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Drug Monograph

Ofev (Nintedanib)

nintedanib — multi-targeted tyrosine kinase inhibitor (anti-fibrotic)

Kinase Inhibitor (PDGFR/FGFR/VEGFR) · Oral Capsule · Pulmonology
Pharmacokinetic Profile
Half-Life
~10–15 hours
Metabolism
Ester hydrolysis (esterases); minor CYP3A4 (~5%); UGT glucuronidation
Protein Binding
~97.8% (albumin)
Bioavailability
~4.7% (fed increases by ~20%)
Volume of Distribution
~1050 L (Vss)
Clinical Information
Drug Class
Multi-targeted kinase inhibitor (PDGFR-α/β, FGFR 1–3, VEGFR 1–3)
Available Doses
100 mg capsule; 150 mg capsule
Route
Oral (with food)
Renal Adjustment
Not required (mild–moderate); not studied in severe
Hepatic Adjustment
Child-Pugh A: 100 mg BID; B/C: Not recommended
Pregnancy
Can cause fetal harm; teratogenic in animals; use contraception
Lactation
Not recommended
Schedule
Rx only (not controlled)
Generic Available
Yes (EU; US generics emerging)
Rx

Indications

Nintedanib is one of only two anti-fibrotic oral therapies available for interstitial lung diseases. It works by inhibiting multiple receptor tyrosine kinases involved in fibrotic tissue remodelling, including the PDGF, FGF, and VEGF receptor families. Its FDA approval spans three distinct ILD populations, making it the broadest-indicated anti-fibrotic agent for lung fibrosis.

IndicationApproved PopulationTherapy TypeStatus
Idiopathic pulmonary fibrosis (IPF)AdultsMonotherapy or with pirfenidoneFDA Approved
Chronic fibrosing ILDs with a progressive phenotype (PPF)AdultsMonotherapyFDA Approved
Systemic sclerosis-associated ILD (SSc-ILD)AdultsMonotherapy or with mycophenolateFDA Approved

Nintedanib slows the rate of FVC decline across all three indications; it is not a cure for fibrosis and does not reverse established lung scarring. The primary clinical benefit is delaying disease progression. Nintedanib is also approved in the EU as Vargatef in combination with docetaxel for adenocarcinoma NSCLC (not covered in this monograph).

Off-Label Uses

Chronic hypersensitivity pneumonitis (progressive) — Patients with progressive fibrosing HP were included in the INBUILD trial and showed benefit consistent with the overall PPF population. Evidence quality: high (subgroup of phase 3 trial).

Unclassifiable ILD with progressive fibrosis — Included in INBUILD. Evidence quality: high.

Dose

Dosing

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
IPF — standard dosing150 mg PO BID150 mg PO BID300 mg/dayTake with food ~12 hours apart; swallow whole
Capsules must not be chewed, crushed, or opened
PPF — chronic fibrosing ILD with progressive phenotype150 mg PO BID150 mg PO BID300 mg/daySame dose regardless of underlying ILD type
INBUILD trial included HP, autoimmune ILDs, unclassifiable ILD
SSc-ILD — slowing FVC decline150 mg PO BID150 mg PO BID300 mg/dayCan be used with stable-dose mycophenolate
49% of SENSCIS patients were on concomitant mycophenolate
Mild hepatic impairment (Child-Pugh A)100 mg PO BID100 mg PO BID200 mg/dayReduced dose; consider interruption or discontinuation for AEs
Child-Pugh B/C: NOT recommended
Adverse reaction management — dose reduction100 mg PO BID100 mg PO BID (may re-escalate)300 mg/dayReduce to 100 mg BID for GI/hepatic AEs; if not tolerated at 100 mg BID, discontinue
May re-escalate to 150 mg BID once AE resolves
Clinical Pearl — Managing the High GI Side Effect Burden

Diarrhea affects 62–76% of patients depending on indication. Proactive counselling is essential: start anti-diarrheal therapy (loperamide) at first signs, ensure adequate hydration, and take nintedanib with food. Many patients will require dose reduction to 100 mg BID (16–34% across trials), but this is preferable to discontinuation. The diarrhea is typically worst in the first 3 months and may improve with continued therapy. Unlike pirfenidone, nintedanib does not cause photosensitivity, and the two agents can be co-administered without PK interaction.

