Palmer S C, McGregor D O, Strippoli G F
University of Otago, Department of Medicine, Christchurch School of Medicine and Health Sciences, PO Box 4345, Christchurch, New Zealand.
Cochrane Database Syst Rev. 2007 Jul 18(3):CD005015. doi: 10.1002/14651858.CD005015.pub3.
Patients with chronic kidney disease have significant abnormalities of bone remodeling and mineral homeostasis and are at increased risk of fracture. The fracture risk for a kidney transplant recipient is four times that of the general population and higher than for a patient on dialysis. Randomised controlled trials (RCTs) report the use of bisphosphonates, vitamin D sterols, calcitonin, and hormone replacement therapy to treat bone disease following transplantation.
To evaluate the use of interventions for treating bone disease following kidney transplantation.
We searched the Cochrane Central Register of Controlled Trials (CENTRAL in The Cochrane Library), Cochrane Renal Group's specialised register, MEDLINE, EMBASE, reference lists, and conference proceedings abstracts without language restriction. Date of last search: May 2006
RCTs and quasi-RCTs comparing different treatments for kidney transplant recipients of any age were selected. We excluded all other transplant recipients, including kidney-pancreas transplant recipients.
Two authors independently assessed trial quality and extracted data. Statistical analyses were performed using the random effects model and the results expressed as relative risk (RR) with 95% confidence intervals (CI) for dichotomous variables and mean difference (MD) for continuous outcomes.
Twenty-four trials (1,299 patients) were included. No individual intervention (bisphosphonates, vitamin D sterol or calcitonin) was associated with a reduction in fracture risk compared with placebo. Combining results for all active interventions against placebo demonstrated any treatment of bone disease was associated with a reduction in the RR of fracture (RR 0.51, 95% CI 0.27 to 0.99). Bisphosphonates (any route), vitamin D sterol, and calcitonin all had a beneficial effect on the bone mineral density at the lumbar spine. Bisphosphonates and vitamin D sterol also had a beneficial effect on the bone mineral density at the femoral neck. Bisphosphonates had greater efficacy for preventing bone mineral density loss when compared head-to-head with vitamin D sterols. Few or no data were available for combined hormone replacement, testosterone, selective oestrogen receptor modulators, fluoride or anabolic steroids. Other outcomes including all-cause mortality and drug-related toxicity were reported infrequently.
AUTHORS' CONCLUSIONS: Treatment with a bisphosphonate, vitamin D sterol or calcitonin after kidney transplantation may protect against immunosuppression-induced reductions in bone mineral density and prevent fracture. Adequately powered trials are required to determine whether bisphosphonates are better than vitamin D sterols for fracture prevention in this population. The optimal route, timing, and duration of administration of these interventions remains unknown.
慢性肾病患者存在骨重塑和矿物质稳态的显著异常,骨折风险增加。肾移植受者的骨折风险是普通人群的四倍,且高于透析患者。随机对照试验(RCT)报告了使用双膦酸盐、维生素D甾醇、降钙素和激素替代疗法来治疗移植后的骨病。
评估肾移植后治疗骨病的干预措施的使用情况。
我们检索了Cochrane对照试验中心注册库(Cochrane图书馆中的CENTRAL)、Cochrane肾脏组的专业注册库、MEDLINE、EMBASE、参考文献列表和会议论文摘要,无语言限制。最后检索日期:2006年5月
选择比较任何年龄的肾移植受者不同治疗方法的RCT和半RCT。我们排除了所有其他移植受者,包括肾胰腺移植受者。
两位作者独立评估试验质量并提取数据。使用随机效应模型进行统计分析,结果以相对风险(RR)表示,二分变量的95%置信区间(CI),连续结果的平均差(MD)。
纳入了24项试验(1299例患者)。与安慰剂相比,没有单一干预措施(双膦酸盐、维生素D甾醇或降钙素)与骨折风险降低相关。将所有活性干预措施与安慰剂的结果合并显示,任何骨病治疗都与骨折RR降低相关(RR 0.51,95%CI 0.27至0.99)。双膦酸盐(任何途径)、维生素D甾醇和降钙素对腰椎骨矿物质密度均有有益作用。双膦酸盐和维生素D甾醇对股骨颈骨矿物质密度也有有益作用。与维生素D甾醇直接比较时,双膦酸盐在预防骨矿物质密度丢失方面疗效更佳。关于联合激素替代、睾酮、选择性雌激素受体调节剂、氟化物或合成代谢类固醇的数据很少或没有。其他结果,包括全因死亡率和药物相关毒性,报告较少。
肾移植后用双膦酸盐、维生素D甾醇或降钙素治疗可能预防免疫抑制引起的骨矿物质密度降低并预防骨折。需要有足够效力的试验来确定在该人群中双膦酸盐在预防骨折方面是否优于维生素D甾醇。这些干预措施的最佳给药途径、时机和持续时间仍不清楚。
