotent inducer of OATP, P-gp, and CYP3A4; initial single-dose uptake may transiently increase ambrisentan levels, but chronic use may reduce exposure

EffectComplex bidirectional effects; clinical significance uncertain

ManagementUse with caution; monitor clinical response and PAH symptoms

Lexicomp

Minor Warfarin

MechanismNo significant pharmacokinetic interaction; ambrisentan does not affect CYP2C9 (unlike bosentan)

EffectNo clinically meaningful change in INR or warfarin dose observed in clinical trials

ManagementRoutine INR monitoring as per standard anticoagulation practice; no dose adjustment needed

ARIES Trials / FDA PI

Minor Sildenafil / Tadalafil (PDE5 Inhibitors)

MechanismNo clinically relevant pharmacokinetic interaction between ambrisentan and PDE5 inhibitors

EffectPharmacodynamic synergy (additive vasodilation) without altered drug levels

ManagementCombination is established therapy (AMBITION trial); monitor for hypotension and edema

AMBITION / FDA PI

Minor Omeprazole

MechanismNo significant effect on ambrisentan pharmacokinetics per population PK analysis

EffectNone clinically relevant

ManagementNo dose adjustment needed

FDA PI

Key Advantage: Favorable Interaction Profile

Unlike bosentan, which induces CYP2C9 and CYP3A4 and alters warfarin and hormonal contraceptive metabolism, ambrisentan does not significantly affect CYP enzymes. This means no warfarin dose adjustment is needed and hormonal contraceptives can be used as part of the required pregnancy prevention strategy without efficacy concerns related to the ERA itself.

Mon

Monitoring

Pregnancy Test Before initiation, then as clinically indicated
Routine Negative pregnancy test required before starting. Advise effective contraception during treatment and for 1 month after stopping. Discontinue immediately if pregnancy is detected.
Hemoglobin / Hematocrit Baseline, 1 month, then periodically
Routine Mean Hb decrease ~0.8 g/dL. Marked decreases (>15% from baseline) in 7% of patients overall, 10% at 10 mg. Do not initiate in patients with clinically significant anemia. Exclude other causes if significant drop occurs.
Liver Function (ALT, AST, Bilirubin) Baseline, then as clinically indicated
Trigger-based Routine periodic LFT monitoring is no longer mandated by the FDA label for ambrisentan specifically (unlike bosentan). However, monitor if symptoms of hepatic injury appear. Discontinue if AST/ALT >5x ULN or if elevations accompany bilirubin >2x ULN.
Weight and Edema Assessment Each visit
Routine Assess for peripheral edema and weight gain at every clinic visit. Rapid weight gain (>2-3 kg) should prompt evaluation for fluid retention versus worsening right heart failure.
Functional Capacity (6MWD, WHO FC) Baseline, 3-6 months, then 6-12 monthly
Routine Improvement in 6MWD expected by 4-12 weeks. Declining walk distance may indicate disease progression or the need for combination therapy escalation.
BNP / NT-proBNP Baseline, then every 3-6 months
Routine Rising natriuretic peptides suggest clinical worsening. Use in conjunction with functional class and echocardiographic findings per ESC/ERS risk stratification.

Contraindications & Cautions

Absolute Contraindications

Pregnancy: Ambrisentan is teratogenic in animals at exposures near or below human therapeutic levels. It caused jaw, palate, heart, and great vessel malformations in rats and rabbits. Absolutely contraindicated in pregnant women or women who may become pregnant without effective contraception.
Idiopathic pulmonary fibrosis (IPF): The ARTEMIS trial was terminated early because ambrisentan increased disease progression and hospitalization in IPF patients. This contraindication applies regardless of whether pulmonary hypertension (WHO Group 3) is present.

