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髋部骨折后一年内的骨代谢血清和尿液标志物。

Serum and urine markers of bone metabolism during the year after hip fracture.

作者信息

Yu-Yahiro J A, Michael R H, Dubin N H, Fox K M, Sachs M, Hawkes W G, Hebel J R, Zimmerman S I, Shapiro J, Magaziner J

机构信息

Department of Orthopaedic Surgery, The Union Memorial Hospital, Baltimore, Maryland, USA.

出版信息

J Am Geriatr Soc. 2001 Jul;49(7):877-83. doi: 10.1046/j.1532-5415.2001.49177.x.

Abstract

OBJECTIVE

As part of a larger study to describe indices of recovery during the year after hip fracture, the current prospective study investigated longitudinal changes in serum and urine markers of bone metabolism for the year after hip fracture and related them to bone mineral density (BMD).

DESIGN

A representative subset of participants provided serum and urine samples and had bone density measured at 3, 10, 60, 180, and 365 days postfracture.

SETTING

Two Baltimore hospitals.

PARTICIPANTS

The subjects were 205 community-dwelling, white women age 65 and older with fresh proximal femur fractures.

MEASUREMENTS

Samples were assayed for specific bone-related proteins and bone turnover markers, including serum osteocalcin (OC), procollagen type 1 carboxy-terminal extension peptide (PICP), bone-specific alkaline phosphatase (BAP), and urinary deoxypyridinoline (DPD) cross-links. Selected hormonal regulators of bone metabolism, including parathyroid hormone (PTH), calcitonin (CT), 1,25-dihydroxy vitamin D(3) (1,25 (OH)(2)D), and estrone (E(1)) were measured from serum samples. Repeated measures analyses were used to evaluate postfracture changes in each of the markers.

RESULTS

BAP, OC, and PICP were most active during the early postfracture period (3-60 days). BAP and OC remained elevated at 365 days compared with 3 days. DPD rose 48% from 3 days to 60 days, but this difference was not statistically significant. PTH and 1,25 (OH)(2)D increased steadily and significantly from 3 to 365 days. E(1) was highest at baseline and decreased at each time point, whereas CT showed no significant changes. When subjects were stratified into high-, medium-, and low-BMD groups based on their measurement at 3 days, both osteoclastic and osteoblastic markers in the low-BMD group displayed exaggerated and different patterns over time compared with the other groups.

CONCLUSION

Currently, the standard treatment of care for hip fractures still results in high morbidity and mortality and failure to regain prefracture quality of life. Gaining an understanding of bone cell activity in these patients after hip fracture, derived by measuring markers longitudinally during recovery, provides a baseline by which to measure the effectiveness of new interventions to improve recovery from hip fracture.

摘要

目的

作为一项关于描述髋部骨折后一年内恢复指标的大型研究的一部分,当前这项前瞻性研究调查了髋部骨折后一年内血清和尿液骨代谢标志物的纵向变化,并将其与骨密度(BMD)相关联。

设计

有代表性的一部分参与者在骨折后3天、10天、60天、180天和365天提供血清和尿液样本,并测量骨密度。

地点

巴尔的摩的两家医院。

参与者

研究对象为205名社区居住的65岁及以上的白人女性,她们均有新鲜的股骨近端骨折。

测量指标

对样本进行特定骨相关蛋白和骨转换标志物的检测,包括血清骨钙素(OC)、I型前胶原羧基末端延长肽(PICP)、骨特异性碱性磷酸酶(BAP)以及尿脱氧吡啶啉(DPD)交联物。从血清样本中测量选定的骨代谢激素调节因子,包括甲状旁腺激素(PTH)、降钙素(CT)、1,25 - 二羟维生素D3(1,25(OH)2D)和雌酮(E1)。采用重复测量分析来评估骨折后各标志物的变化。

结果

BAP、OC和PICP在骨折后早期(3 - 60天)最为活跃。与骨折后3天相比,BAP和OC在365天时仍处于升高状态。DPD从3天到60天上升了48%,但这一差异无统计学意义。PTH和1,25(OH)2D从3天到365天稳步且显著升高。E1在基线时最高,在每个时间点均下降,而CT无显著变化。当根据骨折后3天的测量结果将受试者分为高、中、低骨密度组时,与其他组相比,低骨密度组的破骨细胞和成骨细胞标志物随时间呈现出夸张且不同的模式。

结论

目前,髋部骨折的标准治疗护理仍导致高发病率、高死亡率以及无法恢复骨折前的生活质量。通过在恢复过程中纵向测量标志物来了解这些髋部骨折患者的骨细胞活性,可为衡量改善髋部骨折恢复的新干预措施的有效性提供一个基线。

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