Lal Ritu, Sukbuntherng Juthamas, Luo Wendy, Chen Dan, Vu Amanda, Tovera James, Cundy Kenneth C
XenoPort, Inc., Santa Clara, California 95051, USA.
Clin Ther. 2009 Aug;31(8):1776-86. doi: 10.1016/j.clinthera.2009.07.026.
Gabapentin enacarbil is an actively transported prodrug of gabapentin that provides predictable dose-proportional gabapentin exposure with high (> or =68%) oral bioavailability.
The aims of this study were to investigate the pharmacokinetics and tolerability of gabapentin enacarbil up to supratherapeutic doses and the effects of gabapentin enacarbil on cardiac repolarization in healthy volunteers, and to provide a dose reference for a future definitive QT/corrected QT (QTc) study.
This was a randomized-sequence, double-blind, placebo-controlled, single escalating-dose, crossover study of gabapentin enacarbil 600-mg extended-release tablets administered as a single oral dose of 2400, 3600, 4800, or 6000 mg or placebo, with a 1-week washout between administrations. Blood samples were collected over a period of 36 hours after administration and were analyzed using a validated method of liquid chromatography/tandem mass spec-trometry. Blood gabapentin enacarbil and gabapentin concentrations were analyzed using noncompartmental methods. Tolerability was assessed by monitoring adverse events (AEs) (using subject interview/reporting), laboratory parameters, vital sign measurements, and 12-lead electrocardiography (ECG). Holter ECG was also performed.
Thirty-two healthy volunteers were included in the study (18 women, 14 men; mean [SD] age, 31.2 [11.4] years; body mass index, 24.9 [3.04] kg/m(2)). Gabapentin enacarbil was converted rapidly to gaba-pentin after absorption. Gabapentin exposure in blood was proportional to gabapentin enacarbil dose over the range of 2400 to 6000 mg (1250-3125 mg-equivalent gabapentin). Blood concentrations of intact gabapen-tin enacarbil were low and transient (< or =0.5% of the released gabapentin concentration at all doses). The most commonly reported AEs were dizziness and nausea (50% and 25% of subjects, respectively). All but 4 AEs were mild to moderate in intensity. Two subjects experienced treatment-emergent AEs rated as severe: psychomotor retardation, vertigo, and sedation (4800-mg dose) and somnolence (6000 mg). All treatment-emergent AEs resolved without medical intervention. No serious AEs were reported, and none of the AEs led to study withdrawal. There were no clinically significant changes in laboratory parameters, vital sign measurements, or ECG values; QTc intervals did not exceed 480 msec or change from baseline >30 msec at any gabapentin enacarbil dose.
Gabapentin enacarbil was associated with dose-proportional gabapentin exposure at doses up to 6000 mg and was generally well tolerated in these healthy subjects. These findings support the use of 6000-mg gabapentin enacarbil in a definitive QT/QTc study.
加巴喷丁依那卡比是加巴喷丁的一种主动转运前体药物,能提供可预测的剂量比例性加巴喷丁暴露量,口服生物利用度高(≥68%)。
本研究的目的是调查加巴喷丁依那卡比直至超治疗剂量的药代动力学和耐受性,以及加巴喷丁依那卡比对健康志愿者心脏复极化的影响,并为未来确定的QT/校正QT(QTc)研究提供剂量参考。
这是一项随机序列、双盲、安慰剂对照、单剂量递增、交叉研究,将加巴喷丁依那卡比600毫克缓释片作为单次口服剂量2400、3600、4800或6000毫克或安慰剂给药,给药间隔1周洗脱期。给药后36小时内采集血样,采用经验证的液相色谱/串联质谱法进行分析。采用非房室模型方法分析血中加巴喷丁依那卡比和加巴喷丁浓度。通过监测不良事件(AEs)(通过受试者访谈/报告)、实验室参数、生命体征测量和12导联心电图(ECG)评估耐受性。还进行了动态心电图监测。
32名健康志愿者纳入研究(18名女性,14名男性;平均[标准差]年龄,31.2[11.4]岁;体重指数,24.9[3.04]kg/m²)。加巴喷丁依那卡比吸收后迅速转化为加巴喷丁。在2400至6000毫克(1250 - 3125毫克等效加巴喷丁)范围内,血中加巴喷丁暴露量与加巴喷丁依那卡比剂量成比例。完整加巴喷丁依那卡比的血药浓度较低且短暂(在所有剂量下均≤释放的加巴喷丁浓度的0.5%)。最常报告的不良事件是头晕和恶心(分别为50%和25%的受试者)。除4例不良事件外,所有不良事件强度均为轻度至中度。2名受试者出现治疗中出现的严重不良事件:精神运动迟缓、眩晕和镇静(4800毫克剂量)以及嗜睡(6000毫克)。所有治疗中出现的不良事件无需医疗干预即可缓解。未报告严重不良事件,且无不良事件导致研究中止。实验室参数、生命体征测量或心电图值无临床显著变化;在任何加巴喷丁依那卡比剂量下,QTc间期均未超过480毫秒或较基线变化>30毫秒。
加巴喷丁依那卡比在高达6000毫克剂量时与剂量比例性加巴喷丁暴露相关,在这些健康受试者中总体耐受性良好。这些发现支持在确定的QT/QTc研究中使用6000毫克加巴喷丁依那卡比。
