Kunka R L, Hussey E K, Shaw S, Warner P, Aubert B, Richard I, Fowler P A, Pakes G E
Glaxo Wellcome Inc., Research Triangle Park, NC 27709, USA.
Cephalalgia. 1997 Jun;17(4):532-40. doi: 10.1046/j.1468-2982.1997.1704532.x.
A suppository formulation of the 5HT1 agonist sumatriptan could prove an important therapeutic option in migraine patients who dislike or poorly tolerate injectable therapy and where oral tablet administration is unsuitable because of severe migraine-related vomiting. Two independent double-blind, randomized clinical studies were conducted to evaluate the safety, tolerability and pharmacokinetics of sumatriptan suppositories following ascending single doses (four different dose levels) and multiple doses. In the four-period, crossover, single-dose study, 24 healthy male subjects were randomized to receive a suppository containing 12.5, 25, 50, or 100 mg on separate occasions 3-14 days apart. The suppositories were generally well tolerated; transient asthenia, drowsiness, and headache were the most frequently reported adverse events, and these were not dose-related. Peak plasma concentrations (Cmax) of sumatriptan were proportional to dose from 25 to 100 mg; area under the plasma concentration-time curve (AUC infinity) values were proportional to dose except at the highest doses, when they were greater than those predicted from lower doses. For all doses, the tmax of sumatriptan occurred within 2.5 h, and the t1/2 was approximately 2 h. In the two-period, placebo-controlled, crossover, repeat-dose study, 12 healthy adult male subjects were randomized to receive either a 50-mg sumatriptan suppository or placebo suppository, administered rectally twice a day, for 11 doses (5 1/2 days). Adverse events were no more frequent with sumatriptan than with placebo, and stool guaiac, rectal examinations, and physical examinations remained normal. No significant differences were noted between Day 1 and Day 6 values in the AUC, Cmax, time of peak serum concentration (tmax), elimination half-life (t 1/2), fraction of the dose excreted in the urine (fe), or renal clearance (Clr) of sumatriptan or its pharmacologically inactive indole acetic acid metabolite. Serum metabolite concentrations were two to three-fold higher than corresponding sumatriptan concentrations. No clinically significant accumulation of sumatriptan or its metabolite occurred. Overall, these studies show that sumatriptan administration via a suppository formulation is well tolerated, allows rapid absorption of sumatriptan, results in sumatriptan Cmax values that are proportional to dose from 25 to 100 mg, and is not associated with accumulation of sumatriptan or its metabolite.
对于不喜欢或难以耐受注射疗法且因严重偏头痛相关呕吐而不适于口服片剂给药的偏头痛患者,5-羟色胺1(5HT1)激动剂舒马曲坦的栓剂制剂可能是一种重要的治疗选择。进行了两项独立的双盲、随机临床研究,以评估舒马曲坦栓剂在递增单剂量(四个不同剂量水平)和多剂量后的安全性、耐受性和药代动力学。在为期四个阶段的交叉单剂量研究中,24名健康男性受试者被随机分组,在间隔3 - 14天的不同时间分别接受含12.5、25、50或100毫克的栓剂。这些栓剂总体耐受性良好;短暂乏力、嗜睡和头痛是最常报告的不良事件,且与剂量无关。舒马曲坦的血浆峰浓度(Cmax)在25至100毫克范围内与剂量成正比;血浆浓度-时间曲线下面积(AUC无穷大)值除最高剂量外与剂量成正比,最高剂量时的值大于较低剂量预测的值。对于所有剂量,舒马曲坦的达峰时间(tmax)在2.5小时内出现,半衰期(t1/2)约为2小时。在为期两个阶段的安慰剂对照交叉重复剂量研究中,12名健康成年男性受试者被随机分组,接受50毫克舒马曲坦栓剂或安慰剂栓剂,每天直肠给药两次,共11剂(5.5天)。舒马曲坦组的不良事件发生率并不高于安慰剂组,粪便隐血、直肠检查和体格检查均保持正常。舒马曲坦或其无药理活性的吲哚乙酸代谢物的AUC、Cmax、血清峰浓度时间(tmax)、消除半衰期(t1/2)、尿中排泄剂量分数(fe)或肾清除率(Clr)在第1天和第6天的值之间未观察到显著差异。血清代谢物浓度比相应的舒马曲坦浓度高两到三倍。舒马曲坦或其代谢物未出现临床上显著的蓄积。总体而言,这些研究表明,通过栓剂制剂给药的舒马曲坦耐受性良好,能使舒马曲坦快速吸收,舒马曲坦的Cmax值在25至100毫克范围内与剂量成正比,且与舒马曲坦或其代谢物的蓄积无关。
