Pharmacokinetic, bioavailability and pharmacodynamic study of indobufen (K 3920), an inhibitor of platelet aggregation, after a single dose in man.

IF 2.4 3区医学 Q3 PHARMACOLOGY & PHARMACY

European Journal of Clinical Pharmacology Pub Date : 1979-06-12 DOI:10.1007/BF00558435

L M Fuccella, G Corvi, E Moro, E Pogliani, V Tamassia, G Tosolini

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引用次数: 10

Abstract

Six healthy volunteers received single iv and oral doses of 2-[p-(1-oxo-2-isoindolinyl)phenyl] butyric acid 100 mg (indobufen; K 3920), an inhibitor of platelet aggregation. Plasma levels and urinary excretion of the drug were determined by GLC. Collagen-induced platelet aggregation was assessed turbidimetrically at various intervals after administration. The plasma half-life of the drug was 7--8 h and more than 70% of the administered dose was recovered within 48 h in urine, as unchanged drug and as the glucuronide of indobufen. After oral administration of tablets of two different formulations, the drug was completely absorbed, but one formulation showed faster absorption. The maximal inhibitory effect on platelet aggregation was observed 1 to 4 h after iv administration, and it had decreased by 8h. After tablets, peak effect and the time of the peak were similar, but activity was significantly prolonged, in accordance with the higher plasma levels found at 8 h. The data suggest that the effect of indobufen on platelets is reversible, and that for this drug platelets behave as a compartment that slowly equilibrates with plasma.

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血小板聚集抑制剂indobufen (k3920)单次给药后的药代动力学、生物利用度和药效学研究

6名健康志愿者接受单次静脉注射和口服剂量的2-[对-(1-氧-2-异吲哚啉基)苯基]丁酸100毫克(吲哚芬;K 3920)，一种血小板聚集抑制剂。GLC法测定该药物的血浆水平和尿排出量。在给药后的不同时间间隔用浊度法评估胶原诱导的血小板聚集。该药物的血浆半衰期为7- 8小时，超过70%的给药剂量在48小时内从尿液中恢复，作为不变药物和吲哚布芬的葡萄糖醛酸盐。口服两种不同剂型的片剂后，药物完全吸收，但其中一种剂型吸收更快。对血小板聚集的抑制作用在静脉给药后1 ~ 4 h达到最大，8h后下降。服药后，峰效应和峰时间相似，但活性明显延长，与8小时时发现的较高血浆水平一致。数据表明，吲哚布芬对血小板的影响是可逆的，对于这种药物，血小板表现为一个与血浆缓慢平衡的隔室。

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来源期刊

European Journal of Clinical Pharmacology 医学-药学

CiteScore

5.40

自引率

3.40%

发文量

170

审稿时长

3-8 weeks

期刊介绍： The European Journal of Clinical Pharmacology publishes original papers on all aspects of clinical pharmacology and drug therapy in humans. Manuscripts are welcomed on the following topics: therapeutic trials, pharmacokinetics/pharmacodynamics, pharmacogenetics, drug metabolism, adverse drug reactions, drug interactions, all aspects of drug development, development relating to teaching in clinical pharmacology, pharmacoepidemiology, and matters relating to the rational prescribing and safe use of drugs. Methodological contributions relevant to these topics are also welcomed. Data from animal experiments are accepted only in the context of original data in man reported in the same paper. EJCP will only consider manuscripts describing the frequency of allelic variants in different populations if this information is linked to functional data or new interesting variants. Highly relevant differences in frequency with a major impact in drug therapy for the respective population may be submitted as a letter to the editor. Straightforward phase I pharmacokinetic or pharmacodynamic studies as parts of new drug development will only be considered for publication if the paper involves -a compound that is interesting and new in some basic or fundamental way, or -methods that are original in some basic sense, or -a highly unexpected outcome, or -conclusions that are scientifically novel in some basic or fundamental sense.