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锂使用者骨折的相对风险降低。

Reduced relative risk of fractures among users of lithium.

作者信息

Vestergaard P, Rejnmark L, Mosekilde L

机构信息

Department of Endocrinology and Metabolism C, Aarhus University Hospital, Aarhus Sygehus, Aarhus, Denmark.

出版信息

Calcif Tissue Int. 2005 Jul;77(1):1-8. doi: 10.1007/s00223-004-0258-y. Epub 2005 Jul 14.

DOI:10.1007/s00223-004-0258-y
PMID:16007481
Abstract

Lithium has been shown to inhibit bone resorption and to interact with W nt signaling, potentially pointing to bone anabolic properties. We, therefore, studied the effects of lithium on fracture risk using a case-control study design. Cases were all subjects including children with any fracture sustained during the year 2000 (n=124,655). For each case, three controls (n=373,962) matched according to age and gender was randomly drawn from the background population. Adjustments were made for use of other psychotropic drugs (neuroleptics, antidepressants, and anxiolytics/sedatives), psychiatric disease (manic depressive states, schizophrenia, and other psychoses), and other confounders. The effect of dose was examined by stratifying for cumulated dose (DDD, defined daily dose). In the crude analysis, there was a decreasing relative risk of any fracture with increasing accumulated dose of lithium. After adjustment for psychotropic drug use, the risk of any fracture was decreased (odds ratio [OR] 0.74, 95% confidence interval [CI] 0.60--0.92 for 250--849 DDD, and OR 0.67, 95% CI 0.55--0.81 for >or= 850 DDD of lithium). For Colles' fractures and spine fractures, a significant decrease was seen with >or= 850 DDD (OR 0.57, 95% CI 0.35--0.94 for Colles' fracture and OR 0.32, 95% CI 0.11--0.95 for spine fractures). For hip fractures, a nonsignificant trend toward a decrease was seen; however, without a dose-response relationship. Adjustment for further confounders did not change the results. Lithium treatment was associated with a decreased risk of fractures potentially pointing at bone anabolic properties.

摘要

锂已被证明可抑制骨吸收并与Wnt信号通路相互作用,这可能表明其具有骨合成代谢特性。因此,我们采用病例对照研究设计,研究了锂对骨折风险的影响。病例为2000年期间发生任何骨折的所有受试者(包括儿童)(n = 124,655)。对于每个病例,从背景人群中随机抽取三名年龄和性别匹配的对照(n = 373,962)。对其他精神药物(抗精神病药、抗抑郁药和抗焦虑药/镇静剂)的使用、精神疾病(躁狂抑郁状态、精神分裂症和其他精神病)以及其他混杂因素进行了调整。通过对累积剂量(DDD,限定日剂量)进行分层来检查剂量的影响。在粗分析中,随着锂累积剂量的增加,任何骨折的相对风险都在降低。在对精神药物使用进行调整后,任何骨折的风险降低(锂剂量为250 - 849 DDD时,比值比[OR]为0.74,95%置信区间[CI]为0.60 - 0.92;锂剂量≥850 DDD时,OR为0.67,95% CI为0.55 - 0.81)。对于Colles骨折和脊柱骨折,锂剂量≥850 DDD时可显著降低风险(Colles骨折的OR为0.57,95% CI为0.35 - 0.94;脊柱骨折的OR为0.32,95% CI为0.11 - 0.95)。对于髋部骨折,观察到有降低的非显著趋势;然而,不存在剂量反应关系。对进一步的混杂因素进行调整并未改变结果。锂治疗与骨折风险降低相关,这可能表明其具有骨合成代谢特性。

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