Among people on osteoporosis medication, loss of appendicular or total body lean mass is an independent risk factor for hip and major osteoporotic fractures.

IF 4.2 2区医学 Q1 ENDOCRINOLOGY & METABOLISM

Osteoporosis International Pub Date : 2024-11-01 Epub Date: 2024-09-25 DOI:10.1007/s00198-024-07240-z

Lora M Giangregorio, Mackenzie Ryann Alexiuk, Navdeep Tangri, Clara Bohm, William D Leslie

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引用次数: 0

Abstract

People with prior lean mass loss had a ~ 10% higher risk of MOF and ~ 22-26% higher risk of hip fracture, and the results were similar in people on anti-osteoporosis medications. Loss of lean mass is associated with increased fracture risk. Patients should be encouraged to pursue strategies to prevent loss of lean mass.

Background: Sarcopenia increases fracture risk. If the risk persists after starting osteoporosis medication, patients may need to be encouraged to pursue strategies to prevent loss of lean mass.

Objective: To estimate the effects of loss in appendicular lean mass (ALM) or total body lean mass (TBLM) on subsequent fracture risk and effect modification with anti-osteoporosis medication use.

Methods: We conducted a registry-based cohort study linked to population-based data. We identified individuals ≥ 40 years of age with two DXA assessments ≥ 1 year apart and minimum 0.5 years of observation. ALM and TBLM were estimated from weight, sex, and percent fat from DXA (R² = 0.91 and 0.84 vs total body DXA, respectively). We report hazard ratios (HR) from Cox regression models estimating time to first incident major osteoporotic fracture (MOF) and hip fracture, adjusted for fracture risk; osteoporosis medication was included as an interaction term and used to stratify analyses.

Results: We included 21,249 individuals (mean 67 [SD 10] years, 95% female, 37% on osteoporosis medication). The mean follow-up was 7 years (SD 4). A total of 1868 and 548 people had incident MOF and hip fracture, respectively. People with prior ALM loss (HR per SD 1.09, 95% CI 1.04-1.15) or TBLM loss (HR per SD 1.09, 95% CI 1.42-1.14) had a higher risk of MOF. Hip fracture risk was greater in people with prior ALM loss (HR per SD 1.22, 95% CI 1.12-1.33) and TBLM loss (HR per SD 1.26, 95% CI 1.16-1.38). There were no interactions with anti-osteoporosis medication use (all p > 0.3). When restricted to people on anti-osteoporosis medication, each SD in ALM or TBLM loss was associated with 8-9% increased MOF risk and 18-23% increased hip fracture risk.

Conclusions: Loss of lean mass is associated with increased fracture risk among individuals on anti-osteoporosis medication. Patients should be encouraged to pursue strategies to prevent sarcopenia.

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在服用骨质疏松症药物的人群中，阑尾或全身瘦体重的减少是髋部骨折和主要骨质疏松性骨折的独立风险因素。

之前瘦体重下降的人发生 MOF 的风险高出约 10%，发生髋部骨折的风险高出约 22-26%，服用抗骨质疏松症药物的人的结果与此类似。瘦体重的减少与骨折风险的增加有关。应鼓励患者采取预防瘦体重流失的策略：背景：肌肉疏松症会增加骨折风险。背景：骨质疏松症会增加骨折风险，如果开始服用骨质疏松症药物后风险依然存在，则可能需要鼓励患者采取预防瘦体重流失的策略：目的：估计关节瘦体重（ALM）或全身瘦体重（TBLM）的损失对后续骨折风险的影响，以及使用抗骨质疏松症药物的效果修正：方法：我们进行了一项基于登记的队列研究，该研究与基于人口的数据相关联。我们确定了年龄≥ 40 岁、两次 DXA 评估间隔≥ 1 年且至少观察 0.5 年的个体。ALM和TBLM是根据体重、性别和DXA的脂肪百分比估算得出的（与全身DXA相比，R2分别为0.91和0.84）。我们报告了根据骨折风险调整后的 Cox 回归模型估算的首次发生重大骨质疏松性骨折（MOF）和髋部骨折的时间的危险比（HR）；骨质疏松症药物治疗作为交互项，用于对分析进行分层：我们纳入了 21,249 人（平均 67 [SD 10] 岁，95% 为女性，37% 正在服用骨质疏松症药物）。平均随访时间为 7 年（SD 4）。分别有 1868 人和 548 人发生 MOF 和髋部骨折。曾患 ALM 缺失（HR 每 SD 1.09，95% CI 1.04-1.15）或 TBLM 缺失（HR 每 SD 1.09，95% CI 1.42-1.14）的人发生 MOF 的风险更高。髋部骨折风险较高的人群包括曾丧失ALM者（HR per SD 1.22，95% CI 1.12-1.33）和曾丧失TBLM者（HR per SD 1.26，95% CI 1.16-1.38）。与抗骨质疏松症药物的使用没有交互作用（均 p > 0.3）。如果仅限于服用抗骨质疏松症药物的人群，ALM或TBLM每减少一个SD与MOF风险增加8%-9%和髋部骨折风险增加18%-23%有关：结论：在服用抗骨质疏松症药物的人群中，瘦体重的减少与骨折风险的增加有关。应鼓励患者采取预防肌肉疏松症的策略。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Osteoporosis International 医学-内分泌学与代谢

CiteScore

8.10

自引率

10.00%

发文量

224

审稿时长

3 months

期刊介绍： An international multi-disciplinary journal which is a joint initiative between the International Osteoporosis Foundation and the National Osteoporosis Foundation of the USA, Osteoporosis International provides a forum for the communication and exchange of current ideas concerning the diagnosis, prevention, treatment and management of osteoporosis and other metabolic bone diseases. It publishes: original papers - reporting progress and results in all areas of osteoporosis and its related fields; review articles - reflecting the present state of knowledge in special areas of summarizing limited themes in which discussion has led to clearly defined conclusions; educational articles - giving information on the progress of a topic of particular interest; case reports - of uncommon or interesting presentations of the condition. While focusing on clinical research, the Journal will also accept submissions on more basic aspects of research, where they are considered by the editors to be relevant to the human disease spectrum.