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Drug Monograph

Qulipta (Atogepant)

atogepant
CGRP Receptor Antagonist (Small Molecule Gepant) · Oral Tablet · AbbVie Inc.
Pharmacokinetic Profile
Half-Life
~11 hours
Bioavailability
Not formally reported; dose-proportional PK up to 170 mg/day
Volume of Distribution
~292 L (Vz/F)
Metabolism
Primarily CYP3A4; glucuronide conjugate (M23) also circulates
Protein Binding
~95.3% (unbound fraction ~4.7%)
Clinical Information
Drug Class
CGRP Receptor Antagonist (Gepant)
Available Doses
10 mg, 30 mg, 60 mg tablets
Route
Oral
Renal Adjustment
Episodic: 10 mg in severe/ESRD; Chronic: not recommended in severe/ESRD
Hepatic Adjustment
Avoid in severe impairment; no adjustment for mild/moderate
Pregnancy
Based on animal data, may cause fetal harm; registry available
Lactation
Low transfer (~0.19% RID); milk-to-plasma ratio 0.08
Schedule / Legal Status
Prescription only (not a controlled substance)
Generic Available
No
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Preventive treatment of episodic migraine (4–14 migraine days/month)Adults (≥18 years)Preventive (daily dosing; 10, 30, or 60 mg)FDA Approved
Preventive treatment of chronic migraine (≥15 headache days/month)Adults (≥18 years)Preventive (daily dosing; 60 mg only)FDA Approved

Atogepant is the only oral CGRP receptor antagonist approved specifically as a preventive-only migraine therapy with daily dosing, covering both episodic and chronic migraine. It was first approved for episodic migraine prevention in September 2021, and received the chronic migraine indication in April 2023. Unlike rimegepant, which has dual acute-preventive approval, atogepant is indicated solely for prevention. The 2024 American Headache Society position statement identifies CGRP-targeting therapies, including oral gepants, as first-line options for migraine prevention alongside traditional oral preventives, without requiring prior preventive treatment failure.

Off-Label Uses Under Investigation

Acute migraine treatment: Atogepant is not approved for acute treatment. Unlike rimegepant and ubrogepant, atogepant has not been studied in a phase 3 acute treatment trial. Evidence quality: Very low.

Medication overuse headache: The PROGRESS chronic migraine trial allowed enrollment of patients with medication overuse headache. Gepants lack the medication overuse headache risk of triptans and analgesics. Evidence quality: Low.

Dose

Dosing

Episodic Migraine Prevention

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Episodic migraine — standard prevention10 mg, 30 mg, or 60 mg once dailySame as starting dose60 mg/dayAll three doses demonstrated significant efficacy vs placebo; no titration required
Can be taken with or without food; no loading dose needed
Episodic migraine — with strong CYP3A4 inhibitor10 mg once daily10 mg once daily10 mg/dayStrong CYP3A4 inhibitors increase atogepant AUC 5.5-fold
Applies to ketoconazole, itraconazole, clarithromycin, ritonavir
Episodic migraine — with OATP inhibitors10 mg or 30 mg once daily10 mg or 30 mg once daily30 mg/dayOATP inhibitors increase atogepant AUC ~2.85-fold
Includes cyclosporine, rifampin (single dose as OATP inhibitor)
Episodic migraine — severe renal impairment or ESRD10 mg once daily10 mg once daily10 mg/dayCrCl <30 mL/min; for ESRD on dialysis, take after dialysis
Renal elimination is a minor route but safety data are limited in this population

Chronic Migraine Prevention

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Chronic migraine — standard prevention60 mg once daily60 mg once daily60 mg/dayOnly the 60 mg dose was studied in chronic migraine (PROGRESS trial)
11% of trial patients used one concurrent oral preventive
Chronic migraine — with strong CYP3A4 inhibitor10 mg once daily10 mg once daily10 mg/daySame dose reduction as episodic migraine for strong inhibitors
AUC 5.5-fold increase requires maximum dose reduction
Chronic migraine — with strong/moderate CYP3A4 inducerNot recommendedN/AN/AInducers decrease atogepant exposure (AUC reduced up to 60%); loss of efficacy likely
Includes rifampin, phenytoin, carbamazepine, efavirenz
Chronic migraine — severe renal impairment or ESRDNot recommendedN/AN/AInsufficient safety data in chronic migraine with severe renal impairment
Consider alternative preventive therapy in these patients
Clinical Pearl: Dose Selection for Episodic Migraine

All three approved doses (10, 30, 60 mg) demonstrated statistically significant efficacy over placebo in the ADVANCE trial, with 50% responder rates of 56%, 59%, and 61% respectively (vs 29% placebo). The 60 mg dose showed numerically greater reductions in monthly migraine days but also had higher rates of nausea (9%) and constipation (8%) compared with the 10 mg dose (5% and 6%, respectively). Starting at 10 mg may be reasonable for patients concerned about tolerability, while 60 mg may be preferred when maximal efficacy is desired. No titration is required regardless of starting dose.

