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Absolute bioavailability of clarithromycin after oral administration in humans.

机译:人体口服克拉霉素后的绝对生物利用度。

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摘要

The absolute bioavailability of clarithromycin, a new macrolide antimicrobial agent, was assessed in a three-way, randomized, single-dose, crossover study conducted with 22 healthy volunteers, 19 of whom provided analyzable study data. The bioavailability parameters of two 250-mg oral tablet formulations were calculated with reference to an identical dose administered by intravenous infusion of the lactobionate salt. After adjustment for formulation potency, the mean absolute bioavailabilities of the two oral formulations were 52 and 55%, on the basis of the appearance of parent compound in the systemic circulation. Metabolite peak concentration and area under the plasma concentration-time curve data after oral dosing were generally greater than those after intravenous infusion, suggesting that marked first-pass metabolism of clarithromycin occurs after oral administration. Pharmacokinetic analysis of the parent drug and the active 14-hydroxy metabolite data suggests complete (or nearly complete) absorption of the drug after oral administration.
机译:对22位健康志愿者进行的三项随机,单剂量,交叉研究评估了克拉霉素(一种新的大环内酯类抗菌剂)的绝对生物利用度。其中19名健康志愿者提供了可分析的研究数据。参考通过静脉内输注乳糖酸钙盐所给予的相同剂量,计算出两种250毫克口服片剂的生物利用度参数。在调整制剂效力后,基于母体化合物在体循环中的出现,两种口服制剂的平均绝对生物利用度分别为52和55%。口服给药后的代谢产物峰值浓度和血浆浓度-时间曲线下的面积通常大于静脉输注后的代谢产物,这表明克拉霉素的显着首过代谢发生在口服后。母体药物的药代动力学分析和活性的14-羟基代谢产物数据表明,口服后药物完全(或几乎完全)吸收。

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