PK

Pharmacology

Mechanism of Action

Nintedanib is a small molecule that competitively binds to the ATP-binding pocket of multiple receptor tyrosine kinases (RTKs) involved in the pathogenesis of pulmonary fibrosis. It inhibits platelet-derived growth factor receptors (PDGFR-α and -β), fibroblast growth factor receptors (FGFR 1–3), and vascular endothelial growth factor receptors (VEGFR 1–3), as well as colony stimulating factor 1 receptor (CSF1R) and Fms-like tyrosine kinase-3 (FLT-3). Nintedanib also inhibits non-receptor tyrosine kinases Lck, Lyn, and Src. By blocking these kinase-mediated signalling cascades, nintedanib inhibits fibroblast proliferation, migration, and differentiation into myofibroblasts, reduces extracellular matrix deposition, and attenuates angiogenesis within the lungs. The net effect is a slowing of the fibrotic remodelling process that underlies progressive lung function decline in IPF, PPF, and SSc-ILD. Nintedanib does not reverse established fibrosis.

ADME Profile

ParameterValueClinical Implication
AbsorptionBioavailability ~4.7% (limited by P-gp efflux and extensive first-pass metabolism); Tmax 2–4 hours; food increases exposure by ~20%; linear PK across 50–450 mg QD and 150–300 mg BID rangeMust be taken with food to maximize absorption; very low bioavailability is inherent to the drug and already accounted for in dosing; P-gp substrate status drives key drug interactions
DistributionVss ~1050 L; protein binding ~97.8% (albumin); extensive tissue distribution; low CNS penetrationVery large Vd indicates extensive peripheral tissue distribution; high protein binding means hemodialysis is not effective for overdose
MetabolismPrimarily by ester hydrolysis (esterases) to BIBF 1202 (free acid metabolite), then glucuronidation (UGT1A1 and others) to BIBF 1202 glucuronide; CYP3A4 accounts for only ~5% of metabolism; no CYP inhibition or clinically relevant CYP inductionEster cleavage (not CYP) is the primary metabolic pathway, reducing traditional CYP-mediated drug interaction risk; however, P-gp interactions remain clinically relevant
Eliminationt½ ~10–15 hours; >93% fecal excretion; <1% renal; clearance ~1390 mL/min (IV); steady state within 1 week; accumulation ratio 1.76-fold (negligible)Predominantly biliary/fecal elimination; no renal dose adjustment needed; steady state reached rapidly; twice-daily dosing appropriate given 10–15 h half-life
SE

