My Dashboard
Courses
Articles Evidence Reviews Practice Updates Cases News Presentations
About Us
My Dashboard
Drug Monograph

Ubrelvy (Ubrogepant)

ubrogepant
Small-molecule CGRP receptor antagonist (gepant) · Oral · Acute migraine therapy
Pharmacokinetic Profile
Half-Life
~5–7 h
Metabolism
CYP3A4 (primary)
Protein Binding
87% (in vitro)
Tmax
~1.5 h (fasted)
Volume of Distribution
~350 L (V/F)
Excretion
42% feces, 6% urine (unchanged)
Clinical Information
Drug Class
CGRP receptor antagonist (gepant)
Available Doses
50 mg, 100 mg tablets
Route
Oral
Renal Adjustment
Severe (CrCl 15–29): 50 mg; ESRD: avoid
Hepatic Adjustment
Severe (Child-Pugh C): 50 mg
Pregnancy
No human data; animal fetal toxicity
Lactation
Excreted in low amounts (RID ~0.15%)
Schedule / Legal Status
Rx only, non-controlled
Generic Available
No (US, 2026)
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Acute treatment of migraine, with or without auraAdults (≥18 years)Monotherapy (acute, as-needed)FDA Approved

Ubrogepant is approved by the U.S. FDA only; it does not currently hold marketing authorisation in the European Union. The indication is narrow: acute, abortive treatment of an active migraine attack in adults. The label explicitly states that ubrogepant is not indicated for migraine prevention, and that the safety of treating more than 8 migraines in a 30-day period has not been established.

The principal clinical role is as an oral, non-vasoconstrictive option for adults requiring acute migraine therapy. It is particularly useful when triptans are ineffective, poorly tolerated, or contraindicated — most notably in patients with established or high-risk cardiovascular disease. The 2021 American Headache Society consensus statement positions gepants as appropriate acute therapy for patients with cardiovascular contraindications to triptans, and as a reasonable choice when triptans fail or are not tolerated.

Off-Label and Emerging Uses

Treatment during the migraine prodrome: The phase 3 PRODROME trial (Dodick et al., Lancet 2023) showed that ubrogepant 100 mg taken during prodromal symptoms (1–6 hours before headache) reduced the development of moderate-to-severe headache compared with placebo. While the FDA-approved indication remains acute treatment of an established migraine, prodromal dosing is supported by RCT-level evidence — quality moderate.

Use in patients on CGRP-targeted monoclonal antibody preventives: No clinically significant pharmacokinetic interaction was demonstrated between ubrogepant and erenumab or galcanezumab in dedicated DDI studies; combination is increasingly used in clinical practice for breakthrough attacks — quality moderate.

Dose

Dosing

Ubrogepant is taken at the onset of a migraine attack and may be repeated once after at least 2 hours if the headache persists or recurs. The maximum dose in any 24-hour period is 200 mg in healthy adults. Both available strengths (50 mg and 100 mg) are clinically active; the higher strength offers a modest numeric advantage in pivotal trials.

Clinical ScenarioStarting DoseRepeat Dose (≥2 h)Maximum / 24 hNotes
Acute migraine — otherwise healthy adult, no dose-modifying conditions50 mg or 100 mg PO50 mg or 100 mg PO200 mgTake at onset of attack; with or without food
Safety not established for >8 migraines/30 days
Migraine with prior triptan failure or cardiovascular contraindication to triptans50 mg or 100 mg PO50 mg or 100 mg PO200 mgPreferred over triptans in coronary artery disease, prior MI, prior stroke
No vasoconstrictive activity
Co-administration with moderate CYP3A4 inhibitor (e.g. verapamil, diltiazem, fluconazole, ciprofloxacin, fluvoxamine, cyclosporine, grapefruit juice)50 mg POAvoid within 24 h50 mgVerapamil increases AUC ~3.5-fold
Single 50 mg dose only in 24 h
Co-administration with weak CYP3A4 inhibitor50 mg PO50 mg PO100 mgPredicted ≤2-fold rise in exposure
Co-administration with strong CYP3A4 inhibitor (e.g. ketoconazole, itraconazole, clarithromycin, ritonavir, cobicistat)ContraindicatedKetoconazole increases AUC ~9.7-fold
Use alternative acute migraine therapy
Co-administration with weak or moderate CYP3A4 inducer (e.g. modafinil, efavirenz, etravirine)100 mg PO100 mg PO200 mgUse higher strength to offset induction
No dedicated DDI study; based on conservative prediction of ~50% reduction
Co-administration with strong CYP3A4 inducer (e.g. rifampin, phenytoin, carbamazepine, phenobarbital, St. John’s wort)AvoidRifampin reduced AUC by 80%
Loss of efficacy expected
Co-administration with BCRP and/or P-gp only inhibitor (e.g. quinidine, carvedilol, eltrombopag, curcumin)50 mg PO50 mg PO100 mgPredicted ≤2-fold rise in exposure

