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慢性肾脏病患儿骨病的干预措施。

Interventions for bone disease in children with chronic kidney disease.

作者信息

Geary Denis F, Hodson Elisabeth M, Craig Jonathan C

机构信息

Department of Paediatrics, Hospital for Sick Children, 555 University Ave, Toronto, ON, Canada, M5G 1X8.

出版信息

Cochrane Database Syst Rev. 2010 Jan 20(1):CD008327. doi: 10.1002/14651858.CD008327.

Abstract

BACKGROUND

Bone disease is common in children with chronic kidney disease (CKD) and when untreated may result in bone deformities, bone pain, fractures and reduced growth rates.

OBJECTIVES

To investigate the benefits and harms of interventions for preventing and treating bone disease in children with CKD.

SEARCH STRATEGY

The Cochrane Renal Group's specialised register, the Cochrane Central Register of Controlled Trials, MEDLINE, EMBASE, reference lists and abstracts were searched without language restriction.

SELECTION CRITERIA

Randomised controlled trials (RCTs) comparing different interventions used to prevent or treat bone disease in children with CKD stages 2-5D compared with placebo, no treatment or other agents were included. Studies examining different routes or frequency of treatment were also included.

DATA COLLECTION AND ANALYSIS

Data were extracted by two authors. The random-effects model was used and results were reported as risk ratios or risk differences for dichotomous outcomes and mean differences for continuous outcomes with 95% confidence intervals.

MAIN RESULTS

Fifteen RCTs (369 children) were identified. Compared with oral calcitriol, intraperitoneal calcitriol significantly reduced the level of serum parathyroid hormone (PTH) but there were no significant differences in bone histology or other biochemical measures (2 RCTs). There were no significant differences detected in growth, PTH, serum calcium or phosphorus between daily versus intermittent calcitriol (3 RCTs). Vitamin D therapy significantly reduced PTH levels compared with placebo or no treatment. The number of children with hypercalcaemia did not differ significantly between groups (4 RCTs). No significant differences were detected in growth rates, bone histology or biochemical parameters between calcitriol and either dihydrotachysterol or ergocalciferol (2 RCTs). Though fewer episodes of hypercalcaemia were reported with sevelamer, no significant differences were detected in serum calcium, phosphorus and PTH levels between calcium-containing phosphate binders and either aluminium hydroxide or sevelamer (4 RCTs).

AUTHORS' CONCLUSIONS: Bone disease, assessed by changes in PTH levels, is improved by all vitamin D preparations. However no consistent differences between routes of administration, frequencies of dosing or vitamin D preparations have been demonstrated. Though fewer episodes of high calcium levels occurred with the non calcium-containing binder, sevelamer, compared with calcium-containing binders, there were no differences in serum phosphorus and calcium overall and phosphorus values were reduced to similar extents. All RCTs were small with few data available on patient-centred outcomes (growth, bone deformities) and limited data on biochemical parameters resulting in considerable imprecision of results thus limiting the applicability to care of children with CKD.

摘要

背景

骨病在慢性肾脏病(CKD)患儿中很常见,若不治疗可能导致骨骼畸形、骨痛、骨折及生长速率降低。

目的

探讨预防和治疗CKD患儿骨病的干预措施的益处和危害。

检索策略

检索了Cochrane肾脏组专业注册库、Cochrane对照试验中央注册库、MEDLINE、EMBASE、参考文献列表及摘要,无语言限制。

选择标准

纳入比较用于预防或治疗2 - 5D期CKD患儿骨病的不同干预措施与安慰剂、不治疗或其他药物的随机对照试验(RCT)。也纳入了研究不同治疗途径或频率的研究。

数据收集与分析

由两位作者提取数据。采用随机效应模型,结果以二分类结局的风险比或风险差异以及连续结局的均值差异表示,并给出95%置信区间。

主要结果

共识别出15项RCT(369名儿童)。与口服骨化三醇相比,腹腔内注射骨化三醇显著降低了血清甲状旁腺激素(PTH)水平,但在骨组织学或其他生化指标方面无显著差异(2项RCT)。每日服用与间歇服用骨化三醇在生长、PTH、血清钙或磷方面未检测到显著差异(3项RCT)。与安慰剂或不治疗相比,维生素D治疗显著降低了PTH水平。高钙血症患儿的数量在各组间无显著差异(4项RCT)。在骨化三醇与二氢速甾醇或麦角钙化醇之间,生长速率、骨组织学或生化参数未检测到显著差异(2项RCT)。尽管司维拉姆报告的高钙血症发作较少,但含钙磷结合剂与氢氧化铝或司维拉姆之间在血清钙、磷和PTH水平上未检测到显著差异(4项RCT)。

作者结论

通过PTH水平变化评估的骨病,所有维生素D制剂均可改善。然而,在给药途径、给药频率或维生素D制剂之间未显示出一致的差异。尽管与含钙磷结合剂相比,不含钙的结合剂司维拉姆发生高钙血症的发作较少,但总体血清磷和钙无差异,且磷值降低程度相似。所有RCT规模较小,关于以患者为中心的结局(生长、骨骼畸形)的数据很少,生化参数数据有限,导致结果相当不精确,从而限制了其对CKD患儿护理的适用性。

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