Bischoff-Ferrari Heike A, Willett Walter C, Wong John B, Stuck Andreas E, Staehelin Hannes B, Orav E John, Thoma Anna, Kiel Douglas P, Henschkowski Jana
Centre on Aging and Mobility, University of Zurich, University Hospital, Switzerland.
Arch Intern Med. 2009 Mar 23;169(6):551-61. doi: 10.1001/archinternmed.2008.600.
Antifracture efficacy with supplemental vitamin D has been questioned by recent trials.
We performed a meta-analysis on the efficacy of oral supplemental vitamin D in preventing nonvertebral and hip fractures among older individuals (> or =65 years). We included 12 double-blind randomized controlled trials (RCTs) for nonvertebral fractures (n = 42 279) and 8 RCTs for hip fractures (n = 40 886) comparing oral vitamin D, with or without calcium, with calcium or placebo. To incorporate adherence to treatment, we multiplied the dose by the percentage of adherence to estimate the mean received dose (dose x adherence) for each trial.
The pooled relative risk (RR) was 0.86 (95% confidence interval [CI], 0.77-0.96) for prevention of nonvertebral fractures and 0.91 (95% CI, 0.78-1.05) for the prevention of hip fractures, but with significant heterogeneity for both end points. Including all trials, antifracture efficacy increased significantly with a higher dose and higher achieved blood 25-hydroxyvitamin D levels for both end points. Consistently, pooling trials with a higher received dose of more than 400 IU/d resolved heterogeneity. For the higher dose, the pooled RR was 0.80 (95% CI, 0.72-0.89; n = 33 265 subjects from 9 trials) for nonvertebral fractures and 0.82 (95% CI, 0.69-0.97; n = 31 872 subjects from 5 trials) for hip fractures. The higher dose reduced nonvertebral fractures in community-dwelling individuals (-29%) and institutionalized older individuals (-15%), and its effect was independent of additional calcium supplementation.
Nonvertebral fracture prevention with vitamin D is dose dependent, and a higher dose should reduce fractures by at least 20% for individuals aged 65 years or older.
近期试验对补充维生素D的抗骨折疗效提出了质疑。
我们对口服补充维生素D在预防老年个体(≥65岁)非椎体和髋部骨折方面的疗效进行了荟萃分析。我们纳入了12项针对非椎体骨折的双盲随机对照试验(RCT,n = 42279)和8项针对髋部骨折的RCT(n = 40886),比较口服维生素D(含或不含钙)与钙或安慰剂。为纳入治疗依从性,我们将剂量乘以依从百分比以估算每项试验的平均接受剂量(剂量×依从性)。
预防非椎体骨折的合并相对风险(RR)为0.86(95%置信区间[CI],0.77 - 0.96),预防髋部骨折的RR为0.91(95%CI,0.78 - 1.05),但两个终点均存在显著异质性。纳入所有试验后,两个终点的抗骨折疗效均随剂量增加和达到的血液25 - 羟维生素D水平升高而显著增加。一致地,汇总接受剂量高于400 IU/d的试验可解决异质性问题。对于较高剂量,非椎体骨折的合并RR为0.80(95%CI,0.72 - 0.89;来自9项试验的33265名受试者),髋部骨折的合并RR为0.82(95%CI,0.69 - 0.97;来自5项试验的31872名受试者)。较高剂量降低了社区居住个体的非椎体骨折(-29%)和机构养老的老年个体的非椎体骨折(-15%),其效果与额外补充钙无关。
维生素D预防非椎体骨折具有剂量依赖性,对于65岁及以上个体,较高剂量应至少降低20%的骨折发生率。
Zotero 插件