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Pharmacokinetic and pharmacodynamic evaluation of intermittent versus continuous alendronate administration in rats.

机译:大鼠间歇和连续阿仑膦酸盐给药的药代动力学和药效学评价。

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We studied the differences in pharmacokinetics and pharmacodynamics of the same dose of alendronate administered subcutaneously as intermittent bolus injection or continuous infusion in rats. Two rat models of bone disease were applied. Bone cancer was produced by intratibial inoculation of Walker carcinosarcoma cells, and a model of augmented bone resorption was produced by vitamin D(3) treatment of rats that had undergone thyroidparathyroidectomy. Higher amounts of alendronate were found in bones and in internal organs after bolus drug administration as compared with continuous infusion. Drug effects on plasma calcium levels and on urine calcium excretion were similar in both modes of alendronate administration. Results of the study indicate that the pharmacokinetics (disposition) of alendronate is administration-dependent. The total amount found in bone does not directly represent the amount of alendronate that is pharmacologically active at the site of action in the bone and that affects bone remodeling. The findings suggest that there is no pharmacodynamic advantage for continuous infusion of alendronate. It is concluded that the preferred mode of administration should be selected according to secondary clinical criteria (like incidence of adverse effects and convenience of administration).
机译:我们研究了大鼠皮下注射间歇给药或连续输注相同剂量阿仑膦酸盐的药代动力学和药效学的差异。应用了两种大鼠骨疾病模型。胫骨内接种沃克癌肉瘤细胞可产生骨癌,而维生素D(3)处理已进行甲状腺副甲状腺切除术的大鼠可产生骨吸收增加的模型。与连续输注相比,推注药物后在骨骼和内部器官中发现了更高含量的阿仑膦酸盐。在两种阿仑膦酸盐给药方式中,药物对血浆钙水平和尿钙排泄的影响相似。研究结果表明,阿仑膦酸盐的药代动力学(性状)与给药有关。骨骼中发现的总量并不直接代表在骨骼中作用部位具有药理活性并影响骨骼重塑的阿仑膦酸盐的量。这些发现表明,连续输注阿仑膦酸盐没有药效学优势。结论是,应根据二级临床标准(如不良反应的发生和给药的便利性)选择首选的给药方式。

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