唑来膦酸治疗日本原发性骨质疏松症患者的安全性、药代动力学及骨代谢变化

Safety, pharmacokinetics, and changes in bone metabolism associated with zoledronic acid treatment in Japanese patients with primary osteoporosis.

作者信息

Shiraki Masataka, Tanaka Satoshi, Suzuki Hiroaki, Ueda Satoko, Nakamura Toshitaka

机构信息

Department of Internal Medicine, Research Institute and Practice for Involutional Diseases, 1610-1 Meisei, Misato, Azumino, Nagano, 399-8101, Japan.

Asahi Kasei Pharma Corporation, 1-105 Kanda, Jinbocho, Chiyoda-ku, Tokyo, 101-8101, Japan.

出版信息

J Bone Miner Metab. 2017 Nov;35(6):675-684. doi: 10.1007/s00774-016-0806-3. Epub 2016 Dec 20.

DOI:10.1007/s00774-016-0806-3

PMID:28000034

Abstract

Although once-yearly intravenous administration of zoledronic acid has been reported to inhibit bone resorption and increase bone mineral density, no studies have evaluated its effectiveness in treating osteoporosis in Japanese patients. Therefore, the purpose of this study was to investigate the pharmacokinetics and assess the safety of and changes in bone metabolism associated with zoledronic acid treatment in Japanese patients with primary osteoporosis. This was a single-administration study with a single-blind parallel-group design. The study participants were 24 Japanese patients with primary osteoporosis. The patients were divided into two groups, with each group receiving a single injection of zoledronic acid (4 or 5 mg). Pharmacokinetics and urinary excretion were then compared, and drug-related adverse events and changes in the levels of bone turnover markers were assessed at 12 months. Mean plasma concentrations of zoledronic acid peaked in both groups immediately after administration, and decreased to 1% or less of peak levels after 24 h. Noncompartmental analysis revealed that C and the area under the curve from time zero to infinity increased in proportion to the dose. The levels of bone resorption and formation markers decreased from day 15 and from 3 months after administration respectively, and suppression of these markers remained constant for the entire study period. No serious adverse events were reported. There was no large difference between the 4- and 5-mg groups in terms of pharmacokinetics, changes in the levels of bone turnover markers, and safety profiles. This study demonstrated acceptable pharmacokinetics and changes in bone metabolism associated with zoledronic acid treatment in female Japanese osteoporosis patients. Both the 4-mg dose and the 5-mg dose demonstrated acceptable safety and sustained antiresorptive effects for the duration of the study.

摘要

尽管据报道每年静脉注射一次唑来膦酸可抑制骨吸收并增加骨矿物质密度，但尚无研究评估其对日本患者骨质疏松症的治疗效果。因此，本研究的目的是调查日本原发性骨质疏松症患者使用唑来膦酸治疗后的药代动力学，并评估其安全性以及骨代谢变化。这是一项采用单盲平行组设计的单次给药研究。研究参与者为24名日本原发性骨质疏松症患者。患者被分为两组，每组接受一次唑来膦酸注射（4或5毫克）。然后比较药代动力学和尿排泄情况，并在12个月时评估药物相关不良事件以及骨转换标志物水平的变化。两组唑来膦酸的平均血浆浓度在给药后立即达到峰值，并在24小时后降至峰值水平的1%或更低。非房室分析显示，曲线下面积和从零到无穷大的曲线下面积与剂量成正比增加。骨吸收和形成标志物水平分别在给药后第15天和3个月开始下降，并且在整个研究期间这些标志物的抑制作用保持不变。未报告严重不良事件。4毫克组和5毫克组在药代动力学、骨转换标志物水平变化和安全性方面没有很大差异。本研究证明了日本女性骨质疏松症患者使用唑来膦酸治疗后具有可接受的药代动力学和骨代谢变化。4毫克剂量和5毫克剂量在研究期间均显示出可接受的安全性和持续的抗吸收作用。

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唑来膦酸治疗日本原发性骨质疏松症患者的安全性、药代动力学及骨代谢变化

Safety, pharmacokinetics, and changes in bone metabolism associated with zoledronic acid treatment in Japanese patients with primary osteoporosis.

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