Paquette Jean-Michel, Rufiange Marianne, Iovu Niculita Mirela, Massicotte Julie, Lefebvre Marc, Colin Patrick, Telmat Ariles, Ranger Maxime
Algorithme Pharma Inc, Laval, Quebec, Canada.
gIcare Pharma Inc, Montreal, Quebec, Canada.
Clin Ther. 2014 Nov 1;36(11):1650-64. doi: 10.1016/j.clinthera.2014.08.005. Epub 2014 Sep 15.
Trimebutine 3-thiocarbamoylbenzenesulfonate (GIC-1001) is a new drug intended to be used for the management of visceral pain in patients undergoing sedation-free, full colonoscopy. The objectives of this Phase I, single-center, randomized, double-blinded, placebo-controlled, integrated study were to evaluate the safety and pharmacokinetics of GIC-1001 after single ascending doses (SAD) and multiple ascending doses (MAD) and to evaluate the influence of food on the pharmacokinetics in healthy volunteers.
GIC-1001 or placebo was orally administered to 80 healthy male and female subjects (non- or ex-smokers) aged 18 to 50 years with a body mass index between 18.5 and 30 kg/m(2). The SAD portion of the study consisted of 5 cohorts with dose levels of 125 to 1000 mg. The MAD portion included 4 cohorts in which subjects received TID doses of 125 to 500 mg over 7 days (19 consecutive doses). Subjects were randomized (6:2) to receive GIC-1001 or placebo. The third portion of the study included a single 375-mg dose of GIC-1001 in a randomized, 2-period, crossover design to assess the influence of food (n = 8 subjects). Safety was evaluated by using adverse events (AEs), vital signs, ECGs, physical examination, cardiac monitoring, and laboratory test results. The analytes were assayed by using validated HPLC-MS/MS methods. Pharmacokinetic parameters were evaluated by using a noncompartmental analysis, and regression models were used to assess dose linearity. To evaluate the effect of food, 90% CIs of the ratio of geometric least squares means from ln-transformed pharmacokinetic parameters were calculated.
The most frequently reported drug-related AEs were of nervous system and gastrointestinal origin. The most common AEs included headache, somnolence, and nausea. After single-dose administration, Tmax of trimebutine ranged from 1.0 to 1.5 hours. Cmax and AUCT were linear (nonlinearity P ≥ 0.05) and proportional (P < 0.05) over the studied dose range. Food increased the Cmax and AUC of trimebutine; the ratio of geometric least squares means (90% CI) were 140% (84-234) and 174% (138-221), respectively. In the MAD study portion, the Tmax of trimebutine ranged from 0.5 to 2 hours and AUCτ increased from 38 to 170 ng · h/mL. AUCτ and Cmax were linear and proportional over the studied dose range.
GIC-1001 was well tolerated, and its safety profile was similar to that of placebo. Pharmacokinetics of GIC-1001 and its metabolites were mainly linear and proportional over the studied dose ranges. Steady state was generally considered to be reached after 3 days. Food consumption affected the pharmacokinetic profile of the analytes differently. (ClinicalTrials.gov identifier: NCT01738425.).
曲美布汀3-硫代氨基甲酰基苯磺酸盐(GIC-1001)是一种新药,旨在用于管理在未使用镇静剂的全结肠镜检查患者中的内脏疼痛。这项I期单中心、随机、双盲、安慰剂对照、综合研究的目的是评估单次递增剂量(SAD)和多次递增剂量(MAD)后GIC-1001的安全性和药代动力学,并评估食物对健康志愿者药代动力学的影响。
将GIC-1001或安慰剂口服给予80名年龄在18至50岁之间、体重指数在18.5至30kg/m²之间的健康男性和女性受试者(非吸烟者或曾经吸烟者)。该研究的SAD部分包括5个队列,剂量水平为125至1000mg。MAD部分包括4个队列,受试者在7天内接受每日三次剂量为125至500mg的给药(共19次连续给药)。受试者被随机分组(6:2)接受GIC-1001或安慰剂。该研究的第三部分包括在随机、2期交叉设计中给予单次375mg剂量的GIC-1001,以评估食物的影响(n = 8名受试者)。通过不良事件(AE)、生命体征、心电图、体格检查、心脏监测和实验室检查结果来评估安全性。使用经过验证的HPLC-MS/MS方法测定分析物。通过非房室分析评估药代动力学参数,并使用回归模型评估剂量线性。为了评估食物的影响,计算了来自经ln转换的药代动力学参数的几何最小二乘均值比值的90%置信区间。
最常报告的与药物相关的AE起源于神经系统和胃肠道。最常见的AE包括头痛、嗜睡和恶心。单次给药后,曲美布汀的Tmax范围为1.0至1.5小时。在所研究的剂量范围内,Cmax和AUCT呈线性(非线性P≥0.05)且成比例(P<0.05)。食物增加了曲美布汀的Cmax和AUC;几何最小二乘均值比值(90%置信区间)分别为140%(84-234)和174%(138-221)。在MAD研究部分,曲美布汀的Tmax范围为0.5至2小时,AUCτ从38增加到170ng·h/mL。在所研究的剂量范围内,AUCτ和Cmax呈线性且成比例。
GIC-1001耐受性良好,其安全性与安慰剂相似。在研究的剂量范围内,GIC-1001及其代谢物的药代动力学主要呈线性且成比例。一般认为3天后达到稳态。食物摄入对分析物的药代动力学特征有不同影响。(ClinicalTrials.gov标识符:NCT01738425.)
