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Changes in bone remodelling and antifracture efficacy of intermittent bisphosphonate therapy: implications from clinical studies with ibandronate

机译:间歇性双膦酸盐治疗的骨重塑和抗骨折功效的变化:伊班膦酸的临床研究的意义

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摘要

Bisphosphonates reduce the rate of bone resorption and bone remodelling. Given daily, they decrease the risk of fractures in postmenopausal osteoporosis. When bisphosphonates were given at extended drug‐free intervals this antifracture efficacy was generally not seen. This may be due to the different pattern of bone remodelling changes. Data from randomised clinical studies of ibandronate, given orally or intravenously, at different doses and for variable time intervals to women with osteoporosis were examined to explore the relationship between intermittent bisphosphonate therapy, changes in bone resorption and fracture risk. The magnitude of the reduction of the rate of bone resorption at the end of the drug‐free interval rather than its fluctuation pattern after bisphosphonate administration determines antifracture efficacy, provided that these fluctuations occur within the premenopausal range. Prolongation of the drug‐free interval beyond 2 weeks should be compensated by a dose higher than the cumulative daily dose.
机译:双膦酸盐降低骨吸收和骨重塑的速率。每天服用,可降低绝经后骨质疏松症骨折的风险。当双膦酸盐类药物在延长的无药间隔时间使用时,通常不会看到这种抗骨折功效。这可能是由于骨骼重塑变化的不同模式所致。检查了来自伊班膦酸的随机临床研究的数据,这些数据通过口服或静脉内,以不同剂量和不同时间间隔给予骨质疏松症妇女,以探讨间歇性双膦酸盐治疗,骨吸收变化和骨折风险之间的关系。在无药间隔结束时骨吸收速率降低的幅度,而不是双膦酸盐给药后的波动模式,决定了抗骨折功效,前提是这些波动发生在绝经前范围内。无药间隔时间延长超过2周,应以高于每日累积剂量的剂量来补偿。

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