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一种新型磺酰脲类药物格列喹酮(AR-DF 26)的药代动力学行为。迄今研究总结(作者译)

[Pharmacokinetic behaviour of gliquidone (AR-DF 26), a new sulfonyl urea. Summary of the studies so far (author's transl)].

作者信息

Kopitar Z, Koss F W

出版信息

Arzneimittelforschung. 1975;25(12):1933-8.

PMID:1243665
Abstract

Pharmacokinetic studies of the new antidiabetic agent gliquidone, AR-DF 26, 1-cyclohexyl-3-((p-[2-(3,4-dihydro-7-methoxy-4,4-dimethyl-1,3-dioxo-2 (1H)-isoquinolyl)-ethyl]-phenyl)-sulfonyl)-urea (Glurenorm) in healthy volunteers and patients with several diseases related to diabetes are reported. Plasma levels and excreta were monitored using the 14C-labelled compound and/or a specific radioimmunoassay. Following oral administration of a 30 mg tablet a maximal plasma level of approximately 600 ng/ml was attained after 2 to 3 h. The compound was eliminated mainly with the bile. Urinary excretion amounted to about 5% only. Comparison of diabetic patients with or without concomitant renal insufficiency did not reveal significant differences with respect to the pharmacokinetic behaviour of the drug. This holds true also for administration following a multiple dosage regimen where even three doses of 60 mg each a day, did not result in elevated blood levels in either group. AR-DF 16 is metabolized mainly to four products, which were identified besides unchanged drug in bile, stool and urine. All excreta showed quite a similar pattern of distribution. In plasma, however, unchanged drug accounted for at least 80% of total radioactivity up to 8 h besides some biotransformed products, mainly AR-DF 33.

摘要

报道了新型抗糖尿病药物格列喹酮(AR-DF 26,1-环己基-3-((对-[2-(3,4-二氢-7-甲氧基-4,4-二甲基-1,3-二氧代-2(1H)-异喹啉基)-乙基]-苯基)-磺酰基)-脲(糖适平))在健康志愿者和患有几种糖尿病相关疾病患者中的药代动力学研究。使用14C标记的化合物和/或特异性放射免疫分析法监测血浆水平和排泄物。口服30mg片剂后,2至3小时达到最大血浆水平约600ng/ml。该化合物主要经胆汁消除。尿排泄仅约占5%。比较有或无合并肾功能不全的糖尿病患者,未发现该药物的药代动力学行为有显著差异。这在多剂量给药方案中同样适用,即便是每天服用三次,每次60mg,两组患者的血药水平均未升高。AR-DF 16主要代谢为四种产物,除了在胆汁、粪便和尿液中未变化的药物外,这些产物已被鉴定。所有排泄物显示出相当相似的分布模式。然而,在血浆中,直至8小时,除了一些生物转化产物(主要是AR-DF 33)外,未变化的药物占总放射性的至少80%。

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