Side Effects

≥10% Very Common (IPF Studies 1–3)
Adverse EffectIncidence (IPF / SSc-ILD)Clinical Note
Diarrhea62% / 76% vs 18% / 32% placeboMost common AE; usually mild-moderate; occurs in first 3 months; treat early with loperamide and hydration; led to dose reduction in 11–22% and discontinuation in 5–7%
Nausea24% / 32% vs 7% / 14% placeboOften accompanies diarrhea; anti-emetics may help; led to discontinuation in 2%
Abdominal pain15% / 18% vs 6% / 11% placeboIncludes upper and lower abdominal pain and GI pain
Liver enzyme elevation14% / 13% vs 3% / 3% placeboALT/AST ≥3× ULN in 4.9% (SSc-ILD); majority <5× ULN; reversible with dose modification; monitor per protocol
Vomiting12% / 25% vs 3% / 10% placeboMore common in SSc-ILD; may compromise oral contraceptive efficacy
Decreased appetite11% / 9% vs 5% / 4% placeboContributes to weight loss; monitor nutritional status
Weight decreased10% / 12% vs 3% / 4% placeboMonitor weight regularly; consider nutritional support
5–10% Common
Adverse EffectIncidence (IPF / SSc-ILD)Clinical Note
Headache8% / 9% vs 5% / 8% placeboGenerally mild; marginally above placebo
Hypertension5% / 5% vs 4% / 2% placeboIncludes hypertensive crisis (rare); VEGFR inhibition is the mechanism; monitor blood pressure
Fatigue— / 11% vs — / 7% placeboSSc-ILD specific; may be disease-related
Pyrexia— / 6% vs — / 5% placeboSSc-ILD specific
Back pain / Dizziness— / 6% each vs — / 4% each placeboSSc-ILD specific; marginally above placebo
Serious Serious (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Drug-induced liver injury (DILI)ALT/AST ≥3× ULN: ~5%; fatal cases reported postmarketingMajority within first 3 monthsMonitor LFTs at baseline, regularly × 3 months, then periodically; >5× ULN or >3× ULN with symptoms: discontinue; 3–5× ULN without symptoms: interrupt or reduce to 100 mg BID
Arterial thromboembolic events (MI, stroke)2.5% vs <1% placebo (IPF); MI 1.5% vs <1%Any time during treatmentUse caution in patients with coronary artery disease or high CV risk; consider treatment interruption for signs of acute MI
Bleeding events10–11% vs 7–13% placebo; fatal cases postmarketingAny timeUse only if benefit outweighs risk in patients with known bleeding risk; monitor patients on anticoagulants closely
Gastrointestinal perforation<1% (IPF); fatal cases postmarketingVariableDiscontinue nintedanib; use with caution in patients with recent abdominal surgery, diverticular disease, or concurrent corticosteroids/NSAIDs
Embryo-fetal toxicityTeratogenic in animals at <MRHDThroughout pregnancyVerify pregnancy status before treatment; use highly effective contraception during and for ≥3 months after last dose; if vomiting/diarrhea may reduce OC absorption, use alternative contraception
Nephrotic-range proteinuriaRare (postmarketing)VariableConsider treatment interruption for new or worsening proteinuria; improvement observed after discontinuation in some cases
Discontinuation Discontinuation Rates
IPF (Studies 1–3)
21% vs 15% placebo
Top reasons: Diarrhea (5%), nausea (2%), decreased appetite (2%). Dose reduction: 16% vs 1% (diarrhea 11%).
SSc-ILD (Study 4 / SENSCIS)
16% vs 9% placebo
Top reasons: Diarrhea (7%), nausea (2%), vomiting (1%). Dose reduction: 34% vs 4% (diarrhea 22%).
Managing Diarrhea — The Dominant Tolerability Challenge

Diarrhea affects the majority of patients (62–76%) and is the primary driver of dose reduction (up to 22%) and discontinuation (up to 7%). Proactive management is critical: counsel patients before starting therapy that diarrhea is expected, provide loperamide for early use, advise adequate hydration, take nintedanib with food, and consider dose reduction to 100 mg BID before resorting to discontinuation. Most diarrhea events are mild to moderate, peak in the first 3 months, and do not recur after the initial period.

Int

Drug Interactions

Nintedanib is primarily a substrate of P-glycoprotein (P-gp) and, to a minor extent, CYP3A4. Its metabolism is predominantly via ester hydrolysis (not CYP), so traditional CYP-mediated drug interactions are minimal. Nintedanib does not inhibit or induce CYP enzymes at therapeutic concentrations. The key interaction pathway is P-gp transport, which governs intestinal absorption and exposure levels.

