Early onset of efficacy with erenumab in patients with episodic and chronic migraine |
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| Authors: | Todd Schwedt Uwe Reuter Stewart Tepper Messoud Ashina David Kudrow Gregor Broessner Guy P Boudreau Peter McAllister Thuy Vu Feng Zhang Sunfa Cheng Hernan Picard Shihua Wen Joseph Kahn Jan Klatt Daniel Mikol |
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| Institution: | 1.Department of Neurology,Mayo Clinic,Phoenix,USA;2.Department of Neurology,Charité Universit?tsmedizin Berlin,Berlin,Germany;3.Geisel School of Medicine at Dartmouth,Hanover,USA;4.Danish Headache Center and Department of Neurology, Rigshospitalet Glostrup, Faculty of Medical and Health Sciences,University of Copenhagen,Copenhagen,Denmark;5.California Medical Clinic for Headache,Santa Monica,USA;6.Department of Neurology, Headache Outpatient Clinic,Medical University of Innsbruck,Innsbruck,Austria;7.Clinique de la Migraine et Céphalées, Département de Neurologie,Centre Hospitalier de L’Université de Montréal, H?pital Notre-Dame,Montréal,Canada;8.New England Institute for Neurology & Headache,Stamford,USA;9.Amgen Inc.,Thousand Oaks,USA;10.Novartis Pharmaceuticals Corp.,East Hanover,USA;11.Novartis Pharma AG,Basel,Switzerland |
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| Abstract: | BackgroundSubcutaneous erenumab reduced monthly migraine days and increased the likelihood of achieving a?≥?50% reduction at all monthly assessment points tested in 2 pivotal trials in episodic migraine (EM) and chronic migraine (CM). Early efficacy of migraine preventive medications is an important treatment characteristic to patients. Delays in achievement of efficacy can result in failed adherence. The objective of these post-hoc analyses were to evaluate efficacy in the first 4 weeks after initial subcutaneous administration of erenumab 70 mg, erenumab 140 mg, or placebo.MethodsThere is no generally accepted methodology to measure onset of action for migraine preventive medications. We used a comprehensive approach with data from both studies to evaluate change from baseline in weekly migraine days (WMD), achievement of ≥?50% reduction in WMD, and proportion of patients experiencing migraine measured on a daily basis. The 7-day moving averages were overlaid with observed data.ResultsIn both studies (EM: N?=?955; CM: N?=?667), there was evidence of onset of efficacy of erenumab vs. placebo during the first week of treatment, which in some cases reached nominal significance. For EM the changes in WMD were (least squares mean LSM] 95% CI]): placebo, ??0.1 (??0.3, 0.0); erenumab 70 mg, ??0.3 (??0.5, ??0.2) p?=?0.130; erenumab 140 mg, ??0.6 (??0.7, ??0.4) p?<?0.001. For CM the changes were: placebo, ??0.5 (??0.8, ??0.3); erenumab 70 mg, ??0.9 (??1.2, ??0.7) p?=?0.047; erenumab 140 mg, ??0.8 (??1.1, ??0.5) p?=?0.18. Achievement of ≥?50% reduction in WMD was observed as early as Week 1 (adjusted OR 95% CI] erenumab vs placebo) in EM: erenumab 70 mg, 1.3 (1.0, 1.9) p?=?0.097; erenumab 140 mg, 2.0 (1.4, 2.7) p?<?0.001. A similar outcome was observed for CM: erenumab 70 mg, 1.8 (1.1, 2.8) p?=?0.011; erenumab 140 mg, 1.9 (1.2, 2.9) p?=?0.009. Seven-day moving averages of observed data showed each treatment arm differed from placebo by Week 1 (OR 95% CI]): in EM Day 3 for erenumab 140 mg, 0.7 (0.5, 1.0) p?=?0.031 and at Day 7 for 70 mg, 0.6 (0.4, 0.8) p?=?0.002; in CM: Day 6 for erenumab 70 mg, 0.6 (0.4, 0.9) p?=?0.022 and at Day 7 for 140 mg, 0.7 (0.4, 1.0); p?=?0.038.ConclusionErenumab showed early onset of efficacy with separation from placebo within the first week of treatment in both chronic and episodic migraine patients. |
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