Dose Adjustment for Renal Impairment

Renal FunctionStarting DoseRepeat DoseMaximum / 24 hNotes
Mild–moderate (CrCl 30–89 mL/min)50 or 100 mg50 or 100 mg200 mgNo adjustment
Severe (CrCl 15–29 mL/min)50 mg50 mg100 mgUse 50 mg strength only
End-stage renal disease (CrCl <15 mL/min)AvoidPharmacokinetics not characterised

Dose Adjustment for Hepatic Impairment

Hepatic FunctionStarting DoseRepeat DoseMaximum / 24 hNotes
Mild (Child-Pugh A)50 or 100 mg50 or 100 mg200 mgAUC increased by ~7%; no adjustment
Moderate (Child-Pugh B)50 or 100 mg50 or 100 mg200 mgAUC increased by ~50%; no formal adjustment
Severe (Child-Pugh C)50 mg50 mg100 mgAUC increased by ~115%; use 50 mg strength only

Special Populations

  • Pediatric (<18 years): Safety and effectiveness have not been established. Not recommended.
  • Geriatric (≥65 years): No clinically significant pharmacokinetic differences observed. Trial data in this age group are limited; cautious dose selection (start at 50 mg) is reasonable.
  • Pregnancy: No adequate human data. Animal studies showed embryofetal mortality (rabbits) and decreased offspring body weight (rats) at doses associated with maternal toxicity. AbbVie maintains a pregnancy exposure registry: 1-833-277-0206.
  • Lactation: A study in 12 healthy adult lactating females found ubrogepant excreted in low amounts in breast milk (estimated relative infant dose ~0.15%; milk-to-plasma ratio 0.23). Effects on the breastfed infant are not characterised — weigh maternal need against potential exposure.
Clinical Pearl — Dosing Window and the 8-per-Month Limit

Patients should be coached to take ubrogepant at the earliest sign of a definite migraine attack — not at every minor head sensation. If headache persists or returns after 2 hours, a single repeat dose is allowed within the same 24-hour window (subject to interaction caps). The 24-hour ceiling is 200 mg in healthy adults. The label explicitly states that the safety of treating more than 8 migraines in a 30-day period has not been established — patients exceeding this threshold should be evaluated for preventive therapy.

Medication-Overuse Headache Caution

Although gepants do not appear to drive medication-overuse headache (MOH) to the degree seen with triptans or combination analgesics, the FDA labelling cap of 8 treatment days per month is a practical guide for ubrogepant. Patients exceeding this threshold — or using ≥10–15 days/month across all acute agents combined — should be considered for a preventive strategy.

PK

Pharmacology

Mechanism of Action

Calcitonin gene-related peptide (CGRP) is a vasodilatory neuropeptide released from trigeminal sensory neurons during a migraine attack and a key mediator of migraine pain through pro-nociceptive transmission within the trigeminovascular system. Ubrogepant is a small-molecule, orally bioavailable, competitive antagonist at the human CGRP receptor (a heterodimer of the calcitonin receptor-like receptor and RAMP1). Preclinical characterisation by Moore and colleagues demonstrated high binding affinity for the human CGRP receptor (Ki ~0.07 nM) and high functional potency (IC50 ~0.08 nM in CGRP-stimulated cAMP assays), with selective antagonism over related calcitonin family receptors. By blocking endogenous CGRP from binding its receptor, ubrogepant interrupts trigeminovascular pain signalling without producing arterial vasoconstriction — the mechanistic feature that supports its use in patients with cardiovascular disease.

At doses up to twice the maximum recommended daily dose, ubrogepant does not prolong the QT interval to a clinically relevant extent.

