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首页> 外文期刊>Current medical research and opinion >Sustained vertebral antifracture efficacy of oral anti-osteoporotic therapies in postmenopausal osteoporosis.
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Sustained vertebral antifracture efficacy of oral anti-osteoporotic therapies in postmenopausal osteoporosis.

机译:口服抗骨质疏松疗法在绝经后骨质疏松症中持续的椎体抗骨折疗效。

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摘要

OBJECTIVE: Vertebral fractures are common in women with postmenopausal osteoporosis, a chronic condition requiring long-term treatment with anti-osteoporotic treatments. Therefore, it is important to assess sustainability of antifracture efficacy. METHODS: A review of the literature to determine pivotal vertebral fracture studies for oral bisphosphonates (ibandronate, risedronate and alendronate), strontium ranelate, and raloxifene and to evaluate vertebral antifracture efficacy over time. RESULTS: Data from the BONE trial showed that ibandronate sustained vertebral antifracture efficacy over time (58% vertebral fracture risk reduction in first year p = 0.0561, increased to 62% for years 0-3; p < 0.001). The Vertebral Efficacy with Risedronate Therapy-North America (VERT-NA) and VERT-multi-national (VERT-MN) studies demonstrated that the relative risk reduction (RRR) with risedronate versus placebo decreased over time (VERT-NA: 65% for first year to 41% for years 0-3; VERT-MN: 61% for first year to 49% for years 0-3). Data from the Fracture Intervention Trial (FIT) I trial with alendronate showed that the RRR in the cumulative incidence of new vertebral fractures versus placebo decreased from 62% for years 0-2 to 47% for years 0-3. Similar decreases in RRR over time were reported with strontium ranelate in the Spinal Osteoporosis Therapeutic Intervention study (SOTI; 49% for first year to 33% for years 0-4) and Treatment of Peripheral Osteoporosis Study (TROPOS; 45% for first year to 24% for years 0-5). No clear trend exists for sustained efficacy over time with raloxifene. CONCLUSIONS: Vertebral fracture protection could be interpreted to decrease over time with alendronate, risedronate and strontium ranelate, and may be due to multiple factors. Ibandronate sustained vertebral antifracture efficacy over time.
机译:目的:椎骨骨折常见于绝经后骨质疏松症的妇女,这是一种慢性病,需要长期接受抗骨质疏松症治疗。因此,评估抗骨折疗效的可持续性很重要。方法:文献综述,以确定口服双膦酸盐(伊班膦酸盐,利塞膦酸盐和阿仑膦酸盐),雷奈酸锶和雷洛昔芬的枢纽性椎体骨折研究,并评估随时间推移的椎体抗骨折疗效。结果:来自BONE试验的数据表明,依班膦酸盐具有持续的椎体抗骨折功效(第一年58%的椎体骨折风险降低p = 0.0561,0-3年增加至62%; p <0.001)。北美Risedronate治疗的椎骨功效(VERT-NA)和多国立VERT-MN(VERT-MN)研究表明,利塞膦酸盐与安慰剂的相对风险降低(RRR)随时间降低(VERT-NA:65%第一年为0-3年的41%; VERT-MN:第一年为61%,0-3年为49%)。来自阿仑膦酸盐的骨折干预试验(FIT)I试验的数据表明,与安慰剂相比,新椎骨骨折累积发生率的RRR从0-2年的62%降低到0-3年的47%。雷奈酸锶在脊柱骨质疏松症治疗干预研究(SOTI;第一年为49%,0-4年为33%)和外周骨质疏松症治疗研究(TROPOS;至第一年至第四年为45%)中,RRR随时间推移也有类似的下降。 0-5年为24%)。对于雷洛昔芬,随着时间的推移,持续的疗效尚无明显趋势。结论:阿仑膦酸盐,利塞膦酸盐和雷奈酸锶可以使椎骨骨折的保护作用随着时间的推移而降低,这可能是由于多种因素引起的。随着时间的推移,伊班膦酸持续的椎体抗骨折功效。

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