Affiliation:
1. Geisel School of Medicine at Dartmouth Hanover New Hampshire USA
2. Eli Lilly and Company, and/or one of its subsidiaries Indianapolis Indiana USA
Abstract
AbstractObjectiveTo evaluate, at population and individual patient levels, the sustained response of reduction in migraine headache days in patients with migraine treated with galcanezumab.MethodsThis was a post hoc analysis of double‐blind galcanezumab studies in patients with migraine: two 6‐month episodic migraine (EM; EVOLVE‐1/EVOLVE‐2), one 3‐month chronic migraine (CM; REGAIN), and one 3‐month treatment‐resistant migraine (CONQUER). Patients received monthly subcutaneous galcanezumab 120 mg (after 240 mg initial loading dose), galcanezumab 240 mg, or placebo. In the EM and CM studies, the proportions of patients with ≥50% and ≥75% (EM only) reduction from baseline in average monthly migraine headache days from Months 1 to 3 and Months 4 to 6 were evaluated. A mean monthly response rate was estimated. The sustained effect was defined as maintaining ≥50% response for ≥3 consecutive months in the patient‐level data for EM and CM.ResultsA total of 3348 patients with EM or CM from the EVOLVE‐1/EVOLVE‐2 (placebo, n = 894, galcanezumab, n = 879), REGAIN (placebo, n = 558, galcanezumab, n = 555), and CONQUER (EM: placebo, n = 132, galcanezumab, n = 137; CM: placebo, n = 98, galcanezumab, n = 95) studies were included. Patients were predominantly female, White, and had monthly migraine headache day averages ranging from 9.1 to 9.5 days (EM) and 18.1 to 19.6 days (CM). In patients with EM and CM, 19.0% and 22.6% of galcanezumab‐treated patients, respectively, had significantly higher maintenance of ≥50% response for all months in the double‐blind period compared to 8.0% and 1.5% of placebo‐treated patients. The odds ratios (OR) of achieving clinical response for EM and CM were double with galcanezumab (OR = 3.0 [95% CI 1.8, 4.8] and OR = 6.3 [95% CI 1.7, 22.7], respectively). At the individual patient level, of patients who had ≥75% response at Month 3 in the galcanezumab 120 and 240 mg dose groups and placebo group, 39.9% (55/138) and 43.0% (61/142), respectively, of galcanezumab‐treated patients maintained ≥75% response during Months 4–6 compared to 32.7% (51/156) with placebo.ConclusionMore galcanezumab‐treated patients achieved ≥50% response within the first 3 months of treatment compared to placebo; responses were sustained during Months 4–6. The odds of achieving ≥50% response were double with galcanezumab.
Subject
Neurology (clinical),Neurology