ADME Profile

ParameterValueClinical Implication
AbsorptionTmax ~1.5 h; high-fat meal delays Tmax by 2 h and reduces Cmax 22% with no change in AUC; dose-proportional within recommended rangeRapid onset; food does not require dose timing changes — patients can take with or without food
DistributionApparent V/F ~350 L; plasma protein binding 87% in vitroWide tissue distribution; protein-binding interactions are not clinically significant
MetabolismPrimarily hepatic via CYP3A4; two glucuronide conjugate metabolites are major circulating species but ~6000× less potent at the CGRP receptor; substrate of P-gp and BCRPCYP3A4 inhibitors and inducers dominate the interaction profile; transporter inhibitors add a secondary layer requiring dose adjustment
Eliminationt½ ~5–7 h; mean apparent oral clearance ~87 L/h; primarily biliary/fecal — 42% of dose recovered in feces and 6% in urine as unchanged drugRenal route is minor — no dose adjustment for mild–moderate renal impairment; ESRD avoided due to absent data

Drug interaction conclusions from clinical PK studies: No clinically significant pharmacokinetic interactions were observed when ubrogepant was co-administered with sumatriptan, oral contraceptives (norgestimate/ethinyl estradiol), acetaminophen, naproxen, esomeprazole, or the CGRP-targeted monoclonal antibodies erenumab and galcanezumab, or with atogepant.

SE

Side Effects

Ubrogepant has a notably mild adverse-effect profile in the pivotal acute treatment trials (Studies 1 and 2; ACHIEVE I and ACHIEVE II), with most events being low-grade and transient. The most common adverse reactions occurring at ≥2% and at a frequency greater than placebo were nausea and somnolence. Compared with triptans, the absence of chest tightness, paraesthesia, and vasoconstrictive symptoms is notable.

≥10% Very Common Adverse Effects
Adverse EffectIncidenceClinical Note
No adverse effect occurred at ≥10% incidence in placebo-controlled trials. Ubrogepant has a uniformly low-frequency tolerability profile.
1–10% Common Adverse Effects (FDA PI, Studies 1 & 2)
Adverse Effect50 mg100 mgPlaceboClinical Note
Nausea2%4%2%Usually mild; can be migraine-related rather than drug-related
Somnolence (incl. sedation, fatigue)2%3%1%Counsel against driving until individual response is known after the first dose
Dry mouth<1%2%1%Symptomatic and self-limited
N: placebo 984; 50 mg 954; 100 mg 485. Threshold for inclusion: ≥2% and greater than placebo.
Serious Serious / Labelled Warning-Level Adverse Effects
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Hypersensitivity reactions (anaphylaxis, dyspnoea, facial or throat oedema, rash, urticaria, pruritus)Rare
post-marketing
Minutes, hours, or days after administrationDiscontinue permanently; emergency care if airway, dyspnoea, or anaphylaxis; do not re-challenge
Hypertension (new-onset or worsening of pre-existing)Frequency not established
labelled warning 5.2
Variable; can be acute or insidious with repeated useMonitor BP; consider discontinuation if alternative aetiology excluded or BP inadequately controlled
Raynaud’s phenomenon (new-onset or worsening of pre-existing)Rare
post-marketing; class effect of CGRP antagonists, labelled warning 5.3
Median ~1.5 days after dosing in reported casesDiscontinue ubrogepant; evaluate if symptoms do not resolve; some reported cases included hospitalisation or disability
Discontinuation Treatment Discontinuation Rates
Adults (Long-term safety, 52-week extension)
2.5% over 1 year
Most common reason: Nausea. 813 patients dosed intermittently for up to 1 year; 421 exposed for ≥6 months and 364 for ≥1 year.
Pediatric (<18 years)
N/A not approved
Safety and efficacy in pediatric migraine have not been established; no labelled pediatric data on discontinuation.
Reason for DiscontinuationFrequencyContext
Adverse event — any (1-year safety study)2.5%Pooled 50 mg and 100 mg long-term safety population
NauseaMost commonLeading cause of discontinuation in long-term use
Hypersensitivity reactionRareMandatory permanent discontinuation if confirmed
Raynaud’s phenomenonRarePer labelled warning, discontinue if signs/symptoms develop
Management Tip — Distinguishing Drug Effect from Migraine

Nausea and somnolence are also core migraine-associated symptoms — clinical attribution between drug and disease is often difficult. If a patient reports new nausea after dosing, assess whether it preceded or followed the headache, whether it improves alongside headache resolution, and whether prior attacks (untreated) were similarly nauseating. Genuine drug-induced nausea is mild, low-frequency (4% on 100 mg vs 2% on placebo), and rarely treatment-limiting.

Int

Drug Interactions

Ubrogepant’s interaction profile is dominated by CYP3A4. The drug is also a substrate of P-glycoprotein (P-gp) and BCRP. Strong CYP3A4 inhibition is contraindicated; moderate inhibition mandates a 50 mg cap with no repeat within 24 h. Strong CYP3A4 induction is to be avoided as efficacy is markedly reduced; weak/moderate inducers permit use with a switch to the 100 mg strength. Patients should also be advised that grapefruit juice is a relevant moderate CYP3A4 inhibitor.