PK

Pharmacology

Mechanism of Action

Atogepant is an orally administered small molecule that competitively antagonizes the calcitonin gene-related peptide (CGRP) receptor, blocking CGRP-mediated signaling involved in migraine pathophysiology. Like rimegepant, it targets the receptor (CLR/RAMP1 heterodimer) rather than the CGRP ligand itself. The key distinction of atogepant within the gepant class is its development exclusively as a once-daily preventive agent rather than an acute/dual-purpose treatment. While CGRP receptor antagonism is the shared mechanism among gepants, atogepant has a distinct pharmacokinetic profile from rimegepant and ubrogepant, including a larger volume of distribution and unique transporter substrate properties (OATP1B1/1B3) that create a different drug interaction profile. The daily dosing schedule provides sustained CGRP receptor blockade, reducing the frequency and severity of migraine attacks through continuous modulation of the trigeminovascular pathway.

ADME Profile

ParameterValueClinical Implication
AbsorptionTmax ~1–2 h; dose-proportional up to 170 mg/day; food effect not significant (AUC -18%, Cmax -22%); no accumulationRapid absorption; can be taken with or without food; no loading dose needed
DistributionVz/F ~292 L; unbound fraction ~4.7% (~95.3% protein bound)Large Vd suggests extensive tissue distribution; substrate of P-gp, BCRP, OATP1B1, OATP1B3, and OAT1 transporters
MetabolismPrimarily CYP3A4; parent compound and glucuronide metabolite (M23) are the main circulating componentsCYP3A4 dependence creates significant interactions with strong inhibitors (5.5-fold AUC increase) and inducers (60% AUC decrease with rifampin)
Eliminationt½ ~11 h; CL/F ~19 L/h; 42% unchanged in feces, 5% unchanged in urineShort half-life supports once-daily dosing with no accumulation; hepatic/fecal elimination predominates over renal
SE

Side Effects

1–10% Common
Adverse EffectIncidence (10 / 30 / 60 mg)Clinical Note
Nausea5% / 6% / 9% (vs 3% placebo)Most common adverse effect; dose-related; led to discontinuation in 0.6% of patients
Constipation6% / 6% / 8% (vs 2% placebo)Dose-related; led to discontinuation in 0.5%; advise adequate hydration and fiber intake
Fatigue / Somnolence4% / 4% / 5% (vs 4% placebo)Only marginally above placebo at 60 mg; led to discontinuation in 0.2%
Decreased Appetite2% / 1% / 3% (vs <1% placebo)May contribute to weight loss observed with longer-term use
Dizziness2% / 2% / 3% (vs 2% placebo)Similar to placebo at lower doses; only marginally higher at 60 mg
Serious Serious (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Hypersensitivity (anaphylaxis, dyspnea, rash, urticaria, facial edema)Rare (postmarketing)Can occur days after administrationPermanent discontinuation; initiate appropriate therapy; report to manufacturer
Hypertension (new-onset or worsening)Rare (postmarketing)Most commonly within 7 days of therapy initiationMonitor BP; consider discontinuation if inadequately controlled
Raynaud’s phenomenon (new-onset or worsening)Rare (postmarketing)Median 1.5 days after dosing (small molecule CGRP antagonist class data)Discontinue atogepant; refer for evaluation; most cases resolve after discontinuation
Hepatotransaminase elevation (>3× ULN)0.9% (vs 1.2% placebo)During treatment; temporally associated cases notedAsymptomatic and resolved within 8 weeks of discontinuation; no severe liver injury or jaundice reported
Discontinuation Discontinuation Rates & Weight Changes
Discontinuation Due to Adverse Events
Low
Top reasons: Nausea (0.6%), constipation (0.5%), fatigue/somnolence (0.2%)
Weight Decrease ≥7%
5.3% (60 mg) vs 2.5% placebo
10 mg: 3.8%, 30 mg: 3.2%; dose-related; may be related to decreased appetite and nausea effects
Reason for DiscontinuationIncidenceContext
Nausea0.6%Most common reason for discontinuation across all dose groups
Constipation0.5%Generally manageable with dietary measures
Fatigue / Somnolence0.2%Rare cause of discontinuation despite being a common side effect
Weight Loss Monitoring

Atogepant is associated with dose-related decreases in body weight, with 5.3% of patients on 60 mg experiencing a weight loss of at least 7% at any point during trials (vs 2.5% placebo). This may be related to the combined effects of decreased appetite and gastrointestinal adverse effects. While this may be a desirable effect for some patients, unintended weight loss should be monitored, particularly in underweight individuals or those at risk for eating disorders.