Major P-gp and CYP3A4 Inducers (rifampicin, carbamazepine, phenytoin, St. John’s Wort)
MechanismIncreased P-gp efflux and CYP3A4 metabolism reduce nintedanib absorption and exposure
EffectRifampicin decreased nintedanib exposure by 50%
ManagementAvoid co-administration; may substantially reduce nintedanib efficacy
FDA PI
Moderate P-gp and CYP3A4 Inhibitors (ketoconazole, erythromycin)
MechanismReduced P-gp efflux increases nintedanib absorption and systemic exposure
EffectKetoconazole increased nintedanib exposure by 60%
ManagementMonitor closely for nintedanib tolerability (especially diarrhea and liver enzymes); may require dose reduction or interruption
FDA PI
Moderate Anticoagulants (warfarin, DOACs, heparin)
MechanismNintedanib inhibits VEGFR, which may increase bleeding risk independently
EffectAdditive bleeding risk; not a PK interaction
ManagementMonitor closely for bleeding; adjust anticoagulation therapy as necessary
FDA PI
Minor Pirfenidone
MechanismNo pharmacokinetic interaction between nintedanib and pirfenidone
EffectExposure of neither agent is altered; GI side effects may be additive
ManagementNo dose adjustment needed; monitor for increased GI adverse events (70% vs 53% in combination study)
FDA PI
Minor Bosentan
MechanismNo clinically significant effect on nintedanib PK
EffectCan be co-administered in SSc-ILD patients on bosentan for PAH
ManagementNo dose adjustment
FDA PI
Minor Oral Contraceptives (ethinylestradiol/levonorgestrel)
MechanismNintedanib does not alter OC exposure
EffectNo PK interaction; however, vomiting/diarrhea may reduce OC absorption
ManagementIf vomiting/diarrhea occurs, advise alternative highly effective contraception
FDA PI
Mon

Monitoring

  • Liver Function Tests Baseline; regular × 3 months; then periodically
    Routine     ALT, AST, and bilirubin prior to initiation, at regular intervals during the first 3 months, and periodically thereafter. Majority of hepatic events occur in the first 3 months. Higher risk in low body weight (<65 kg), Asian, female, and elderly patients. Discontinue if >3× ULN with symptoms or >5× ULN.
  • Pregnancy Testing Before initiation; during treatment as appropriate
    Routine     Verify pregnancy status in females of reproductive potential before starting and during therapy. Nintedanib is teratogenic. Ensure highly effective contraception during and for at least 3 months after last dose.
  • GI Tolerability Each visit; proactively in first 3 months
    Routine     Assess for diarrhea (62–76%), nausea (24–32%), vomiting (12–25%), and abdominal pain (15–18%). Initiate loperamide and hydration early. Dose reduce to 100 mg BID if needed. Discontinue if intolerable at 100 mg BID.
  • Blood Pressure Baseline; each visit
    Routine     Hypertension reported in 5% vs 2–4% placebo (VEGFR inhibition mechanism). Monitor and manage with standard anti-hypertensives.
  • Cardiovascular Risk Baseline assessment
    Trigger-based     Arterial thromboembolic events including MI reported in 2.5% vs <1% in IPF trials. Use caution in patients with known CAD. Monitor for signs of acute ischemia.
  • Pulmonary Function Q3–6 months
    Routine     Serial FVC measurements to assess treatment effect. Nintedanib slows FVC decline but does not improve or stabilize FVC in all patients. Consider continuing treatment if decline rate has slowed relative to pre-treatment trajectory.
  • Weight Each visit
    Routine     Weight loss reported in 10–12% vs 3–4% placebo. Combined with decreased appetite (9–11%) and GI symptoms, nutritional status should be monitored, especially in underweight patients.
CI

Contraindications & Cautions

Absolute Contraindications

  • None formally listed in the FDA PI. However, moderate-to-severe hepatic impairment is effectively a contraindication as the PI states treatment is “not recommended” in Child-Pugh B/C patients.

Relative Contraindications (Specialist Input Recommended)

  • Moderate or severe hepatic impairment (Child-Pugh B or C) — nintedanib is predominantly eliminated via biliary/fecal excretion (>90%). Exposure is increased in hepatic impairment. Treatment is not recommended.
  • Pregnancy — nintedanib is teratogenic (embryo-fetal deaths and structural abnormalities in animals at <MRHD in rats). Can cause fetal harm. Females of reproductive potential must use highly effective contraception during and for ≥3 months after the last dose.
  • Known risk of GI perforation — recent abdominal surgery, diverticular disease, concurrent corticosteroids/NSAIDs. Use only if benefit outweighs risk.