Major Ketoconazole / Itraconazole
MechanismStrong CYP3A4 inhibition
EffectKetoconazole increases AUC ~9.7-fold and Cmax ~5.3-fold
ManagementContraindicated; use alternative acute migraine therapy
FDA PI
Major Clarithromycin
MechanismStrong CYP3A4 inhibition
EffectMarked rise in plasma ubrogepant (extrapolated from ketoconazole data)
ManagementContraindicated; substitute azithromycin if a macrolide is needed
FDA PI
Major Ritonavir / Cobicistat-boosted antiretrovirals
MechanismStrong CYP3A4 inhibition
EffectSubstantial AUC increase
ManagementContraindicated; choose lasmiditan or NSAID-based acute therapy
FDA PI
Major Rifampin
MechanismStrong CYP3A4 induction
Effect80% reduction in ubrogepant exposure → loss of efficacy
ManagementAvoid; treat acute migraine with a non-CYP3A4-dependent agent
FDA PI · Jakate 2021
Major Phenytoin / Carbamazepine / Phenobarbital
MechanismStrong CYP3A4 induction
EffectReduced efficacy; loss of response expected
ManagementAvoid; consider lasmiditan, triptans (if no CV contraindication), or NSAIDs
FDA PI
Major St. John’s wort (Hypericum)
MechanismStrong CYP3A4 induction
EffectReduced ubrogepant exposure and efficacy
ManagementAvoid; counsel patients explicitly — herbal product use is often unreported
FDA PI
Moderate Verapamil / Diltiazem
MechanismModerate CYP3A4 inhibition (verapamil also inhibits P-gp)
EffectVerapamil increases AUC ~3.5-fold and Cmax ~2.8-fold
ManagementCap at 50 mg single dose; avoid second dose within 24 h
FDA PI · Jakate 2021
Moderate Fluconazole / Fluvoxamine / Ciprofloxacin
MechanismModerate CYP3A4 inhibition
EffectIncreased ubrogepant exposure
ManagementCap at 50 mg single dose; avoid second dose within 24 h during the antibiotic course
FDA PI
Moderate Cyclosporine
MechanismModerate CYP3A4 inhibition + P-gp/BCRP inhibition
EffectIncreased ubrogepant exposure
ManagementCap at 50 mg single dose; avoid second dose within 24 h
FDA PI
Moderate Grapefruit / grapefruit juice
MechanismModerate CYP3A4 inhibition (intestinal)
EffectIncreased ubrogepant exposure
ManagementTreat as moderate inhibitor on days of consumption: 50 mg dose only, no repeat in 24 h
FDA PI
Moderate Quinidine / Carvedilol / Eltrombopag / Curcumin
MechanismP-gp and/or BCRP inhibition (no CYP3A4 effect)
EffectPredicted ≤2-fold increase in ubrogepant exposure
Management50 mg starting and repeat dose; max 100 mg / 24 h
FDA PI
Moderate Modafinil / Efavirenz / Etravirine
MechanismWeak–moderate CYP3A4 induction
EffectPredicted ~50% reduction in exposure
ManagementUse 100 mg starting and repeat dose to offset induction
FDA PI (conservative prediction)
No PK Effect Sumatriptan and other triptans
MechanismNo PK interaction; ubrogepant has no vasoactivity
EffectNo additive vasoconstrictive risk
ManagementSequential same-attack use is permitted; dose adjustments not required
FDA PI
No PK Effect Erenumab / Galcanezumab / Atogepant
MechanismNo PK interaction (different elimination pathways for mAbs)
EffectCombination commonly used: prevention + acute breakthrough
ManagementNo dose change needed; supported by dedicated DDI studies
Jakate 2021 · FDA PI
No PK Effect Oral contraceptives, acetaminophen, naproxen, esomeprazole
MechanismNo PK interaction in dedicated studies
EffectNo effect on either drug exposure
ManagementNo dose adjustment; combine freely as clinically indicated
FDA PI
Practical Screening Question

Before any new ubrogepant prescription, screen explicitly for: (1) “Are you taking any antifungal pills?” — captures azoles; (2) “Any HIV or hepatitis C medicines?” — captures protease inhibitors and cobicistat; (3) “Any antiseizure medicines?” — captures carbamazepine, phenytoin, phenobarbital; (4) “Any herbal supplements, especially St. John’s wort?”; (5) “Do you drink grapefruit juice?” — easily missed but a labelled moderate CYP3A4 inhibitor.