Int

Drug Interactions

Atogepant is metabolized primarily by CYP3A4 and is a substrate of multiple transporters including P-gp, BCRP, OATP1B1, OATP1B3, and OAT1. This creates clinically significant interactions with strong CYP3A4 inhibitors and inducers, as well as a unique OATP-mediated interaction not seen with other gepants. Atogepant is not a clinically significant CYP inhibitor or inducer at therapeutic concentrations.

Major Strong CYP3A4 Inhibitors (itraconazole, ketoconazole, clarithromycin, ritonavir)
MechanismInhibition of CYP3A4-mediated atogepant metabolism
EffectIncreases atogepant AUC 5.5-fold and Cmax 2.15-fold (itraconazole study)
ManagementReduce dose to 10 mg once daily for both episodic and chronic migraine
FDA PI
Major Strong/Moderate CYP3A4 Inducers (rifampin, phenytoin, carbamazepine)
MechanismCYP3A4 induction (and P-gp induction) increases atogepant clearance
EffectRifampin (steady-state): decreases atogepant AUC by 60% and Cmax by 30%; loss of efficacy likely
ManagementEpisodic: use 60 mg daily, monitor for reduced efficacy; Chronic: not recommended with strong/moderate inducers
FDA PI
Moderate OATP Inhibitors (cyclosporine, rifampin single dose)
MechanismInhibition of OATP1B1/1B3 hepatic uptake transporters reduces atogepant clearance
EffectSingle-dose rifampin (OATP inhibitor only): increases atogepant AUC 2.85-fold and Cmax 2.23-fold
ManagementEpisodic: 10 or 30 mg once daily; Chronic: 30 mg once daily
FDA PI
Moderate Weak CYP3A4 Inducers (topiramate)
MechanismMild CYP3A4 induction modestly reduces atogepant exposure
EffectTopiramate: decreases atogepant AUC by 25% and Cmax by 24%
ManagementEpisodic: use 30 or 60 mg; Chronic: use 60 mg, monitor for reduced efficacy
FDA PI
Minor Sumatriptan, Ubrogepant, OCs, NSAIDs, Acetaminophen
MechanismNo significant pharmacokinetic interactions in dedicated studies
EffectNo change in exposure of atogepant or co-administered drugs
ManagementNo dose adjustment needed; safe to use concurrently
FDA PI (12.3)
Minor Moderate/Weak CYP3A4 Inhibitors, P-gp Inhibitors, BCRP Inhibitors
MechanismModerate CYP3A4 inhibitors increase AUC ~1.7-fold (PBPK); P-gp inhibitors +26% AUC; BCRP inhibitors ~1.2-fold
EffectChanges not expected to be clinically significant
ManagementNo dose adjustment needed
FDA PI (12.3)
Mon

Monitoring

  • Migraine Diary Continuous; review at 3 months
    Routine     Track monthly migraine days, headache severity, and acute medication use days. Assess response at 12 weeks as per the ADVANCE and PROGRESS trial endpoints. For patients on strong CYP3A4 inducers, monitor monthly for reduced efficacy.
  • Blood Pressure Baseline, then periodically
    Routine     Postmarketing reports of new-onset and worsening hypertension with CGRP antagonists, most commonly within 7 days of initiation. Consider discontinuation if BP is inadequately controlled.
  • Body Weight Baseline, then periodically
    Routine     Weight decrease of at least 7% occurred in up to 5.3% of patients on 60 mg (vs 2.5% placebo). Monitor for unintended weight loss, especially in underweight patients.
  • Hepatic Function Baseline; as clinically indicated
    Trigger-based     Transaminase elevations >3× ULN occurred in 0.9% of patients (vs 1.2% placebo). Cases temporally associated with treatment resolved within 8 weeks of discontinuation. No severe liver injury reported.
  • Drug Interaction Review At initiation; with any medication change
    Routine     Atogepant has a complex dose-adjustment table. Check for strong CYP3A4 inhibitors/inducers, OATP inhibitors, and topiramate (weak inducer) co-administration. Dose changes differ between episodic and chronic migraine.
  • Raynaud’s Symptoms Ongoing patient reporting
    Trigger-based     Median onset ~1.5 days for small molecule CGRP antagonists. Discontinue if new cold-induced color changes or pain in extremities develop.
CI

Contraindications & Cautions

Absolute Contraindications

  • Hypersensitivity to atogepant or any component of Qulipta. Reactions have included anaphylaxis and dyspnea, and can occur days after administration.