Relative Contraindications (Specialist Input Recommended)

Moderate or severe hepatic impairment: Not recommended. No data on use in patients with pre-existing moderate or severe liver disease. Exposure may be increased and hepatic safety has not been established in this population.
Clinically significant anemia (Hb below lower limit of normal): Ambrisentan reduces hemoglobin further; initiation is not recommended until anemia is corrected or an informed risk-benefit decision is made.
Suspected pulmonary veno-occlusive disease: Vasodilators including ERAs can precipitate acute pulmonary edema in PVOD. If acute pulmonary edema develops during initiation, PVOD should be considered and the drug discontinued.

Use with Caution

Elderly patients (age 65 and older): Higher rates of peripheral edema (29%) and smaller functional improvements observed in subgroup analyses.
Males desiring fertility: Endothelin receptor antagonists as a class have been associated with decreased sperm counts in animal and human studies. Counsel regarding potential effect on spermatogenesis before starting therapy.
Mild hepatic impairment: Limited data; use with monitoring for hepatic enzyme elevations.
Concurrent cyclosporine use: Requires dose cap at 5 mg daily due to approximately 2-fold increase in ambrisentan exposure.

FDA Boxed Warning Embryo-Fetal Toxicity

Ambrisentan is contraindicated during pregnancy because it may cause major birth defects based on animal studies. In both rats and rabbits, ambrisentan caused malformations of the jaw, palate, heart, and great vessels, as well as failure of thymus and thyroid formation. For females of reproductive potential, exclude pregnancy before starting treatment, advise effective contraception during treatment and for one month after discontinuation, and discontinue immediately if pregnancy is detected. As of April 2025, the FDA removed the REMS program (including elements to assure safe use) from the ambrisentan labeling, determining that a REMS was no longer necessary. The boxed warning and contraception requirements remain in the prescribing information.

Patient Counselling

Purpose of Therapy

Ambrisentan works by blocking a substance called endothelin that narrows blood vessels in the lungs. Taking this medication daily helps lower the pressure in lung arteries, improves the ability to exercise, and slows worsening of the disease. It does not cure pulmonary arterial hypertension but is an important part of long-term management.

How to Take

Take one tablet once daily at the same time each day, with or without food. Swallow the tablet whole; do not split, crush, or chew. If a dose is missed, take it as soon as remembered and continue with the regular schedule. Do not take two doses to make up for a missed one. Store at room temperature in the original packaging.

Pregnancy Prevention (Critical)

Tell patient Ambrisentan causes serious birth defects. All women who can become pregnant must use effective contraception before starting, during treatment, and for one month after stopping. A pregnancy test is required before the first dose.

Call prescriber Immediately if pregnancy is suspected or confirmed, or if a menstrual period is missed.

Swelling of Ankles and Legs

Tell patient Swelling in the ankles, feet, or legs is common with this medication. It does not always mean the heart condition is worsening. Weigh yourself regularly and report sudden weight gain.

Call prescriber If swelling becomes severe, is accompanied by shortness of breath at rest, or if weight increases by more than 2-3 kg over a few days.

Nasal Congestion and Flushing

Tell patient Stuffy nose and facial flushing are expected effects of the medication opening blood vessels. These are usually mild and often improve over time.

Call prescriber If nasal congestion is severe enough to impair breathing or sleep, or if flushing is accompanied by lightheadedness or fainting.

Blood Count Changes

Tell patient This medication may cause a drop in red blood cells, which can cause tiredness. Blood tests will be done before starting, at one month, and periodically. Report unusual fatigue, paleness, or dizziness.

Call prescriber If experiencing significant new fatigue, shortness of breath disproportionate to usual, or any signs of bleeding.

Male Fertility

Tell patient This class of medication may reduce sperm counts. Discuss fertility preservation options with your doctor before starting if planning to father children.

Call prescriber If fertility concerns arise during treatment; a semen analysis may be considered.

Ref

Sources

Regulatory (PI / SmPC)

Letairis (ambrisentan) tablets. Full Prescribing Information. Gilead Sciences, Inc. Revised 2025. Gilead PI Primary reference for all dosing, pharmacokinetics, adverse reactions, and contraindications.
Ambrisentan tablets. DailyMed (generic label, Mylan). Updated April 2025. DailyMed Updated generic label reflecting 2025 REMS modifications and boxed warning revisions.
Ambrisentan Viatris. Summary of Product Characteristics (SmPC). European Medicines Agency. EMA SmPC European regulatory reference with frequency-based adverse reaction classification (MedDRA).