Mon

Monitoring

Ubrogepant requires minimal laboratory monitoring. The most important post-marketing additions to the label — hypertension and Raynaud’s phenomenon (both class-effect warnings) — make blood pressure surveillance and digital symptom screening clinically relevant additions to routine follow-up.

  • Blood pressure Baseline, then 2–4 weeks after initiation; then periodically
    Routine     Monitor for new-onset or worsening hypertension. Consider discontinuation if BP is inadequately controlled and an alternative aetiology is excluded.
  • Digital / extremity symptoms (Raynaud’s) Every visit and on patient report
    Trigger-based     Ask about colour change, numbness, coolness, or pain in fingers/toes. Onset has been reported a median of ~1.5 days after dosing in post-marketing cases. Discontinue if symptoms develop.
  • Migraine days / month Every visit (e.g. 3-monthly)
    Routine     Track via headache diary or app. Rising frequency is the cue to consider preventive therapy rather than escalating acute use.
  • Acute treatment days / month Every visit
    Routine     Sum across all acute agents. Per FDA labelling, safety of treating >8 migraines/30 days has not been established — use this as an explicit threshold.
  • Treatment response (2-h pain freedom, MBS freedom) After 2–3 attacks treated
    Routine     Reasonable trial period before declaring failure. If 2/3 or 3/3 attacks fail, step from 50 to 100 mg or switch to another class.
  • Renal function (CrCl) Recheck if status changes
    Trigger-based     No routine monitoring in stable normal renal function. Reassess if CrCl drops below 30 mL/min — switch to 50 mg cap; avoid use if CrCl <15 mL/min.
  • Hepatic function (LFTs) On symptoms; consider baseline in known liver disease
    Trigger-based     Routine LFT monitoring is not required at acute treatment doses; published healthy-volunteer data have not shown clinically meaningful ALT elevation.
  • Concomitant medication review Every visit and at each new prescription
    Routine     Specifically screen for new strong/moderate CYP3A4 inhibitors and inducers, P-gp/BCRP inhibitors, and grapefruit juice intake.
Key Clinical Action

The single most useful “monitoring” metric for ubrogepant is treatment days per month. The FDA-labelled threshold is >8 migraines treated in 30 days; beyond this, safety has not been established. A patient repeatedly hitting that ceiling — across any combination of acute agents — should be assessed for migraine prevention rather than offered more acute therapy. Combine BP monitoring at the 2–4-week post-initiation visit with the medication-days conversation: it captures both the new labelled hypertension warning and the medication-overuse risk in one visit.

CI

Contraindications & Cautions

Absolute Contraindications

  • Concomitant use of a strong CYP3A4 inhibitor — including ketoconazole, itraconazole, voriconazole, posaconazole, clarithromycin, ritonavir-boosted regimens, and cobicistat. Ketoconazole co-administration produces a ~9.7-fold increase in AUC.
  • History of serious hypersensitivity to ubrogepant or any component of Ubrelvy — including prior anaphylaxis, dyspnoea, facial or throat oedema, severe cutaneous reaction, or angioedema temporally linked to a prior dose.

Relative Contraindications (Specialist Input Recommended)

  • End-stage renal disease (CrCl <15 mL/min) or dialysis dependence — the FDA label advises avoiding use; no pharmacokinetic data are available in this population.
  • Severe hepatic impairment (Child-Pugh C) — ubrogepant exposure is approximately 115% higher than in normal hepatic function; use only at the 50 mg dose with no second dose >50 mg in 24 h.
  • Pregnancy — no adequate human data; animal studies showed embryofetal mortality (rabbits) and decreased offspring body weight (rats) at maternally-toxic exposures. Use only if alternatives are unsuitable; encourage enrolment in the AbbVie pregnancy registry (1-833-277-0206).
  • Concurrent strong CYP3A4 inducer — efficacy is markedly reduced (rifampin reduces AUC by 80%); avoid use and select an alternative acute therapy.
  • History of Raynaud’s phenomenon with ischaemic complications (e.g. prior digital ulcers, tissue loss) — case reports of debilitating Raynaud’s with CGRP antagonists indicate caution; specialist input is appropriate.
  • Suspected medication-overuse headache — co-manage with a headache specialist; adding more acute therapy will not resolve the underlying pattern.

