Moore K H, Hussey E K, Shaw S, Fuseau E, Duquesnoy C, Pakes G E
Glaxo Wellcome Inc., Research Triangle Park, NC 27709, USA.
Cephalalgia. 1997 Jun;17(4):541-50. doi: 10.1046/j.1468-2982.1997.1704541.x.
The delivery of sumatriptan doses intranasally could add greater flexibility in the treatment of migraine than is possible with the currently available subcutaneous and oral sumatriptan preparations. Two independent double-blind, randomized, placebo-controlled clinical studies were conducted to evaluate the safety, tolerability and pharmacokinetics of intranasally administered sumatriptan following ascending single doses (three different dose levels) and multiple doses. In the four-way, crossover, ascending-dose study, 20 healthy female subjects were randomized to receive on separate occasions single intranasal spray doses of 5, 10, or 20 mg sumatriptan (as the hemisulphate salt) or placebo into one nostril. Adverse events were mild and consisted mainly of bitter taste at the back of the throat and events typical of sumatriptan administered by other routes (headache, lightheadedness and tingling). Area under the plasma sumatriptan concentration versus time curve (AUC infinity) and peak plasma concentration (Cmax) increased with the dose. Dose proportionality was demonstrated between 5 and 10 mg but not across the dose range 5-20 mg. Time to maximum plasma concentration (tmax) was variable due to multiple peaking. The elimination half-life (t1/2), approximately 2 h, was unaffected by the magnitude of dose. In the two-period, multiple-dose, crossover study, 12 healthy adult male and female subjects were randomized to receive either sumatriptan hemisulphate 20 mg or placebo, administered intranasally as a spray three times a day for 4 days. The two dosing periods were separated by 3 to 14 days. Multiple doses of sumatriptan were well tolerated, with no serious adverse events occurring or withdrawals due to adverse events. All patients reported a mild to moderate drug-related disturbance of taste. Nasal examinations remained normal, and olfactory function was unaffected. The AUC over the first 8 h following dosing (AUC8) and fraction of the dose excreted in the urine (fe; 6.2% vs 3.6%) were similar on Days 1 and 4. Day 4 values were significantly higher (p < or = 0.05) for Cmax (16.9 ng/ml vs 13.1 ng/ml), renal clearance (Clr; 19.0 l/h vs 14.2 l/h), and t1/2 (2.18 h vs 1.93 h), and shorter for tmax (0.88 h vs 1.75 h). Some accumulation (22%) occurred over the 4 days of dosing. Serum concentrations of the pharmacologically inactive indole acetic acid metabolite of sumatriptan were fourfold to fivefold higher than corresponding sumatriptan concentrations. Overall, these studies show that the sumatriptan intranasal spray formulation is well tolerated, allows rapid absorption of sumatriptan, and results in only a clinically insignificant degree of sumatriptan accumulation upon repeated dosing.
与目前可用的皮下注射和口服舒马曲坦制剂相比,鼻内给药舒马曲坦剂量在偏头痛治疗中可能会增加更大的灵活性。进行了两项独立的双盲、随机、安慰剂对照临床研究,以评估鼻内给予舒马曲坦在递增单剂量(三种不同剂量水平)和多剂量后的安全性、耐受性和药代动力学。在四交叉、递增剂量研究中,20名健康女性受试者被随机分组,在不同时间分别向一侧鼻孔给予5、10或20毫克舒马曲坦(半硫酸盐)鼻内喷雾剂量或安慰剂。不良事件轻微,主要包括喉咙后部苦味以及其他给药途径给予舒马曲坦时典型的事件(头痛、头晕和刺痛)。血浆舒马曲坦浓度-时间曲线下面积(AUC无穷大)和血浆峰浓度(Cmax)随剂量增加而升高。在5至10毫克之间显示出剂量比例关系,但在5 - 20毫克剂量范围内未显示。由于多次峰值,达最大血浆浓度时间(tmax)可变。消除半衰期(t1/2)约为2小时,不受剂量大小影响。在两期、多剂量、交叉研究中,12名健康成年男性和女性受试者被随机分组,接受20毫克舒马曲坦半硫酸盐或安慰剂,每天鼻内喷雾给药三次,共4天。两个给药期相隔3至14天。多次剂量的舒马曲坦耐受性良好,未发生严重不良事件,也没有因不良事件而停药。所有患者均报告有轻度至中度与药物相关的味觉障碍。鼻腔检查保持正常,嗅觉功能未受影响。给药后前8小时的AUC(AUC8)和尿中排泄的剂量分数(fe;6.2%对3.6%)在第1天和第4天相似。第4天的Cmax(16.9纳克/毫升对13.1纳克/毫升)、肾清除率(Clr;19.0升/小时对14.2升/小时)和t1/2(2.18小时对1.93小时)值显著更高(p≤0.05),而tmax更短(0.88小时对1.75小时)。在4天给药期间出现了一些蓄积(22%)。舒马曲坦的药理活性无的吲哚乙酸代谢物的血清浓度比相应的舒马曲坦浓度高4至5倍。总体而言,这些研究表明,舒马曲坦鼻内喷雾制剂耐受性良好,允许舒马曲坦快速吸收,并且在重复给药时仅导致临床上无显著意义的舒马曲坦蓄积程度。
