TY - JOUR
T1 - Ubrogepant for the treatment of migraine
AU - Dodick, David W.
AU - Lipton, Richard B.
AU - Ailani, Jessica
AU - Lu, Kaifeng
AU - Finnegan, Michelle
AU - Trugman, Joel M.
AU - Szegedi, Armin
N1 - Funding Information:
Dr. Dodick reports receiving consulting fees from Alder Bio-Pharmaceuticals, Autonomic Technologies, Biohaven, Chameleon Communications, electroCore, Foresite Capital, Global Access Meetings, Global Life Sciences, Global Scientific Communications, Haymarket Medical Education, HealthLOGIX, Impel NeuroPharma, Ipsen Biopharm, MediCom Worldwide, Mednet, Miller Medical, Neurolief, Novartis Pharma, Novartis Pharmaceuticals Canada, PeerView, Satsuma Pharmaceuticals, Universal Meeting Management, W.L. Gore, WebMD, Xoc Pharmaceuticals, and Zosano, consulting fees and advisory board fees from Allergan, Amgen, Eli Lilly, eNeura Therapeutics, and Promius Pharma, holding stock options in Aural Analytics, EPIEN Medical, Healint, Mobile Health, and Nocira, receiving fees for serving as a chair on a data and safety monitoring board for Axsome Therapeutics, fees for serving as a board member and holding stock options in King-Devick Technologies and Ontologics, travel support from Sun Pharmaceutical Industries, advisory board fees from Teva Pharmaceuticals, and receiving consulting fees and holding stock options from Theranica; Dr. Lipton, receiving consulting fees from Acorda Therapeutics, Alder Bio-Pharmaceuticals, Allergan, Amgen, Avanir Pharmaceuticals, CVS Health, Dr. Reddy’s Laboratories, Eli Lilly, GlaxoSmith-Kline, Merck, Novartis, Sun Pharmaceutical Industries, Supernus Pharmaceuticals, Teva Pharmaceuticals, Vector Psychometric Group, and Vedanta Research, and receiving consulting fees and holding stock options from Biohaven and eNeura Therapeutics; Dr. Ailani, receiving advisory fees and fees for serving on a steering committee from Alder, consulting fees, fees for serving on a speaker’s bureau, advisory board fees, and fees for serving as a principal investigator for a clinical trial from Allergan, advisory board fees, consulting fees, and lecture fees from Amgen, Eli Lilly, and Teva Pharmaceuticals, consulting fees and advisory board fees from Biohaven, consulting fees from electroCore, Impel NeuroPharma, Revance, and Satsuma Pharmaceuticals, advisory board fees, consulting fees, and fees for serving as a principal investigator for a clinical trial from Zosano, and lecture fees from Promius Pharma; Dr. Lu, being employed by Allergan; Dr. Finnegan, being employed by Allergan, and holding pending patents 62/682,656 and 62/682,345 on treatment of migraine; Dr. Trugman, being employed by and holding stock in Allergan, and holding pending patents 62/682,345 and 62/682,656, licensed to Allergan; Dr. Szegedi, being employed by and holding stock in Allergan, and holding stock in Merck. No other potential conflict of interest relevant to this article was reported.
Publisher Copyright:
© 2019 Massachusetts Medical Society.