Use with Caution

  • Mild hepatic impairment (Child-Pugh A) — reduce dose to 100 mg BID. Monitor closely; consider interruption or discontinuation for adverse reactions.
  • Higher cardiovascular risk (known CAD) — arterial thromboembolic events (MI 1.5%) were more frequent with nintedanib in IPF trials. Consider treatment interruption for signs of acute myocardial ischemia.
  • Patients on full anticoagulation — VEGFR inhibition may increase bleeding risk. Monitor closely and adjust anticoagulation as necessary.
  • Lactation — not recommended; nintedanib and metabolites present in rat milk at concentrations similar to plasma.
  • Smokers — smoking decreases nintedanib exposure, which may alter efficacy. Encourage smoking cessation before and during treatment.
  • Low body weight (<65 kg), Asian, and female patients — higher risk of liver enzyme elevations. Monitor LFTs more closely.
FDA Safety Advisory Embryo-Fetal Toxicity and Drug-Induced Liver Injury

Nintedanib does not carry a formal FDA Boxed Warning. However, the PI prominently warns about embryo-fetal toxicity (teratogenic in animals at sub-MRHD exposures; pregnancy must be excluded before treatment and highly effective contraception used) and drug-induced liver injury (DILI with fatal outcomes reported in the postmarketing period; LFT monitoring is mandatory). Clinicians should verify pregnancy status and liver function before every initiation of therapy.

Pt

Patient Counselling

Purpose of Therapy

Nintedanib is an oral anti-fibrotic medication that works by blocking the growth factors that drive scar tissue formation in the lungs. It slows the rate at which your lung function declines but does not cure the disease or reverse existing scarring. You will need regular blood tests and lung function assessments throughout treatment.

How to Take

Take one capsule twice daily, approximately 12 hours apart, with food. Swallow the capsule whole with liquid. Do not chew, crush, or open the capsule as it has a bitter taste. If you miss a dose, take the next dose at your regular scheduled time; do not double the dose. Do not exceed 300 mg per day.

Diarrhea, Nausea, and Vomiting
Tell patientDiarrhea is very common (affects most patients) and usually starts in the first few weeks to months. It is typically mild to moderate. Always take nintedanib with food. Your doctor may provide you with loperamide (Imodium) to take at the first sign of diarrhea. Stay well hydrated. Nausea and vomiting can also occur; anti-nausea medications may help.
Call prescriberIf diarrhea is severe, persistent, or bloody; if you cannot eat or drink due to nausea/vomiting; if you notice significant weight loss; or if you are taking a birth control pill and experience vomiting or diarrhea (pill may not work as well).
Liver Problems
Tell patientNintedanib can affect your liver. You will need blood tests before starting and regularly during the first 3 months, then periodically after that. Most liver enzyme changes are mild and reversible with dose adjustment.
Call prescriberImmediately if you develop fatigue, loss of appetite, pain in the upper right abdomen, dark urine, or yellowing of the skin or eyes (jaundice).
Pregnancy Prevention
Tell patientNintedanib can cause serious harm to an unborn baby. You must not become pregnant while taking this medicine. Use highly effective birth control while taking nintedanib and for at least 3 months after your last dose. If you are taking a birth control pill and have vomiting or diarrhea, the pill may not be absorbed properly, so use a backup method of contraception.
Call prescriberImmediately if you think you may be pregnant or if your period is late.
Heart Attack, Stroke, and Bleeding Risk
Tell patientNintedanib may slightly increase the risk of blood clots in arteries (heart attack or stroke) and may increase bleeding risk. Tell your doctor if you have a history of heart disease or take blood-thinning medications.
Call prescriberImmediately if you experience chest pain, sudden numbness or weakness, trouble speaking, sudden severe headache, unusual bleeding or bruising, or coughing up blood.
Smoking
Tell patientSmoking lowers the amount of nintedanib in your blood, which may make it work less well. You are strongly encouraged to stop smoking before starting this medication and to avoid smoking during treatment.
Call prescriberIf you need help with smoking cessation; your prescriber can provide resources and support.
Ref

