Winner 2006.
| Methods | Multicentre, randomised, double‐blind, placebo‐controlled, parallel‐group. Single dose to treat single attack. Medication administered to treat a morning migraine (defined as a headache of moderate or severe intensity on awakening) within 1 hour of awakening Assessments at 10, 20, 30, 60, and 120 minutes after dosing Second dose of study medication or alternative rescue medication available after 2 h for participants with inadequate relief or for those experiencing recurrence within 24 h 2 identically designed studies: Study 1 and Study 2 |
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| Participants | Aged 18 to 65 years, meeting IHS criteria for migraine (1988) with or without aura. At least 1‐year history of migraine with 1 to 6 attacks per month, and had awakened with moderate or severe migraine pain at least once in the 3 months preceding screening. No migraine prophylactic medication containing ergotamine, an ergot derivative, or methysergide, and no use of a monoamine oxidase inhibitor within 2 weeks before the studies. Participants were eligible for the studies only if they had previously treated a migraine successfully with a 5‐HT1B/1D agonist, but participants who had previously used subcutaneous sumatriptan were excluded No analgesics, antiemetics, or acute migraine medications from 6 h before through to 2 h after administration of study medication. No other 5‐HT agonists within 24 h before or after use of study medication, and no ergotamine or ergot‐type medications (including methysergide) for the duration of the studies Study 1 N = 299 (297 for efficacy) M 50, F 247 (83%) Mean age 41 years Without aura 61% Study 2 N = 288 (287 for efficacy) M 38, F 249 (87%) Mean age 39 years Without aura 73% |
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| Interventions | Study 1 Sumatriptan 6 mg, n = 146 (145 for efficacy, 144 with moderate or severe baseline pain intensity) Placebo, n = 153 (152 for efficacy, 151 with moderate or severe baseline pain intensity) Study 2 Sumatriptan 6 mg, n = 149 (148 for efficacy) Placebo, n = 139 |
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| Outcomes | Headache relief (at 1 and 2 h) Pain‐free (at 2 h) 24 h sustained pain‐free Improvement in nausea, vomiting, photophobia, and phonophobia at 2 h Improvement in functional disability at 2 h Adverse events Withdrawals |
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| Notes | Oxford Quality Score: R2, DB2, W1. Total = 5. | |
| Risk of bias | ||
| Bias | Authors' judgement | Support for judgement |
| Random sequence generation (selection bias) | Low risk | Computer‐generated randomisation schedule |
| Allocation concealment (selection bias) | Low risk | Remote allocation |
| Blinding (performance bias and detection bias) All outcomes | Low risk | Matching inactive vehicle injection in identical prefilled single‐dose syringe cartridges |
| Study size | Unclear risk | Treatment groups 50 to 200 participants |
All medication delivered subcutaneously unless otherwise stated
AE: adverse event; DB: double‐blinding; DHE: dihydroergotamine; GP: general practitioner; h: hour; IHS: International Headache Society; NSAIDs: non‐steroidal anti‐inflammatory drugs; R: randomisation; W: withdrawals