Leiden University Medical Centre, The Netherlands.
Cephalalgia. 2010 Oct;30(10):1170-8. doi: 10.1177/0333102410375512. Epub 2010 Jun 15.
Lasmiditan (COL-144; LY573144) is a novel, highly selective and potent agonist at 5-HT(1F) receptors that lacks vasoconstrictor activity. Preclinical and early clinical experiments predict acute antimigraine efficacy of COL-144 that is mediated through a non-vascular, primarily neural, mechanism.
In a randomised, multicentre, placebo-controlled, double-blind, group-sequential, adaptive treatment-assignment, proof-of-concept and dose-finding study, we treated 130 subjects in-hospital during a migraine attack. Subjects were allocated to an intravenous dose level of lasmiditan or placebo in small cohorts. The starting dose was 2.5 mg. Subsequent doses were adjusted, up or down, according to the safety and efficacy seen in the preceding cohort. The primary outcome measure was headache response defined as improvement from moderate or severe headache at baseline to mild or no headache at 2 h post-dose. The study was designed to explore the overall dose response relationship but was not powered to differentiate individual doses from placebo, nor to detect effect differences for other migraine symptoms.
Forty-two subjects received placebo and 88 received lasmiditan in doses of 2.5-45 mg. Subjects were observed in the clinic for 4 h after treatment and used a diary card to record symptoms and adverse events for up to 24 h. The study was terminated when the 20 mg dose met predefined efficacy stopping rules. Of subjects treated in the 10, 20, 30 and 45 mg lasmiditan dose groups, 54-75% showed a 2 h headache response, compared to 45% in the placebo group (P = 0.0126 for the linear association between response rates and dose levels). Patient global impression at 2 h and lack of need for rescue medication also showed statistically significant linear correlations with dose. Lasmiditan was generally well tolerated. Adverse events were reported by 65% of subjects on lasmiditan and by 43% on placebo and were generally mild. Dizziness, paresthesia and sensations of heaviness (usually limb) were more common on lasmiditan.
At intravenous doses of 20 mg and higher, lasmiditan proved effective in the acute treatment of migraine. Further studies to assess the optimal oral dose and full efficacy and tolerability profile are under way. The non-vascular, neural mechanism of action of lasmiditan may offer an alternative means to treat migraine especially in patients who have contra-indications for agents with vasoconstrictor activity. The clinicaltrials.gov identifier for this study is NCT00384774.
Lasmiditan(COL-144;LY573144)是一种新型的、高度选择性和有效的 5-HT(1F)受体激动剂,没有血管收缩活性。临床前和早期临床试验预测 COL-144 具有急性抗偏头痛疗效,其通过非血管、主要是神经机制介导。
在一项随机、多中心、安慰剂对照、双盲、分组序贯、适应性治疗分配、概念验证和剂量发现研究中,我们在偏头痛发作期间对 130 名住院患者进行了治疗。受试者被分配到静脉内 lasmiditan 或安慰剂的剂量水平。起始剂量为 2.5mg。根据前一组的安全性和疗效,调整后续剂量,增加或减少。主要终点是头痛反应,定义为从基线时中度或重度头痛改善到 2 小时后轻度或无头痛。该研究旨在探索总体剂量反应关系,但没有足够的能力来区分个体剂量与安慰剂的差异,也无法检测其他偏头痛症状的疗效差异。
42 名受试者接受安慰剂治疗,88 名受试者接受 lasmiditan 治疗,剂量为 2.5-45mg。治疗后,受试者在诊所观察 4 小时,并使用日记卡记录症状和不良反应,最长达 24 小时。当 20mg 剂量达到预定的疗效停止规则时,研究终止。在接受 10、20、30 和 45mg lasmiditan 剂量组的受试者中,54-75%在 2 小时时出现头痛反应,而安慰剂组为 45%(反应率与剂量水平之间的线性关联 P=0.0126)。2 小时时患者整体印象和无需抢救药物也显示出与剂量的统计学显著线性相关性。Lasmiditan 通常耐受性良好。接受 lasmiditan 治疗的受试者中有 65%和接受安慰剂治疗的受试者中有 43%报告了不良反应,通常为轻度。头晕、感觉异常和沉重感(通常为肢体)在 lasmiditan 中更为常见。
在 20mg 及更高剂量的静脉内给药时,lasmiditan 已被证明可有效治疗偏头痛。正在进行进一步的研究,以评估最佳口服剂量和充分的疗效和耐受性特征。Lasmiditan 的非血管、神经作用机制可能为治疗偏头痛提供一种替代方法,特别是在对具有血管收缩活性的药物有禁忌症的患者中。本研究的 ClinicalTrials.gov 标识符为 NCT00384774。
