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双膦酸盐在慢性肾脏病中起作用吗?

Is there a role for bisphosphonates in chronic kidney disease?

作者信息

Miller Paul D

机构信息

Department of Medicine, University of Colorado Health Sciences Center, Denver, Colorado, USA.

出版信息

Semin Dial. 2007 May-Jun;20(3):186-90. doi: 10.1111/j.1525-139X.2007.00271.x.

Abstract

Patients with stage 5 chronic kidney disease (CKD) including those on dialysis can and do develop osteoporosis. They also develop a wide range of other metabolic bone diseases that may look like osteoporosis when it is defined by either the World Health Organization bone mineral density (BMD) criteria or by the development of fragility fractures. Those dialysis patients with osteoporosis that is due to gonadal hormone deficiency such as postmenopausal osteoporosis, glucocorticoid-induced osteoporosis, or male osteoporosis may benefit from the administration of bisphosphonates (BPs). The challenges lie in the diagnosis of osteoporosis in this population where adynamic, osteomalacic, hyperparathyroid, or aluminum bone disease are also prevalent, with concommitant low BMD and low trauma fractures, but where BPs may be contraindicated. The only secure means to diagnose osteoporosis in this patient population is by quantitative bone histomorphometry demonstrating low trabecular bone volume and disrupted microarchitecture. Once the diagnosis of osteoporosis is established, BPs should be considered for a well-defined brief period of time (e.g., 2-3 years), even though there is no evidence for a fracture reduction benefit in this population. If a BP is chosen there may be a need for dose adjustment or slower infusion rates (for the intravenous formulations), as a greater bone retention may occur for these renally cleared agents. While it is unknown what consequences could develop from increased bone retention in patients with little renal function, data are needed if more bone retention of BP might lead to a greater risk of the development of adynamic bone disease and lower bone strength. More data are needed to define the risks and benefits of BPs in patients with stage 5 CKD.

摘要

5期慢性肾脏病(CKD)患者,包括透析患者,会发生骨质疏松症。他们还会患上一系列其他代谢性骨病,当按照世界卫生组织骨密度(BMD)标准或脆性骨折的发生来定义骨质疏松症时,这些疾病可能看似骨质疏松症。那些因性腺激素缺乏导致骨质疏松症的透析患者,如绝经后骨质疏松症、糖皮质激素诱导的骨质疏松症或男性骨质疏松症,可能会从双膦酸盐(BP)的给药中获益。挑战在于该人群骨质疏松症的诊断,其中骨动力不足、骨软化、甲状旁腺功能亢进或铝骨病也很常见,伴有骨密度低和低创伤性骨折,但BP可能是禁忌的。在该患者群体中诊断骨质疏松症的唯一可靠方法是通过定量骨组织形态计量学,显示小梁骨体积低和微结构破坏。一旦确诊骨质疏松症,即使没有证据表明BP对该人群有降低骨折的益处,也应在明确的短时间内(如2 - 3年)考虑使用BP。如果选择了BP,可能需要调整剂量或减慢输注速度(对于静脉制剂),因为这些经肾脏清除的药物可能会有更多的骨潴留。虽然尚不清楚肾功能差的患者骨潴留增加会产生什么后果,但如果BP更多的骨潴留可能导致骨动力不足性骨病发生风险增加和骨强度降低,则需要相关数据。需要更多数据来确定BP在5期CKD患者中的风险和益处。

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