Ino Hiroko, Takahashi Naoki, Terao Takumi, Mudd Paul N, Hirama Toshiyasu
Medicines Development, Japan Development & Medical Affairs Division, GlaxoSmithKline K.K., TokyoJapan.
Biomedical Data Sciences Department, GlaxoSmithKline K.K., TokyoJapan.
J Drug Assess. 2013 Jul 24;2(1):87-93. doi: 10.3109/21556660.2013.827117. eCollection 2013.
Fabry disease is a rare X-linked disease caused by mutations to the GLA gene, resulting in a deficiency of the lysosomal enzyme alpha-galactosidase A. This study evaluated the pharmacokinetics, safety, and tolerability of ascending single doses of oral migalastat hydrochloride (HCl), an investigational drug, in healthy Japanese volunteers.
In this phase I, randomized, placebo-controlled, single-blind, ascending single-dose, cross-over study, migalastat HCl (50 mg, 150 mg, or 450 mg) or placebo was administered orally to 14 fasting male Japanese volunteers (aged 20-55 years) on 4 non-consecutive days. Main plasma and urine pharmacokinetic end-points included maximum observed plasma concentration (C max), time to C max (t max), area under the plasma concentration-time curve (AUC), apparent terminal-phase half-life (t 1/2), urinary recovery of unchanged drug, renal clearance, and percentage of drug excreted in urine. Safety end-points included adverse events, clinical signs and symptoms (e.g., hematology, chemistry, and urinalysis), vital signs (blood pressure and heart rate), and 12-lead electrocardiogram.
ClinicalTrials.gov registration identifier is NCT01853852.
Median t max of migalastat was 3.0-3.5 h. Migalastat HCl concentrations declined relatively rapidly, with a mean t 1/2 of 3.2-4.0 h. The amount of migalastat HCl recovered in the urine and the percentage of migalastat HCl excreted unchanged over 24 h were consistent (∼45-50%) across the dose range. The AUC and C max of migalastat HCl were dose proportional from 50-450 mg. Safety results were similar to those observed in non-Japanese populations.
This study demonstrated that ascending single doses of migalastat HCl (50 mg, 150 mg, 450 mg) are absorbed at a moderate rate and eliminated relatively rapidly, with a safety profile consistent with that observed in non-Japanese populations. These results confirm the dose-proportional pharmacokinetics of migalastat HCl from 50-450 mg. This study was limited by a small subject population and a short-term follow-up.
法布里病是一种罕见的X连锁疾病,由GLA基因突变引起,导致溶酶体酶α-半乳糖苷酶A缺乏。本研究评估了递增单剂量口服研究药物盐酸米加司他在健康日本志愿者中的药代动力学、安全性和耐受性。
在这项I期、随机、安慰剂对照、单盲、递增单剂量、交叉研究中,14名空腹的日本男性志愿者(年龄20 - 55岁)在4个非连续日口服盐酸米加司他(50毫克、150毫克或450毫克)或安慰剂。主要血浆和尿液药代动力学终点包括观察到的最大血浆浓度(Cmax)、达到Cmax的时间(tmax)、血浆浓度-时间曲线下面积(AUC)、表观终末相半衰期(t1/2)、原形药物的尿回收率、肾清除率以及尿中排泄药物的百分比。安全性终点包括不良事件、临床体征和症状(如血液学、化学和尿液分析)、生命体征(血压和心率)以及12导联心电图。
ClinicalTrials.gov注册标识符为NCT01853852。
米加司他的中位tmax为3.0 - 3.5小时。盐酸米加司他浓度下降相对较快,平均t1/2为3.2 - 4.0小时。在整个剂量范围内,尿中回收的盐酸米加司他量以及24小时内原形排泄的盐酸米加司他百分比一致(约45 - 50%)。盐酸米加司他的AUC和Cmax在50 - 450毫克范围内与剂量成正比。安全性结果与在非日本人群中观察到的结果相似。
本研究表明,递增单剂量的盐酸米加司他(50毫克、150毫克、450毫克)吸收速率适中,消除相对较快,安全性与在非日本人群中观察到的一致。这些结果证实了盐酸米加司他在50 - 450毫克范围内的剂量成正比药代动力学。本研究受受试者数量少和随访时间短的限制。
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