Sources

Regulatory (PI / SmPC)
  1. Ofev (nintedanib capsules), for oral use. Full Prescribing Information. Boehringer Ingelheim Pharmaceuticals, Inc. Revised 06/2024. https://www.accessdata.fda.gov/drugsatfda_docs/label/2024/205832s027lbl.pdf Primary source for all dosing, indications, adverse reactions, warnings, PK data, drug interactions, and clinical trial summaries.
Key Clinical Trials
  1. Richeldi L, du Bois RM, Raghu G, et al. Efficacy and safety of nintedanib in idiopathic pulmonary fibrosis. N Engl J Med. 2014;370(22):2071-2082. doi:10.1056/NEJMoa1402584 INPULSIS-1 and INPULSIS-2 pivotal phase 3 trials for IPF; primary source for IPF adverse reaction rates (Table 1) and FVC decline data.
  2. Distler O, Highland KB, Gahlemann M, et al. Nintedanib for systemic sclerosis-associated interstitial lung disease. N Engl J Med. 2019;380(26):2518-2528. doi:10.1056/NEJMoa1903076 SENSCIS trial; established nintedanib efficacy in SSc-ILD; source for SSc-ILD-specific adverse reaction rates (Table 2).
  3. Flaherty KR, Wells AU, Cottin V, et al. Nintedanib in progressive fibrosing interstitial lung diseases. N Engl J Med. 2019;381(18):1718-1727. doi:10.1056/NEJMoa1908681 INBUILD trial; extended nintedanib approval to progressive fibrosing ILDs beyond IPF; included HP, autoimmune ILDs, and unclassifiable ILD.
  4. Richeldi L, Costabel U, Selman M, et al. Efficacy of a tyrosine kinase inhibitor in idiopathic pulmonary fibrosis. N Engl J Med. 2011;365(12):1079-1087. doi:10.1056/NEJMoa1103690 TOMORROW phase 2 dose-finding trial for IPF; established the 150 mg BID dose and proof of concept.
  5. Vancheri C, Kreuter M, Richeldi L, et al. Nintedanib with add-on pirfenidone in IPF: results of the INJOURNEY trial. Am J Respir Crit Care Med. 2018;197(3):356-363. doi:10.1164/rccm.201706-1301OC INJOURNEY open-label trial assessing nintedanib + pirfenidone combination; source for GI tolerability data of dual anti-fibrotic therapy.
Guidelines
  1. Raghu G, Remy-Jardin M, Richeldi L, et al. Idiopathic pulmonary fibrosis (an update) and progressive pulmonary fibrosis in adults: an official ATS/ERS/JRS/ALAT clinical practice guideline. Am J Respir Crit Care Med. 2022;205(9):e18-e47. doi:10.1164/rccm.202202-0399ST Joint ATS/ERS/JRS/ALAT guideline providing conditional recommendation for nintedanib in IPF and PPF.
Mechanistic / Basic Science
  1. Wollin L, Wex E, Pautsch A, et al. Mode of action of nintedanib in the treatment of idiopathic pulmonary fibrosis. Eur Respir J. 2015;45(5):1434-1445. doi:10.1183/09031936.00174914 Comprehensive preclinical review of nintedanib’s multi-kinase inhibition, anti-fibrotic and anti-angiogenic effects in lung fibrosis models.
  2. Roth GJ, Binder R, Colbatzky F, et al. Nintedanib: from discovery to the clinic. J Med Chem. 2015;58(3):1053-1063. doi:10.1021/jm501562a Drug discovery story of nintedanib covering SAR, preclinical pharmacology, and early PK characterization.
Pharmacokinetics / Special Populations
  1. Wind S, Schmid U, Freiwald M, et al. Clinical pharmacokinetics and pharmacodynamics of nintedanib. Clin Pharmacokinet. 2019;58(9):1131-1147. doi:10.1007/s40262-019-00766-0 Comprehensive PK review covering bioavailability (~5%), P-gp substrate status, ester hydrolysis metabolism, and covariate effects (weight, age, smoking, ethnicity).
  2. Stopfer P, Rathgen K, Bischoff D, et al. Pharmacokinetic properties of nintedanib in healthy volunteers and patients with advanced cancer. J Clin Pharmacol. 2016;56(11):1387-1394. doi:10.1002/jcph.752 Phase 1 PK study establishing absolute bioavailability (~5%), Vss (~1050 L), clearance, and half-life in healthy volunteers and cancer patients.