Key Clinical Trials

Galiè N, Olschewski H, Oudiz RJ, et al. Ambrisentan for the treatment of pulmonary arterial hypertension: results of the ARIES study 1 and 2. Circulation. 2008;117(23):3010-3019. doi:10.1161/CIRCULATIONAHA.107.742510 Pivotal phase III trials establishing efficacy in 6MWD improvement across 2.5-10 mg doses.
Galiè N, Barberà JA, Frost AE, et al. Initial use of ambrisentan plus tadalafil in pulmonary arterial hypertension. N Engl J Med. 2015;373(9):834-844. doi:10.1056/NEJMoa1413687 AMBITION trial: 50% reduction in clinical failure with initial combination therapy; landmark trial informing ESC/ERS guidelines.
Hoeper MM, McLaughlin VV, Barberá JA, et al. Initial combination therapy with ambrisentan and tadalafil and mortality in patients with PAH. Lancet Respir Med. 2016;4(11):894-901. doi:10.1016/S2213-2600(16)30307-1 Secondary mortality analysis of AMBITION suggesting potential survival advantage with combination therapy.
Coghlan JG, Galiè N, Barberà JA, et al. Initial combination therapy with ambrisentan and tadalafil in CTD-PAH: subgroup analysis from the AMBITION trial. Ann Rheum Dis. 2017;76(7):1219-1227. doi:10.1136/annrheumdis-2016-210236 Demonstrates combination therapy benefit in CTD-PAH and SSc-PAH subgroups.

Guidelines

Humbert M, Kovacs G, Hoeper MM, et al. 2022 ESC/ERS Guidelines for the diagnosis and treatment of pulmonary hypertension. Eur Heart J. 2022;43(38):3618-3731. doi:10.1093/eurheartj/ehac237 Current comprehensive guideline recommending initial ambrisentan + tadalafil combination as Class I for treatment-naive iPAH/hPAH.
Klinger JR, Elliott CG, Levine DJ, et al. Therapy for pulmonary arterial hypertension in adults: update of the CHEST guideline and expert panel report. Chest. 2019;155(3):565-586. doi:10.1016/j.chest.2018.11.030 CHEST 2019 guideline with conditional recommendation for ambrisentan + tadalafil in treatment-naive WHO FC II-III PAH.

Mechanistic / Basic Science

Galiè N, Badesch D, Oudiz R, et al. Ambrisentan therapy for pulmonary arterial hypertension. J Am Coll Cardiol. 2005;46(3):529-535. doi:10.1016/j.jacc.2005.04.050 Phase II dose-ranging study establishing the 5-10 mg therapeutic range and ET_A selectivity profile.

Pharmacokinetics / Special Populations

Barst RJ. A review of pulmonary arterial hypertension: role of ambrisentan. Vasc Health Risk Manag. 2007;3(1):11-22. PMC1994051 Comprehensive early review covering ambrisentan PK profile including steady-state half-life, protein binding, and glucuronidation pathway.
Rivera-Lebron BN, Risbano MG. Ambrisentan: a review of its use in pulmonary arterial hypertension. Ther Adv Respir Dis. 2017;11(5):233-244. doi:10.1177/1753465817696040 Clinical review synthesizing pharmacokinetics, ARIES long-term extension data, and AMBITION trial outcomes.
McGoon MD, Frost AE, Oudiz RJ, et al. Ambrisentan therapy in patients with pulmonary arterial hypertension who discontinued bosentan or sitaxsentan due to liver function test abnormalities. Chest. 2009;135(1):122-129. doi:10.1378/chest.08-1028 Key study supporting ambrisentan use in patients with prior ERA-related hepatotoxicity; no recurrence of aminotransferase elevations.

Letairis (Ambrisentan)