van Troostenburg A R, Clark E V, Carey W D H, Warrington S J, Kerns W D, Cohn I, Silverman M H, Bar-Yehuda S, Fong K L L, Fishman P
HMR, Central Middlesex Hospital, London, UK.
Int J Clin Pharmacol Ther. 2004 Oct;42(10):534-42. doi: 10.5414/cpp42534.
To assess safety, tolerability, pharmacokinetics and hemodynamic effects of oral CF 101, an A3 adenosine receptor (A3AR) agonist, in healthy men.
One single and 1 repeated dose, parallel-group, ascending dose, double-blind and placebo-controlled study in normal volunteers. In the single dose study, n = 15 subjects received 1, 5 or 10 mg oral CF101; in each group 1 subject received placebo, the remainder active CF101. In the repeat-dose study, n = 28 subjects received repeated 12-hourly oral doses of CF 101 (2, 3, 4 or 5 mg) for 7 days, in each group 2 subjects received placebo, the remainder active CF101. TEST MATERIALS: Single-dose study: CF101 in 30% Cremophor RH40. Multiple-dose sudy: CF101 in 0.5% methylcellulose suspension. Both studies: the corresponding vehicles were used as placebos. Galenicals were prepared remotely from the clinical study site to ensure double-blind nature of the study. RESULTS TOLERABILITY: Single doses up to 5 mg CF101 were safe and well-tolerated. However, the single dose of 10 mg CF101 was associated with flushing, tachycardia, nausea and vomiting, which were viewed as dose-limiting in normal volunteers. Single doses of CF101 (as well as the first of the multiple doses) were associated with increases in heart rate (8 - 24 beats/min after 5 mg and 18 - 55 beats/min after 10 mg). Multiple doses up to 4 mg 12-hourly for 7 days were safe and well-tolerated. However, the 5 mg multiple-dose group reported headache, drowsiness, hot flushes and dizziness on standing; this declined with dosing duration and was not dose-limiting in this study. Adverse events were commonest near t(max). RESULTS PHARMACOKINETICS: For oral CF101, the t(max) was always 1 - 2 h post-dose and t 1/2 about 9 h, in both the single- and multiple-dose studies. For a single 5 mg dose (mean +/- SD) C(max) = 81.6 +/- 23.6 ng/ml in the single dose study, and 63.6 +/- 22.0 ng/ml after the first of the multiple doses; AUC if was 904.0 +/- 221.9 ng.h/ml and 596.1 +/- 196.6 ng.h/ml for the 2 studies, respectively. After 7 days of multiple dosing there was little change, and AUC(0-24h) = 601.0 +/- 163.6 ng.h/ml. These pharmacokinetic parameters were linearly proportional to dose in the other treatment groups. RESULTS PHARMACODYNAMICS: Increases in heart rate were related to plasma concentration and evident only in the upper range of concentrations observed. There were no changes on ECG monitoring beyond sinus tachycardia, and, in particular, no evidence of PR prolongation in any subject (n = 43). In comparison with single doses, this response was almost absent after 7 days of dosing. Leucocytosis (increases up to about 1.5 x 10(9)/l after 5 and 10 mg) was similarly transient and reversible after multiple dosing.
Single oral doses up to 5 mg CF101 and repeated doses up to 4 mg 12-hourly for 7 days were safe and well-tolerated. Multiple-dose CF101 pharmacokinetics were unchanged and predictable from single-dose estimates, and were linearly proportional to dose. Increases in heart rate and neutrophil count were reversible during multiple dosing and were not dose-limiting in the repeat dose study. CF101 warrants further study for its efficacy in treating human disease.
评估口服CF 101(一种A3腺苷受体(A3AR)激动剂)在健康男性中的安全性、耐受性、药代动力学和血流动力学效应。
在正常志愿者中进行一项单剂量和1次重复剂量、平行组、递增剂量、双盲和安慰剂对照研究。在单剂量研究中,n = 15名受试者接受1、5或10 mg口服CF101;每组1名受试者接受安慰剂,其余接受活性CF101。在重复剂量研究中,n = 28名受试者每12小时重复口服CF 101(2、3、4或5 mg),共7天,每组2名受试者接受安慰剂,其余接受活性CF101。试验材料:单剂量研究:CF101溶于30%聚氧乙烯蓖麻油RH40。多剂量研究:CF101溶于0.5%甲基纤维素混悬液。两项研究:相应的赋形剂用作安慰剂。草药制剂在远离临床研究地点制备,以确保研究的双盲性质。结果耐受性:高达5 mg CF101的单剂量是安全且耐受性良好的。然而,10 mg CF101的单剂量与潮红、心动过速、恶心和呕吐有关,这些在正常志愿者中被视为剂量限制因素。CF101的单剂量(以及多剂量中的首次剂量)与心率增加有关(5 mg后心率增加8 - 24次/分钟,10 mg后增加18 - 55次/分钟)。每12小时重复给予高达4 mg的剂量,共7天,是安全且耐受性良好的。然而,5 mg多剂量组报告有头痛、嗜睡、潮热和站立时头晕;随着给药持续时间,这种情况有所下降,在本研究中不是剂量限制因素。不良事件在t(max)附近最为常见。结果药代动力学:对于口服CF101,在单剂量和多剂量研究中,t(max)始终在给药后1 - 2小时,t 1/2约为9小时。对于单次5 mg剂量(平均值±标准差),在单剂量研究中C(max) = 81.6 ± 23.6 ng/ml,在多剂量中的首次剂量后为63.6 ± 22.0 ng/ml;两项研究的AUC分别为904.0 ± 221.9 ng.h/ml和596.1 ± 196.6 ng.h/ml。多次给药7天后变化不大,AUC(0 - 24h) = 601.0 ± 163.6 ng.h/ml。这些药代动力学参数在其他治疗组中与剂量呈线性比例关系。结果药效动力学:心率增加与血浆浓度相关,且仅在观察到的浓度上限范围内明显。心电图监测除窦性心动过速外无变化,特别是在任何受试者(n = 43)中均无PR间期延长的证据。与单剂量相比,给药7天后这种反应几乎消失。多次给药后白细胞增多(5和10 mg后增加高达约1.5×10⁹/l)同样是短暂且可逆的。
高达5 mg CF101的单次口服剂量和每12小时重复给予高达4 mg的剂量,共7天,是安全且耐受性良好的。多剂量CF101的药代动力学不变,可根据单剂量估计预测,且与剂量呈线性比例关系。多次给药期间心率和中性粒细胞计数的增加是可逆的,在重复剂量研究中不是剂量限制因素。CF101在治疗人类疾病方面的疗效值得进一步研究。