Relative Contraindications (Specialist Input Recommended)

  • Severe hepatic impairment: Total atogepant exposure increased by 38%. Avoid use per FDA labeling due to potential for liver injury.
  • Chronic migraine with severe renal impairment or ESRD: Use of atogepant is not recommended in these patients for the chronic migraine indication.

Use with Caution

  • Episodic migraine with severe renal impairment or ESRD (CrCl <30 mL/min): Reduce dose to 10 mg once daily. In ESRD on dialysis, preferably take after dialysis session.
  • Pre-existing hypertension: Postmarketing reports of new-onset and worsening hypertension. Most common within 7 days of initiation.
  • History of Raynaud’s phenomenon: New-onset or worsening symptoms reported; median onset 1.5 days for small molecule CGRP antagonists.
  • Pregnancy: Based on animal data, atogepant may cause fetal harm (decreased fetal body weight and skeletal variations in rats; increased visceral and skeletal variations in rabbits). Pregnancy exposure registry available (1-833-277-0206 or empresspregnancyregistry.com).
  • Concurrent strong CYP3A4 inhibitors or OATP inhibitors: Requires dose adjustment per Table 1 in prescribing information.
FDA Class-Wide Regulatory Warning CGRP Antagonists: Hypertension and Raynaud’s Phenomenon (March 2025 Update)

The FDA updated labeling for all CGRP antagonists, including atogepant, to include warnings for hypertension and Raynaud’s phenomenon based on postmarketing reports. For small molecule CGRP antagonists, Raynaud’s symptom onset occurred a median of 1.5 days following dosing. Many cases involved serious outcomes including hospitalization and disability. In most cases, discontinuation of the CGRP antagonist resulted in symptom resolution. Hypertension was most frequently reported within 7 days of therapy initiation, with some cases requiring hospitalization.

Pt

Patient Counselling

Purpose of Therapy

Atogepant is a daily preventive medication that reduces the frequency and severity of migraine attacks. It does not treat migraine attacks once they start. Patients should continue to use their prescribed acute migraine treatments (such as triptans or NSAIDs) for breakthrough attacks. Benefit is typically assessed after 12 weeks of consistent daily use. Unlike triptans, atogepant does not carry a risk of medication overuse headache.

How to Take

Take one tablet by mouth once daily, with or without food, at approximately the same time each day. Swallow the tablet whole. If a dose is missed, take it as soon as remembered on the same day, then resume the regular schedule the next day. Do not take two doses in one day to make up for a missed dose. Store at room temperature (20–25°C / 68–77°F).

Nausea & Constipation
Tell patient Nausea and constipation are the most common side effects (up to 9% and 8% at the 60 mg dose). They are generally mild to moderate and often improve over time. Drinking adequate water and eating fiber-rich foods can help manage constipation.
Call prescriber If nausea or constipation is severe, persistent, or interferes with daily activities. A dose reduction (e.g., from 60 mg to 30 mg or 10 mg) may help for episodic migraine.
Allergic Reactions
Tell patient Serious allergic reactions including facial swelling, rash, hives, itching, and difficulty breathing can occur, sometimes days after taking a dose. Stop atogepant and seek emergency help if these symptoms develop.
Call prescriber Seek emergency help immediately for trouble breathing, facial swelling, or severe rash. Contact your prescriber for any new rash, hives, or itching after starting treatment.
Blood Pressure & Circulation Changes
Tell patient Blood pressure may increase during treatment. Home monitoring may be recommended, especially in the first week. Rarely, numbness, color changes, or pain in fingers and toes (Raynaud’s phenomenon) may occur.
Call prescriber If BP readings are consistently elevated, or if you experience color changes, numbness, or pain in your fingers or toes. Stop atogepant if Raynaud’s symptoms occur.
Drug Interactions & Dose Changes
Tell patient Many medications can change the dose of atogepant needed. Always inform your prescriber before starting any new medication, including antifungals, certain antibiotics, HIV medications, seizure medications (phenytoin, carbamazepine), topiramate, cyclosporine, and herbal supplements (St. John’s Wort).
Call prescriber Before starting or stopping any medication. Your atogepant dose may need to be adjusted.
Pregnancy & Breastfeeding
Tell patient Animal studies suggest atogepant may cause harm to an unborn baby. A pregnancy registry is available (1-833-277-0206 or empresspregnancyregistry.com). Very small amounts pass into breast milk (~0.19% of maternal dose).
Call prescriber Contact your prescriber immediately if you become pregnant or plan to become pregnant during treatment.
Ref

