Charlesworth Bruce R, Dowson Andrew J, Purdy Allan, Becker Werner J, Boes-Hansen Steen, Färkkilä Markus
AstraZeneca, Macclesfield, England.
CNS Drugs. 2003;17(9):653-67. doi: 10.2165/00023210-200317090-00005.
Zolmitriptan oral tablet is highly effective and well tolerated in the acute treatment of migraine with and without aura in adults. A nasal spray formulation has now been developed. The objective of this study was to compare the efficacy and tolerability of fixed doses of zolmitriptan administered via a nasal spray with placebo and zolmitriptan oral tablet in the acute treatment of migraine.
This was a randomised, double-blind, double-dummy, placebo-controlled, parallel-group, multicentre, dose-ranging study. 1547 patients aged 18-65 years with an established diagnosis of migraine with or without aura (as defined by International Headache Society criteria) who had at least a 1-year history of migraine and an age of onset <50 years were included. Patients were able to distinguish typical migraine from nonmigraine headaches and had experienced an average of one to six migraine headaches per month during the 2 months preceding the study. Patients were randomised to zolmitriptan (Zomig) The use of tradenames is for product identification purposes only and does not imply endorsement.) nasal spray (5.0, 2.5, 1.0 or 0.5 mg), zolmitriptan oral tablet (2.5mg) or placebo for the treatment of three moderate or severe migraine attacks. The primary outcome measure was headache response at 2 hours following treatment, defined as reduced intensity of migraine pain (using a scale of none, mild, moderate or severe) from severe or moderate at baseline to mild or no pain at 2 hours after treatment. Secondary outcome measures included early headache response at 15, 30 and 45 minutes and headache response at 1 and 4 hours postdose, as well as pain-free rates at 15, 30 and 45 minutes and 1, 2 and 4 hours postdose. Laboratory assessments, vital signs, 12-lead ECGs and nose and throat examinations were performed at screening and follow-up visits. Adverse events were recorded throughout the study using Coding Symbols for Thesaurus of Adverse Reaction Terms (COSTART) terminology.
Each dose of zolmitriptan nasal spray produced a greater 2-hour headache response rate than placebo (70.3%, 58.6%, 54.8% and 41.5% for zolmitriptan nasal spray 5.0, 2.5, 1.0 and 0.5mg, compared with 30.6% for placebo [all p < 0.001 vs placebo]). The 2-hour headache response rate for zolmitriptan nasal spray 5.0mg was significantly higher than that of the zolmitriptan 2.5mg oral tablet (61.3%; p < 0.05), while comparisons of nasal spray 0.5, 1.0 and 2.5mg with zolmitriptan 2.5mg oral tablet were not statistically significant. The nasal spray 5.0 and 2.5mg showed a rapid onset of action, with a significant difference in headache response compared with placebo from 15 minutes through 4 hours after administration and a significant difference between the nasal spray 5.0mg and 2.5mg oral tablet from 15 minutes through to 2 hours (the other nasal spray doses were not statistically significant compared with 2.5mg oral tablet). Zolmitriptan nasal spray resulted in pain-free rates that were dose dependent. While all doses from 1.0 mg upwards produced significant pain-free outcomes from 30 minutes versus placebo, only the 5.0mg dose produced pain-free rates significantly superior to both placebo and the 2.5mg oral tablet. Zolmitriptan nasal spray was well tolerated, with the most common adverse events being unusual taste and paresthesia. The majority of adverse events were of short duration and mild or moderate intensity. Only ten patients were withdrawn from the trial because of adverse events. Serious adverse events were reported by nine patients after taking study medication, but none was considered to be causally related to study medication. Zolmitriptan was not associated with any clinically significant changes in laboratory test values or vital signs.
All doses of zolmitriptan nasal spray produced significant 2-hour headache response rates compared with placebo. The 5.0 and 2.5mg doses were also significantly more effective than placebo for the majority of secondary efficacy measures. Zolmitriptan nasal spray 5.0mg provided a headache response statistically superior to both placebo and the 2.5mg tablet as early as 15 minutes after administration, while demonstrating pain-free outcomes significantly superior to placebo and the 2.5mg tablet as early as 30 minutes after administration. All doses of zolmitriptan nasal spray were well tolerated, resulting in an optimal therapeutic index and clinical recommendation for the 5.0mg dose.