Use with Caution

  • Severe renal impairment (CrCl 15–29 mL/min) — cap at 50 mg starting dose, 50 mg repeat, and 100 mg/24 h.
  • Concomitant moderate CYP3A4 inhibitor — cap at 50 mg single dose; no repeat dose within 24 h. Includes verapamil, diltiazem, fluconazole, fluvoxamine, ciprofloxacin, cyclosporine, and grapefruit juice.
  • Concomitant P-gp / BCRP only inhibitor (e.g. quinidine, carvedilol, eltrombopag, curcumin) — cap at 50 mg starting dose and 50 mg repeat dose.
  • Pre-existing hypertension — monitor blood pressure at baseline and at the 2–4-week follow-up; adjust antihypertensive therapy or discontinue ubrogepant if blood pressure becomes uncontrolled.
  • Pre-existing Raynaud’s phenomenon (uncomplicated) — counsel on symptom recognition; discontinue at first signs of worsening.
  • Older adults (≥65 years) — limited trial data; cautious dose selection (start at 50 mg) is reasonable.
  • Lactation — low transfer demonstrated (RID ~0.15%, milk-to-plasma ratio 0.23); risk-benefit decision; effects on the breastfed infant are uncharacterised.
  • Operators of heavy machinery / professional drivers — confirm absence of somnolence after the first treated attack before unsupervised use during work.
FDA Class-Wide Regulatory Warning Hypersensitivity Reactions, Hypertension, and Raynaud’s Phenomenon

Hypersensitivity (5.1): Reactions including anaphylaxis, dyspnoea, facial or throat oedema, rash, urticaria, and pruritus have been reported. Reactions can occur minutes, hours, or days after administration. Discontinue Ubrelvy permanently and institute appropriate therapy if a serious or severe reaction occurs.

Hypertension (5.2): New-onset hypertension or worsening of pre-existing hypertension may occur with Ubrelvy. Monitor blood pressure during therapy. If hypertension develops, evaluate for alternative aetiologies; consider discontinuation if blood pressure is inadequately controlled.

Raynaud’s phenomenon (5.3): Development or worsening of Raynaud’s phenomenon has been reported in the post-marketing setting with CGRP antagonists, including Ubrelvy. In reported cases with small-molecule CGRP antagonists, symptom onset occurred a median of 1.5 days following dosing; many cases involved serious outcomes including hospitalisation and disability. Discontinue Ubrelvy if signs or symptoms of Raynaud’s phenomenon develop, and arrange specialist evaluation if symptoms do not resolve.

There is no FDA boxed warning for ubrogepant. The above are class-wide labelled Warnings and Precautions that all prescribers must address with patients before initiation.

Pt

Patient Counselling

Purpose of Therapy

Ubrogepant is taken at the start of a migraine attack to stop it — it is not a daily preventive medicine. It works by blocking a chemical messenger called CGRP that is released during migraine and is responsible for much of the pain. It is a useful alternative for people who cannot take triptans (for example, because of heart or circulation problems), or for whom triptans have not worked or have been poorly tolerated. The medicine has no narrowing effect on blood vessels, which is why it is considered safer in cardiovascular disease.

How to Take

Swallow one tablet whole at the first definite sign of a migraine — not at every minor headache. The dose can be taken with or without food. If the headache is still present or has come back after at least 2 hours, a second tablet may be taken (subject to any cap your prescriber has set). Do not exceed 200 mg in any 24-hour period. The label states that the safety of treating more than 8 migraines in any 30-day period has not been established — keep a simple diary of how many days each month any acute migraine medicine is used and share this at every follow-up visit.

