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芬喹宗在健康志愿者中的单剂量药代动力学。

Single-dose pharmacokinetics of fenquizone in healthy volunteers.

作者信息

Maggi G C, Donati C, Gueli Alletti D

出版信息

Arzneimittelforschung. 1985;35(6):994-8.

PMID:4026929
Abstract

A pharmacokinetic study of fenquizone (Idrolone), a thiazide-like diuretic, was conducted with single oral doses in 6 healthy volunteers. The substance thus administered was readily absorbed from the gut, with peak plasma levels being detected on average at 3 h after dosing; after that, plasma concentrations of fenquizone decreased biexponentially in a pattern fitting an open two-compartment model. Plasma half-life values were 1 h for phase alpha and 17 h for phase beta. The half-life calculated from urinary concentrations was 18 h. The apparent distribution volume for phase beta was 686 l; renal clearance was 220 ml/min, and the absorption constant (Ka) was 1055 h-1. Cumulative urinary excretion accounted for 53.1% of the administered dose in 72 h. Thus the pharmacokinetic profile of fenquizone was that of an "intermediate-acting" diuretic about half-way between the short-acting hydrochlorothiazide, chlorothiazide and furosemide and the long-acting chlorthalidone. In summation, fenquizone is described as a low-dosage diuretic apparently not conducive to accumulation; its pharmacokinetic profile qualifies the product particularly well for maintenance therapy, such as is needed for the management of essential hypertension, both as sole medication and in fixed-ratio combination with beta-blockers, and at any rate with once-a-day administration.

摘要

对6名健康志愿者单次口服噻嗪类利尿剂芬喹宗(Idrolone)进行了药代动力学研究。口服给药后,该物质很容易从肠道吸收,给药后平均3小时检测到血浆峰值浓度;之后,芬喹宗的血浆浓度呈双指数下降,符合开放二室模型。α相血浆半衰期值为1小时,β相为17小时。根据尿浓度计算的半衰期为18小时。β相的表观分布容积为686升;肾清除率为220毫升/分钟,吸收常数(Ka)为1055小时-1。72小时内累积尿排泄量占给药剂量的53.1%。因此,芬喹宗的药代动力学特征表明它是一种“中效”利尿剂,其作用时长约介于短效的氢氯噻嗪、氯噻嗪和呋塞米与长效的氯噻酮之间。总之,芬喹宗被描述为一种低剂量利尿剂,显然不易蓄积;其药代动力学特征使其非常适合维持治疗,例如原发性高血压的治疗,既可以作为单一药物,也可以与β受体阻滞剂按固定比例联合使用,无论如何都可以每日给药一次。

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