二嗪的药代动力学:低生物利用度,通过食物摄入改善。

Drug-nutrient interactions Pub Date : 1985-01-01
H Liedholm, A Lidén, L Kroon, A Melander, E Wåhlin-Boll
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引用次数: 0

摘要

精神药物吩噻嗪二嗪的单剂量动力学在8名年轻健康志愿者中进行了评估,在三种情况下给予药物:静脉注射10mg,空腹状态下口服25mg,以及口服25mg,同时标准早餐为1840 kJ。采用高压液相色谱法测定血药浓度。与其他亲脂性弱碱性药物一样,二嗪在血浆中消失迅速,消除半衰期为3.4 h,清除率约为1200 ml/min,表观分布容积为5.9 l/kg。发现二嗪的生物利用度非常低且个体间变化;在禁食状态下,二嗪的生物利用度在1名受试者中仅为1%,在其他5名受试者中为3-6%,在其余2名受试者中为11%和24%。平均空腹生物利用度为7.4%。早餐摄入后,平均生物利用度提高至12.4% (p < 0.01),范围为2 ~ 29%。口服生物利用度低可能是由于广泛的系统前(肝脏)降解,而食物效应减少了这一过程。
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Pharmacokinetics of dixyrazine: low bioavailability, improved by food intake.

The single-dose kinetics of the psychotropic phenothiazine dixyrazine was assessed in eight young healthy volunteers given the drug at three occasions: 10 mg intravenously, 25 mg orally in the fasting state, and 25 mg orally together with a standardized breakfast of 1,840 kJ. The plasma concentrations of dixyrazine were measured by high-pressure liquid chromatography. Like some other lipophilic weakly basic drugs, dixyrazine showed a rapid disappearance from plasma, having an elimination half-life of 3.4 h, a clearance of about 1,200 ml/min, and an apparent volume of distribution of 5.9 l/kg. Dixyrazine was found to have a very low and interindividually varying bioavailability; in the fasting state, dixyrazine bioavailability was only 1% in one subject, 3-6% in five others, and 11 and 24% in the remaining two subjects. The mean fasting bioavailability was 7.4%. After intake with breakfast, the mean bioavailability was increased to 12.4% (p less than 0.01), with a range of 2-29%. Probably, the low oral bioavailability is due to extensive presystemic (hepatic) degradation, and the food effect to a reduction of this process.

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