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骨质疏松症与骨强度的新观念

Emerging concepts in osteoporosis and bone strength.

作者信息

Rubin Craig D

机构信息

Geriatric Section, University of Texas Southwestern Medical Center at Dallas, TX 75390-8889, USA.

出版信息

Curr Med Res Opin. 2005 Jul;21(7):1049-56. doi: 10.1185/030079905X50525.

Abstract

OBJECTIVE

Osteoporosis is a systemic skeletal disorder characterized by compromised bone strength and increased fracture risk. The factors that contribute to bone strength include bone mineral density (BMD) and bone quality, which encompasses factors such as bone turnover, microarchitecture, mineralization, and geometry. The objective of this paper was to review the factors that contribute to bone strength and osteoporosis.

RESEARCH DESIGN

A MEDLINE search of English language journals between 1 January 1995 and 1 March 2005 was conducted using the term 'osteoporosis' combined with 'bone strength' or 'bone quality'. Reference lists of pivotal studies and reviews were also examined. Studies were otherwise not excluded on the basis of quality or size, the aim being to present an overview of research conducted to date on osteoporosis and bone strength.

RESULTS

While there is a relationship between BMD and fracture risk, evidence suggests that BMD measurements reflect only 1 component of bone strength. For example, small changes in BMD produced by osteoporosis treatments do not fully explain the reductions in fracture risk observed after initiation of therapy, and substantial fracture risk reduction is observed before peak increases in BMD are achieved. In addition to their effects on BMD, anti-resorptive therapies for osteoporosis (i.e., bisphosphonates, selective estrogen receptor modulators, calcitonin, and estrogen) produce positive effects on bone turnover, microarchitecture, and/or mineralization, all of which can contribute to the reductions in fracture risk observed with these agents. Anabolic agents such as teriparatide also appear to have beneficial effects on bone strength independent of bone mass. New, non-invasive, high-resolution imaging methods, such as magnetic resonance imaging and computed tomography, may offer a comprehensive assessment of bone quality in the future.

CONCLUSIONS

The development of clinical tools that assess bone quality independent of BMD will be essential to advance our assessment of fracture risk and response to osteoporosis treatment.

摘要

目的

骨质疏松症是一种全身性骨骼疾病,其特征为骨强度受损和骨折风险增加。影响骨强度的因素包括骨矿物质密度(BMD)和骨质量,骨质量涵盖骨转换、微结构、矿化和几何形状等因素。本文的目的是综述影响骨强度和骨质疏松症的因素。

研究设计

使用“骨质疏松症”与“骨强度”或“骨质量”相结合的术语,对1995年1月1日至2005年3月1日期间的英文期刊进行了MEDLINE检索。还查阅了关键研究和综述的参考文献列表。其他研究不根据质量或规模排除,目的是概述迄今为止关于骨质疏松症和骨强度的研究。

结果

虽然BMD与骨折风险之间存在关联,但有证据表明BMD测量仅反映骨强度的一个组成部分。例如,骨质疏松症治疗引起的BMD小变化并不能完全解释治疗开始后观察到的骨折风险降低,并且在BMD达到峰值增加之前就观察到了显著的骨折风险降低。除了对BMD的影响外,骨质疏松症的抗吸收疗法(即双膦酸盐、选择性雌激素受体调节剂、降钙素和雌激素)对骨转换、微结构和/或矿化产生积极影响,所有这些都有助于降低使用这些药物观察到的骨折风险。诸如特立帕肽等促合成代谢药物似乎对骨强度也有独立于骨量的有益影响。新的非侵入性高分辨率成像方法,如磁共振成像和计算机断层扫描,可能在未来提供对骨质量的全面评估。

结论

开发独立于BMD评估骨质量的临床工具对于推进我们对骨折风险的评估以及对骨质疏松症治疗的反应至关重要。

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