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骨质疏松症中长期使用双磷酸盐。

Long-term use of bisphosphonates in osteoporosis.

机构信息

University of Cincinnati Bone Health and Osteoporosis Center, Cincinnati, Ohio 45219, USA.

出版信息

J Clin Endocrinol Metab. 2010 Apr;95(4):1555-65. doi: 10.1210/jc.2009-1947. Epub 2010 Feb 19.

Abstract

CONTEXT

Bisphosphonates have been widely used in the treatment of osteoporosis. Uncommon side effects have emerged in postapproval use. Because bisphosphonates accumulate in bone and are released for months or years after treatment is stopped, it is reasonable to consider the clinical question of how long to treat.

OBJECTIVE

In this personal perspective, we review the pharmacology and mechanism of action of bisphosphonates and the clinical studies that support their efficacy. We then review the literature for longer-term studies and reports of possible side effects that were not seen in clinical trials.

RESULTS

Bisphosphonates have demonstrated antifracture efficacy in randomized, placebo-controlled trials of 3 and 4 yr duration and have been widely used since the initial release of alendronate in 1995. For zoledronic acid and risedronate, an early effect (fractures reduced within 6-12 months of starting therapy) has been shown. A sustained effect for risedronate has been shown through 5 yr and suggested through 7 yr. Ten-year data with alendronate and 8 yr data with risedronate indicated good tolerability and safety; it is unlikely that longer-term studies will be done. Side effects that emerged in clinical trials include esophageal irritation with oral administration and acute phase response with iv treatment or high-dose oral therapy. Uncommon side effects that have been noted with wide clinical use include osteonecrosis of the jaw, musculoskeletal complaints, and atypical fractures. The numbers of events are small, and a clear cause-and-effect relationship between these events and bisphosphonate treatment has not been established. Because bisphosphonates accumulate in bone, they create a reservoir leading to continued release from bone for months or years after treatment is stopped. Studies with risedronate and alendronate suggest that if treatment is stopped after 3-5 yr, there is persisting antifracture efficacy, at least for 1-2 yr.

CONCLUSIONS

Bisphosphonates are popular and effective for treatment of osteoporosis. Because they accumulate in bone and provide some residual antifracture reduction when treatment is stopped, we recommend a drug holiday after 5-10 yr of bisphosphonate treatment. The duration of treatment and length of the holiday are based on fracture risk and pharmacokinetics of the bisphosphonate used. Patients at mild risk might stop treatment after 5 yr and remain off as long as bone mineral density is stable and no fractures occur. Higher risk patients should be treated for 10 yr, have a holiday of no more than a year or two, and perhaps be on a nonbisphosphonate treatment during that time.

摘要

背景

双膦酸盐已广泛用于骨质疏松症的治疗。在批准后的使用中出现了罕见的副作用。由于双膦酸盐在骨骼中蓄积,并在停药后数月或数年内释放,因此有理由考虑治疗时间的长短。

目的

在这篇个人观点中,我们回顾了双膦酸盐的药理学和作用机制以及支持其疗效的临床研究。然后,我们回顾了长期研究的文献和可能的副作用报告,这些副作用在临床试验中没有观察到。

结果

双膦酸盐在为期 3 年和 4 年的随机、安慰剂对照试验中显示出抗骨折疗效,并自 1995 年阿伦膦酸盐首次上市以来得到广泛应用。唑来膦酸和利塞膦酸的早期疗效(治疗开始后 6-12 个月内骨折减少)已经得到证实。利塞膦酸盐的持续疗效已通过 5 年研究和 7 年研究提示。阿伦膦酸盐 10 年数据和利塞膦酸盐 8 年数据表明其具有良好的耐受性和安全性;不太可能进行更长期的研究。临床试验中出现的副作用包括口服时食管刺激和静脉治疗或高剂量口服治疗时的急性期反应。在广泛的临床应用中注意到的罕见副作用包括下颌骨坏死、肌肉骨骼投诉和非典型骨折。事件数量较少,并且这些事件与双膦酸盐治疗之间没有建立明确的因果关系。由于双膦酸盐在骨骼中蓄积,因此在停药后数月或数年内会持续从骨骼中释放,从而形成一个储库。利塞膦酸盐和阿伦膦酸盐的研究表明,如果在 3-5 年后停止治疗,至少在 1-2 年内仍会有持续的抗骨折疗效。

结论

双膦酸盐是治疗骨质疏松症的常用且有效的药物。由于它们在骨骼中蓄积,并且在停药后仍能提供一定程度的抗骨折减少,因此我们建议在双膦酸盐治疗 5-10 年后进行药物假期。治疗时间和假期长度取决于骨折风险和所用双膦酸盐的药代动力学。风险较低的患者可以在 5 年后停止治疗,只要骨密度稳定且没有发生骨折,就可以长期停药。高风险患者应接受 10 年治疗,停药不超过一两年,在此期间可能需要使用非双膦酸盐治疗。

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