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A review of minodronic acid hydrate for the treatment of osteoporosis

机译:水合米诺膦酸治疗骨质疏松症的研究进展

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摘要

Minodronic acid hydrate was the first bisphosphonate developed and approved for osteoporosis treatment in Japan. With regard to inhibition of bone resorption, minodronic acid hydrate is 1000 times more effective than etidronic acid and 10–100 times more effective than alendronic acid. Clinical trials conducted to date have focused on postmenopausal female patients suffering from primary osteoporosis. In these trials, 1 mg of oral minodronic acid hydrate was administrated once daily, and a significant increase was observed in lumbar-spine and hip-joint bone density 1–2 years after administration. All markers of bone metabolism urinary collagen type 1 cross-linked N-telopeptide, urinary free deoxypyridinoline, serum bone alkaline phosphatase, and serum osteocalcin were decreased. The incidence rate of new vertebral and nonvertebral fractures was also decreased. Therefore, effectiveness in fracture prevention was confirmed. A form of minodronic acid (50 mg) requiring once-monthly administration has been developed and is currently being used clinically. A comparative study between this new formulation and once-daily minodronic acid (1 mg) showed no significant differences between the two formulations in terms of improvement rates in lumbar-spine and hip-joint bone density, changes in bone metabolism markers, or incidence of side effects. This indicates the noninferiority of the monthly formulation. Side effects such as osteonecrosis of the jaw or atypical femoral fractures were not reported with other bisphosphonates, although it is believed that these side effects may emerge as future studies continue to be conducted. On the basis of studies conducted to date, minodronic acid hydrate is considered effective for improving bone density and preventing fractures. We anticipate further investigations in the future.
机译:米诺膦酸水合物是日本最早开发并批准用于骨质疏松症治疗的双膦酸盐。关于抑制骨吸收,水合美德龙酸的功效比乙二膦酸的功效高1000倍,比阿仑膦酸的功效高10-100倍。迄今为止进行的临床试验集中于绝经后患有原发性骨质疏松症的女性患者。在这些试验中,每天一次口服1毫克的水合美诺膦酸水合物,给药后1-2年腰椎和髋关节骨密度显着增加。骨代谢的所有标志物1型尿胶原交联的N-端肽,尿中游离的脱氧吡啶并啉,血清骨碱性磷酸酶和血清骨钙素均降低。新椎骨和非椎骨骨折的发生率也降低了。因此,确认了预防骨折的有效性。已经开发出一种需要每月一次给药的米诺膦酸(50毫克),目前正在临床上使用。这项新配方与每日一次的米诺膦酸(1 mg)的对比研究表明,两种配方在腰椎和髋关节骨密度的改善率,骨代谢标志物的变化或发生率方面无显着差异。副作用。这表明每月配方的非劣势性。其他双膦酸盐类药物未报告如颌骨坏死或不典型股骨骨折等副作用,尽管据信随着未来的研究继续进行,这些副作用可能会出现。根据迄今进行的研究,米诺膦酸水合物被认为对改善骨密度和预防骨折有效。我们预计将来会进行进一步的调查。

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