Sources

Regulatory (PI / SmPC)
  1. AbbVie Inc. QULIPTA (atogepant) tablets, for oral use: US Prescribing Information. Revised September 2025. FDA Label Primary source for dosing, pharmacokinetics, adverse reactions, drug interactions, dose adjustments, and September 2025 labeling updates.
Key Clinical Trials
  1. Ailani J, Lipton RB, Goadsby PJ, et al. Atogepant for the preventive treatment of migraine (ADVANCE). N Engl J Med. 2021;385(8):695–706. doi:10.1056/NEJMoa2035908 Pivotal phase 3 trial (Study 1) in episodic migraine (N=910) demonstrating significant MMD reduction at all three doses (10, 30, 60 mg) vs placebo.
  2. Lipton RB, Pozo-Rosich P, Blumenfeld AM, et al. Effect of atogepant for preventive migraine treatment on patient-reported outcomes in the ADVANCE trial. Neurology. 2023;100(8):e764–e777. doi:10.1212/WNL.0000000000201568 Patient-reported outcome analysis from ADVANCE showing significant improvements in migraine-related disability and quality of life measures.
  3. Pozo-Rosich P, Ailani J, Engstrom E, et al. Atogepant for the preventive treatment of chronic migraine (PROGRESS). Lancet. 2023;402(10404):775–785. doi:10.1016/S0140-6736(23)01049-8 Pivotal phase 3 trial (Study 3) establishing efficacy of atogepant 60 mg QD for chronic migraine prevention (N=778 randomized across three arms; FDA approved the 60 mg QD dose).
  4. Ashina M, Tepper SJ, Reuter U, et al. Once-daily oral atogepant for the long-term preventive treatment of migraine: findings from a multicenter, randomized, open-label, phase 3 trial. Headache. 2023;63(1):79–88. doi:10.1111/head.14439 52-week open-label extension demonstrating sustained efficacy and long-term safety of daily atogepant in 744 patients.
Guidelines
  1. Charles AC, Digre KB, Goadsby PJ, Robbins MS, Hershey A. 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 statement upgrading CGRP-targeting therapies to first-line preventive status alongside traditional oral preventives.
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 Comprehensive review of CGRP pathway pharmacology and the development of small molecule receptor antagonists (gepants).
  2. Russo AF. Calcitonin gene-related peptide (CGRP): a new target for migraine. Annu Rev Pharmacol Toxicol. 2015;55:533–552. doi:10.1146/annurev-pharmtox-010814-124701 Foundational review of the CGRP signaling pathway and its role as a therapeutic target in migraine.
Pharmacokinetics / Special Populations
  1. Deeks ED. Atogepant: first approval. Drugs. 2022;82(1):65–70. doi:10.1007/s40265-021-01661-w Concise first-approval review covering atogepant pharmacology, clinical trial results, and place in therapy.
  2. Boinpally R, Jakate A, Butler M, Borbridge L, Periclou A. Single-dose pharmacokinetics and safety of atogepant in adults with hepatic impairment: results from an open-label, phase 1 trial. Clin Pharmacol Drug Dev. 2021;10(7):726–733. doi:10.1002/cpdd.916 Phase 1 hepatic impairment PK study establishing the 15–38% AUC increases across impairment severity grades with atogepant 60 mg.
  3. Boinpally R, Trugman JM, Engstrom E, et al. Pharmacokinetics of atogepant in subjects with renal impairment. Headache. 2023;63(3):399–408. doi:10.1111/head.14474 Renal impairment PK study supporting dose adjustment recommendations for severe renal impairment and ESRD.
  4. Goadsby PJ, Dodick DW, Ailani J, et al. Safety, tolerability, and efficacy of orally administered atogepant for the prevention of episodic migraine in adults: a double-blind, randomised phase 2b/3 trial (Study 2). Lancet Neurol. 2020;19(9):727–737. doi:10.1016/S1474-4422(20)30234-9 Phase 2b/3 episodic migraine trial (Study 2 in PI, N=652) providing supporting efficacy data across all three dose levels.