PY - 2019/12/5
Y1 - 2019/12/5
N2 - BACKGROUND Ubrogepant is an oral, small-molecule calcitonin gene-related peptide receptor antagonist for acute migraine treatment. METHODS We conducted a randomized trial to evaluate the efficacy, safety, and side-effect profile of ubrogepant. We assigned adults with migraine, with or without aura, in a 1:1:1 ratio to receive an initial dose of placebo, ubrogepant at a dose of 50 mg, or ubrogepant at a dose of 100 mg for treatment of a single migraine attack, with the option to take a second dose. The coprimary efficacy end points were freedom from pain at 2 hours after the initial dose and absence of the most bothersome migraine-associated symptom at 2 hours. Secondary end points included pain relief (at 2 hours), sustained pain relief (from 2 to 24 hours), sustained freedom from pain (from 2 to 24 hours), and absence of symptoms associated with migraine (photophobia, phonophobia, and nausea) at 2 hours. RESULTS A total of 1672 participants were enrolled; 559 were assigned to receive placebo, 556 to receive 50 mg of ubrogepant, and 557 to receive 100 mg of ubrogepant. The percentage of participants who had freedom from pain at 2 hours was 11.8% in the placebo group, 19.2% in the 50-mg ubrogepant group (P=0.002, adjusted for multiplicity, for the comparison with placebo), and 21.2% in the 100-mg ubrogepant group (P<0.001). The percentage of participants who had freedom from the most bothersome symptom at 2 hours was 27.8% in the placebo group, 38.6% in the 50-mg ubrogepant group (P=0.002), and 37.7% in the 100-mg ubrogepant group (P=0.002). Adverse events within 48 hours after the initial or optional second dose were reported in 12.8% of participants in the placebo group, in 9.4% in the 50-mg ubrogepant group, and in 16.3% in the 100-mg ubrogepant group. The most common adverse events were nausea, somnolence, and dry mouth (reported in 0.4 to 4.1%); these events were more frequent in the 100-mg ubrogepant group (reported in 2.1 to 4.1%). Serious adverse events reported within 30 days in the ubrogepant groups included appendicitis, spontaneous abortion, pericardial effusion, and seizure; none of the events occurred within 48 hours after the dose. CONCLUSIONS A higher percentage of participants who received ubrogepant than of those who received placebo had freedom from pain and absence of the most bothersome symptom at 2 hours after the dose. The most commonly reported adverse events were nausea, somnolence, and dry mouth. Further trials are needed to determine the durability and safety of ubrogepant for acute migraine treatment and to compare it with other drugs for migraine.
AB - BACKGROUND Ubrogepant is an oral, small-molecule calcitonin gene-related peptide receptor antagonist for acute migraine treatment. METHODS We conducted a randomized trial to evaluate the efficacy, safety, and side-effect profile of ubrogepant. We assigned adults with migraine, with or without aura, in a 1:1:1 ratio to receive an initial dose of placebo, ubrogepant at a dose of 50 mg, or ubrogepant at a dose of 100 mg for treatment of a single migraine attack, with the option to take a second dose. The coprimary efficacy end points were freedom from pain at 2 hours after the initial dose and absence of the most bothersome migraine-associated symptom at 2 hours. Secondary end points included pain relief (at 2 hours), sustained pain relief (from 2 to 24 hours), sustained freedom from pain (from 2 to 24 hours), and absence of symptoms associated with migraine (photophobia, phonophobia, and nausea) at 2 hours. RESULTS A total of 1672 participants were enrolled; 559 were assigned to receive placebo, 556 to receive 50 mg of ubrogepant, and 557 to receive 100 mg of ubrogepant. The percentage of participants who had freedom from pain at 2 hours was 11.8% in the placebo group, 19.2% in the 50-mg ubrogepant group (P=0.002, adjusted for multiplicity, for the comparison with placebo), and 21.2% in the 100-mg ubrogepant group (P<0.001). The percentage of participants who had freedom from the most bothersome symptom at 2 hours was 27.8% in the placebo group, 38.6% in the 50-mg ubrogepant group (P=0.002), and 37.7% in the 100-mg ubrogepant group (P=0.002). Adverse events within 48 hours after the initial or optional second dose were reported in 12.8% of participants in the placebo group, in 9.4% in the 50-mg ubrogepant group, and in 16.3% in the 100-mg ubrogepant group. The most common adverse events were nausea, somnolence, and dry mouth (reported in 0.4 to 4.1%); these events were more frequent in the 100-mg ubrogepant group (reported in 2.1 to 4.1%). Serious adverse events reported within 30 days in the ubrogepant groups included appendicitis, spontaneous abortion, pericardial effusion, and seizure; none of the events occurred within 48 hours after the dose. CONCLUSIONS A higher percentage of participants who received ubrogepant than of those who received placebo had freedom from pain and absence of the most bothersome symptom at 2 hours after the dose. The most commonly reported adverse events were nausea, somnolence, and dry mouth. Further trials are needed to determine the durability and safety of ubrogepant for acute migraine treatment and to compare it with other drugs for migraine.
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U2 - 10.1056/NEJMoa1813049
DO - 10.1056/NEJMoa1813049
M3 - Article
C2 - 31800988
AN - SCOPUS:85076042559
SN - 0028-4793
VL - 381
SP - 2230
EP - 2241
JO - New England Journal of Medicine
JF - New England Journal of Medicine
IS - 23
ER -