佐米曲普坦口服片在成人偏头痛伴或不伴先兆的急性治疗中疗效显著且耐受性良好。现已研发出一种鼻喷雾剂剂型。本研究的目的是比较固定剂量的佐米曲普坦鼻喷雾剂与安慰剂及佐米曲普坦口服片在偏头痛急性治疗中的疗效和耐受性。
这是一项随机、双盲、双模拟、安慰剂对照、平行组、多中心、剂量范围研究。纳入了1547例年龄在18 - 65岁之间、已确诊偏头痛伴或不伴先兆(根据国际头痛协会标准定义)、偏头痛病史至少1年且发病年龄<50岁的患者。患者能够区分典型偏头痛与非偏头痛性头痛,且在研究前2个月内平均每月经历1至6次偏头痛发作。患者被随机分为接受佐米曲普坦(佐米格,使用商品名仅用于产品识别目的,并不意味着认可)鼻喷雾剂(5.0、2.5、1.0或0.5毫克)、佐米曲普坦口服片(2.5毫克)或安慰剂治疗三次中度或重度偏头痛发作。主要结局指标是治疗后2小时的头痛反应,定义为偏头痛疼痛强度从基线时的重度或中度降至治疗后2小时的轻度或无疼痛(使用无、轻度、中度或重度量表)。次要结局指标包括给药后15、30和45分钟的早期头痛反应以及给药后1和4小时的头痛反应,还有给药后15、30和45分钟以及1、2和4小时的无痛率。在筛查和随访时进行实验室评估、生命体征检查、12导联心电图检查以及鼻咽喉检查。在整个研究过程中使用不良反应术语词典编码符号(COSTART)术语记录不良事件。
与安慰剂相比,各剂量的佐米曲普坦鼻喷雾剂在2小时时均产生了更高的头痛反应率(佐米曲普坦鼻喷雾剂5.0、2.5、1.0和0.5毫克的头痛反应率分别为70.3%、58.6%、54.8%和41.5%,而安慰剂为30.6%[与安慰剂相比,所有p<0.001])。佐米曲普坦鼻喷雾剂5.0毫克的2小时头痛反应率显著高于佐米曲普坦2.5毫克口服片(61.3%;p<0.05),而鼻喷雾剂0.5、1.0和2.5毫克与佐米曲普坦2.5毫克口服片的比较无统计学意义。5.0和2.5毫克的鼻喷雾剂起效迅速,给药后15分钟至4小时与安慰剂相比头痛反应有显著差异,5.0毫克鼻喷雾剂与2.5毫克口服片在给药后15分钟至2小时有显著差异(其他鼻喷雾剂剂量与2.5毫克口服片相比无统计学意义)。佐米曲普坦鼻喷雾剂导致的无痛率呈剂量依赖性。虽然1.0毫克及以上的所有剂量在给药后第30分钟与安慰剂相比产生了显著的无痛效果,但只有5.0毫克剂量产生的无痛率显著优于安慰剂和2.5毫克口服片。佐米曲普坦鼻喷雾剂耐受性良好,最常见的不良事件是味觉异常和感觉异常。大多数不良事件持续时间短,强度为轻度或中度。仅有10例患者因不良事件退出试验。9例患者在服用研究药物后报告了严重不良事件,但均不认为与研究药物有因果关系。佐米曲普坦与实验室检查值或生命体征的任何临床显著变化均无关。
与安慰剂相比,所有剂量的佐米曲普坦鼻喷雾剂在2小时时均产生了显著的头痛反应率。5.0和2.5毫克剂量在大多数次要疗效指标上也比安慰剂显著更有效。佐米曲普坦鼻喷雾剂5.0毫克在给药后仅15分钟时头痛反应在统计学上就显著优于安慰剂和2.5毫克片剂,而在给药后仅30分钟时无痛效果就显著优于安慰剂和2.5毫克片剂。所有剂量的佐米曲普坦鼻喷雾剂耐受性良好,得出了最佳治疗指数,并对5.0毫克剂量给出了临床推荐。