When to Take the Tablet
Tell patient Take it as soon as you are confident an attack has begun — this is when migraine medicines work best. Waiting until the headache is fully established makes the response weaker. The drug works whether or not you have eaten.
Call prescriber If 2 out of 3 consecutive attacks fail to respond despite correct timing — a different strength or a different class of medicine may be more suitable.
Drowsiness After a Dose
Tell patient About 2–3% of people feel sleepy or slowed for a few hours after a dose. Until you know how the medicine affects you, do not drive, operate machinery, or perform safety-critical work after the first treated attack.
Call prescriber If drowsiness is intense, prolonged, or interferes with daily activities — a 50 mg dose or a different class may be considered.
Nausea or Stomach Upset
Tell patient Mild nausea is the most common side effect. Often it is part of the migraine itself rather than the medicine. It typically settles within a few hours and does not usually require treatment to stop.
Call prescriber If nausea is severe, interferes with hydration, or persists more than 24 hours after the last dose — review is appropriate.
Blood Pressure Changes
Tell patient Ubrogepant can sometimes raise blood pressure, or worsen high blood pressure that you already have. Your prescriber will check your blood pressure 2–4 weeks after starting the medicine. If you measure your own BP at home, take a reading every couple of weeks for the first few months.
Call prescriber If you notice consistent home readings above your usual range, new headache patterns suggesting hypertension, or symptoms such as visual disturbance or chest discomfort.
Cold or Discoloured Fingers / Toes (Raynaud’s)
Tell patient A small number of people have developed circulation problems in the fingers or toes after CGRP-blocking medicines like ubrogepant. The fingers or toes can feel numb, cool, or painful, and may change colour from pale to blue to red. Symptoms usually start within a few days of a dose.
Call prescriber Stop ubrogepant and contact your prescriber if you notice any of these changes. In rare cases people have needed hospitalisation, so do not wait until symptoms are severe.
Drug Interactions and Other Medicines
Tell patient Tell every prescriber and pharmacist that you take ubrogepant. Check before starting any antifungal pill, antibiotic (especially clarithromycin or ciprofloxacin), HIV/hepatitis medicine, antiseizure medicine, or herbal supplement. Grapefruit and grapefruit juice can also interact — let your prescriber know if you drink it regularly. St. John’s wort can make ubrogepant stop working.
Call prescriber Before starting any new prescription medicine — especially short courses (antibiotics, antifungals) — to check whether the dose needs adjusting or a temporary alternative is needed.
Allergic Reactions
Tell patient Serious allergic reactions are uncommon but possible — even after several uneventful doses. Reactions can be delayed by hours or days and may include rash, hives, swelling of the face or throat, or difficulty breathing.
Call prescriber Stop ubrogepant and seek emergency care for tongue or throat swelling, difficulty breathing, faintness, or a widespread rash. Do not take any further doses.
Pregnancy and Breastfeeding
Tell patient Use during pregnancy is not recommended unless your prescriber has weighed the alternatives — animal studies suggest possible risk and there are no adequate human data. The manufacturer maintains a pregnancy registry (1-833-277-0206) for women who become pregnant while taking ubrogepant. Small amounts of the medicine pass into breast milk; effects on a breastfed infant are not known.
Call prescriber As soon as pregnancy is confirmed or planned, or before starting breastfeeding — to discuss alternative acute migraine therapy and registry enrolment.
Using Migraine Medicine Too Often
Tell patient The label states that the safety of treating more than 8 migraines in 30 days with ubrogepant is unknown. Using any acute migraine medicine on too many days each month can also paradoxically make headaches more frequent. If you find yourself reaching for treatment that often, you likely need a daily preventive medicine instead.
Call prescriber If you are using ubrogepant on more than 8 days per month, or any combination of acute treatments on more than 10 days per month, or if your migraine pattern is changing or worsening.
Ref

