GlaxoSmithKline, Research Triangle Park, NC 27709, USA.
Headache. 2011 Oct;51(9):1374-87. doi: 10.1111/j.1526-4610.2011.01965.x. Epub 2011 Jul 28.
To evaluate the long-term safety, tolerability, effectiveness, impact on quality of life, and medication satisfaction of sumatriptan/naproxen sodium in the acute treatment of migraine headache in adolescents.
This 12-month, multicenter, open-label, safety study was conducted in adolescents (aged 12-17 years) with an average of 2-8 migraines/month typically lasting >2 hours untreated for >6 months prior to initiation. Subjects were instructed to treat migraines as early as possible and were allowed to rescue 2 hours post dose with a single dose of a naproxen-containing product, over-the-counter pain reliever, or anti-emetics. Subjects were advised not to take a second tablet of sumatriptan/naproxen sodium without at least a 24-hour headache-free period. Safety evaluations included adverse events, laboratory tests, and vital signs and electrocardiogram evaluation. Other evaluations included freedom from pain, quality of life, and medication satisfaction.
Of the 656 subjects enrolled, 622 (95%) treated at least 1 migraine with sumatriptan/naproxen sodium, of which 435 (70%) and 363 (58%) completed 6 and 12 months of the study, respectively. Overall, there were 12,927 exposures to sumatriptan/naproxen sodium: on average 2.5 tablets were taken per month per subject. The most common treatment-related adverse events were nausea (7%), dizziness (3%), muscle tightness (3%), and chest discomfort (3%). There were no deaths; 4 subjects had 5 serious adverse events (suicide attempt, hemolytic anemia and syncope, suicidal ideation, spontaneous abortion) unrelated to sumatriptan/naproxen sodium and resolved without sequelae. Seven percent of subjects discontinued participation in the study because of an adverse event; 5% of subjects discontinued due to lack of efficacy. Overall, 42% of the migraine attacks were pain-free within 2 hours of treatment with sumatriptan/naproxen sodium, subjects reported improvements from baseline in 2 of 3 quality of life domains over time, and were generally satisfied with the efficacy and overall treatment at the end of the study.
In adolescent migraineurs, after up to 12 months and over 12,000 exposures to sumatriptan/naproxen sodium, there were no new or clinically significant findings in the safety parameters, including the frequency and nature of adverse events, as compared to the individual components or to the adverse event profile in adults. In addition, sumatriptan/naproxen sodium provided freedom from pain over time, improvements in quality of life and medication satisfaction.
评估舒马曲坦/萘普生钠在青少年偏头痛急性治疗中的长期安全性、耐受性、有效性、对生活质量的影响和药物满意度。
这是一项为期 12 个月的多中心、开放性、安全性研究,纳入了平均每月有 2-8 次偏头痛、未经治疗的偏头痛发作持续时间>2 小时且在研究开始前>6 个月的青少年(年龄 12-17 岁)。患者被指示尽早治疗偏头痛,并允许在剂量后 2 小时使用单次剂量的含萘普生产品、非处方止痛药或止吐药进行解救。建议患者在没有至少 24 小时无头痛期的情况下,不要服用第二片舒马曲坦/萘普生钠。安全性评估包括不良事件、实验室检查以及生命体征和心电图评估。其他评估包括疼痛缓解、生活质量和药物满意度。
在 656 名入组的患者中,有 622 名(95%)至少用舒马曲坦/萘普生钠治疗了 1 次偏头痛,其中 435 名(70%)和 363 名(58%)分别完成了 6 个月和 12 个月的研究。总体而言,共进行了 12927 次舒马曲坦/萘普生钠暴露:平均每位患者每月服用 2.5 片。最常见的治疗相关不良事件是恶心(7%)、头晕(3%)、肌肉紧张(3%)和胸部不适(3%)。无死亡事件;4 名患者发生 5 例严重不良事件(自杀未遂、溶血性贫血和晕厥、自杀意念、自然流产),与舒马曲坦/萘普生钠无关,且无后遗症。7%的患者因不良事件而退出研究;5%的患者因疗效不佳而退出。总体而言,有 42%的偏头痛发作在服用舒马曲坦/萘普生钠后 2 小时内疼痛缓解,患者报告随着时间的推移在 3 个生活质量领域中的 2 个领域有改善,并且在研究结束时对疗效和整体治疗总体上感到满意。
在青少年偏头痛患者中,在接受了长达 12 个月和超过 12000 次舒马曲坦/萘普生钠暴露后,与单一成分或成年人的不良事件概况相比,在安全性参数方面,包括不良事件的频率和性质,均无新的或临床意义重大的发现。此外,舒马曲坦/萘普生钠随着时间的推移提供了疼痛缓解、生活质量和药物满意度的改善。
