硝唑尼特单次递增口服剂量在人体中的药代动力学和耐受性

Nitazoxanide pharmacokinetics and tolerability in man using single ascending oral doses.

作者信息

Stockis A, Allemon A M, De Bruyn S, Gengler C

机构信息

SGS Biopharma S.A., Wavre, Belgium.

出版信息

Int J Clin Pharmacol Ther. 2002 May;40(5):213-20. doi: 10.5414/cpp40213.

DOI:10.5414/cpp40213

PMID:12051573

Abstract

OBJECTIVES

Nitazoxanide (N) is a new broad-spectrum intestinal antiparasitic agent. Deacetyl-N or tizoxanide (T) and its glucuronide (TG) are the major circulating species metabolites after oral administration of N. Bioavailability is substantially increased by food. The objectives of this phase IA study were to assess the tolerability and to determine the pharmacokinetic linearity of T and TG after single oral administration of increasing doses of N with and without food in healthy volunteer subjects.

METHODS

Thirty-two healthy male volunteers were randomly assigned to 1 of 4 treatment groups. In each successive group, 2 subjects received a placebo and 6 received a single oral dose of 1 g, 2 g, 3 g, or 4 g of N, first under fasted conditions and a week later with a standardized breakfast. Blood samples were collected during 24 h for plasma determination of T and TG. General tolerability, adverse reactions, ECG, vital signs and laboratory tests were recorded.

RESULTS

Tolerability was good up to the maximum dose of 4 g. Mild, mostly gastrointestinal side effects were observed and their frequency increased significantly with the dose level. No significant changes were noted in the ECGs, vital signs and laboratory tests. Plasma concentrations increased linearly with the dose from 1 - 4 g, although a trend to increased bioavailability was observed at 4 g. Food approximately doubled the concentrations of T and TG irrespective of dose. Peak times and apparent half-lives increased in proportion to the dose. The apparent body clearance for total T (T+TG) at the highest dose was only half that at the low dose. TG was eliminated more slowly than T.

CONCLUSION

Nitazoxanide can be safely administered up to 4 g single oral doses, with or without food. The slow elimination of TG and the overproportional concentrations at the highest dose can be accounted for by solubility- or transport-limited elimination mechanisms becoming apparent at the upper dose level.

摘要

目的

硝唑尼特（N）是一种新型广谱肠道抗寄生虫药。脱乙酰硝唑尼特或替唑尼特（T）及其葡萄糖醛酸苷（TG）是口服N后主要的循环代谢产物。食物可显著提高其生物利用度。本IA期研究的目的是评估健康志愿者在有或无食物的情况下单次口服递增剂量N后T和TG的耐受性，并确定其药代动力学线性。

方法

32名健康男性志愿者被随机分配到4个治疗组中的1组。在每个连续的组中，2名受试者接受安慰剂，6名受试者分别接受1 g、2 g、3 g或4 g N的单次口服剂量，首先在禁食条件下，一周后在进食标准化早餐的情况下进行。在24小时内采集血样，用于血浆中T和TG的测定。记录一般耐受性、不良反应、心电图、生命体征和实验室检查结果。

结果

高达4 g的最大剂量耐受性良好。观察到轻度的、主要是胃肠道的副作用，其频率随剂量水平显著增加。心电图、生命体征和实验室检查未见明显变化。血浆浓度在1 - 4 g剂量范围内随剂量呈线性增加，尽管在4 g时观察到生物利用度有增加的趋势。无论剂量如何，食物使T和TG的浓度增加了约一倍。达峰时间和表观半衰期与剂量成比例增加。最高剂量下总T（T + TG）的表观体内清除率仅为低剂量时的一半。TG的消除比T慢。