Sources

Regulatory (Prescribing Information)
  1. U.S. Food and Drug Administration. UBRELVY (ubrogepant) tablets — full Prescribing Information. AbbVie. Most recent revision available at: accessdata.fda.gov Primary regulatory document — source of dosing, contraindications, drug interactions, adverse reaction incidence, and the Hypertension and Raynaud’s phenomenon warnings (sections 5.2 and 5.3).
  2. U.S. Food and Drug Administration. NDA 211765 Approval Letter — UBRELVY (ubrogepant). 23 December 2019. accessdata.fda.gov Documents the original FDA approval pathway and labelled indication for acute migraine in adults; confirms US-only approval status.
  3. DailyMed. UBRELVY (ubrogepant) tablet — current label. National Library of Medicine. dailymed.nlm.nih.gov Public-facing repository of the most current FDA-approved label, including the post-marketing class-wide additions for hypertension and Raynaud’s phenomenon.
Key Clinical Trials
  1. Dodick DW, Lipton RB, Ailani J, et al. Ubrogepant for the Treatment of Migraine. N Engl J Med. 2019;381(23):2230–2241. doi: 10.1056/NEJMoa1813049 Pivotal phase 3 ACHIEVE I trial establishing efficacy of 50 mg and 100 mg doses on 2-hour pain freedom and most bothersome symptom freedom.
  2. Lipton RB, Dodick DW, Ailani J, et al. Effect of Ubrogepant vs Placebo on Pain and the Most Bothersome Associated Symptom in the Acute Treatment of Migraine: The ACHIEVE II Randomized Clinical Trial. JAMA. 2019;322(19):1887–1898. doi: 10.1001/jama.2019.16711 Confirmatory phase 3 trial supporting efficacy of 50 mg ubrogepant; informs the lower-strength dosing strategy used in many patients.
  3. Ailani J, Lipton RB, Hutchinson S, et al. Long-Term Safety Evaluation of Ubrogepant for the Acute Treatment of Migraine: Phase 3, Randomized, 52-Week Extension Trial. Headache. 2020;60(1):141–152. doi: 10.1111/head.13682 52-week open-label extension informing the 2.5% discontinuation rate and long-term tolerability profile referenced in this monograph.
  4. Dodick DW, Goadsby PJ, Schwedt TJ, et al. Ubrogepant for the treatment of migraine attacks during the prodrome: a phase 3, multicentre, randomised, double-blind, placebo-controlled, crossover trial in the USA. Lancet. 2023;402(10419):2307–2316. doi: 10.1016/S0140-6736(23)01683-5 PRODROME trial demonstrating efficacy of 100 mg ubrogepant taken during prodromal symptoms in preventing development of moderate-to-severe headache; underpins the off-label prodromal-dosing discussion.
Guidelines / Position Statements
  1. Ailani J, Burch RC, Robbins MS; Board of Directors of the American Headache Society. The American Headache Society Consensus Statement: Update on integrating new migraine treatments into clinical practice. Headache. 2021;61(7):1021–1039. doi: 10.1111/head.14153 AHS consensus statement positioning gepants (including ubrogepant) for acute migraine treatment, including in patients with cardiovascular contraindications to triptans.
  2. Charles AC, Digre KB, Goadsby PJ, Robbins MS, Hershey A; American Headache Society. Calcitonin gene-related peptide-targeting therapies are a first-line option for the prevention of migraine: An American Headache Society position statement update. Headache. 2024;64(4):333–341. doi: 10.1111/head.14692 2024 AHS position update on CGRP-targeting therapies as first-line prevention; relevant for combined preventive-plus-acute strategies in patients on anti-CGRP mAbs who use ubrogepant for breakthrough attacks.
  3. National Institute for Health and Care Excellence (NICE). Headaches in over 12s: diagnosis and management. Clinical Guideline CG150. nice.org.uk/guidance/cg150 UK reference for stepwise migraine management against which gepant positioning is benchmarked, with the caveat that ubrogepant is not currently EMA-approved.
Mechanistic / Basic Science
  1. Edvinsson L, Haanes KA, Warfvinge K, Krause DN. CGRP as the target of new migraine therapies — successful translation from bench to clinic. Nat Rev Neurol. 2018;14(6):338–350. doi: 10.1038/s41582-018-0003-1 Authoritative review of CGRP biology in migraine; provides the mechanistic framework for gepants and anti-CGRP monoclonal antibodies.
  2. Moore E, Fraley ME, Bell IM, et al. Characterization of Ubrogepant: A Potent and Selective Antagonist of the Human Calcitonin Gene-Related Peptide Receptor. J Pharmacol Exp Ther. 2020;373(1):160–166. doi: 10.1124/jpet.119.261065 Preclinical characterisation of ubrogepant binding affinity (Ki ~0.07 nM) and selectivity at the human CGRP receptor; basis for the mechanism statements in this monograph.
Pharmacokinetics / Drug Interactions / Special Populations
  1. Jakate A, Boinpally R, Butler M, Ankrom W, Dockendorf MF, Periclou A. Effects of CYP3A4 and P-glycoprotein inhibition or induction on the pharmacokinetics of ubrogepant in healthy adults: Two phase 1, open-label, fixed-sequence, single-center, crossover trials. Cephalalgia Reports. 2021;4. doi: 10.1177/25158163211037344 DDI study quantifying ubrogepant exposure changes with ketoconazole (~9.7-fold AUC), verapamil (~3.5-fold AUC), and rifampin (80% reduction); supports contraindication and dose-adjustment rules.
  2. Jakate A, Boinpally R, Butler M, et al. Pharmacokinetics and safety of ubrogepant when coadministered with calcitonin gene-related peptide-targeted monoclonal antibody migraine preventives in participants with migraine: A randomized phase 1b drug-drug interaction study. Headache. 2021;61(4):642–652. doi: 10.1111/head.14095 Phase 1b DDI study showing no clinically significant pharmacokinetic interaction between ubrogepant and erenumab or galcanezumab; supports combined acute + preventive strategy.
  3. Ankrom W, Bondiskey P, Li CC, et al. Ubrogepant Is Not Associated With Clinically Meaningful Elevations of Alanine Aminotransferase in Healthy Adult Males. Clin Transl Sci. 2020;13(3):462–472. doi: 10.1111/cts.12728 Healthy-volunteer hepatic safety study supporting the absence of routine LFT monitoring at therapeutic doses.
  4. Scott LJ. Ubrogepant: First Approval. Drugs. 2020;80(3):323–328. doi: 10.1007/s40265-020-01264-5 Concise overview of ubrogepant’s development, mechanism, pharmacokinetics, and the December 2019 FDA approval as the first oral gepant for acute migraine.