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使用活体纵向高分辨率外周定量计算机断层扫描评估人类骨机械调节的精确性。

Precision of bone mechanoregulation assessment in humans using longitudinal high-resolution peripheral quantitative computed tomography in vivo.

机构信息

Institute for Biomechanics, ETH Zurich, Zurich, Switzerland.

Institute for Biomechanics, ETH Zurich, Zurich, Switzerland; Department of Osteoporosis, Bern University Hospital, University of Bern, Bern, Switzerland.

出版信息

Bone. 2023 Jul;172:116780. doi: 10.1016/j.bone.2023.116780. Epub 2023 May 1.

Abstract

Local mechanical stimuli in the bone microenvironment are essential for the homeostasis and adaptation of the skeleton, with evidence suggesting that disruption of the mechanically-driven bone remodelling process may lead to bone loss. Longitudinal clinical studies have shown the combined use of high-resolution peripheral quantitative computed tomography (HR-pQCT) and micro-finite element analysis can be used to measure load-driven bone remodelling in vivo; however, quantitative markers of bone mechanoregulation and the precision of these analyses methods have not been validated in human subjects. Therefore, this study utilised participants from two cohorts. A same-day cohort (n = 33) was used to develop a filtering strategy to minimise false detections of bone remodelling sites caused by noise and motion artefacts present in HR-pQCT scans. A longitudinal cohort (n = 19) was used to develop bone imaging markers of trabecular bone mechanoregulation and characterise the precision for detecting longitudinal changes in subjects. Specifically, we described local load-driven formation and resorption sites independently using patient-specific odds ratios (OR) and 99 % confidence intervals. Conditional probability curves were computed to link the mechanical environment to the remodelling events detected on the bone surface. To quantify overall mechanoregulation, we calculated a correct classification rate measuring the fraction of remodelling events correctly identified by the mechanical signal. Precision was calculated as root-mean-squared averages of the coefficient of variation (RMS-SD) of repeated measurements using scan-rescan pairs at baseline combined with a one-year follow-up scan. We found no significant mean difference (p < 0.01) between scan-rescan conditional probabilities. RMS-SD was 10.5 % for resorption odds, 6.3 % for formation odds, and 1.3 % for correct classification rates. Bone was most likely to be formed in high-strain and resorbed in low-strain regions for all participants, indicating a consistent, regulated response to mechanical stimuli. For each percent increase in strain, the likelihood of bone resorption decreased by 2.0 ± 0.2 %, and the likelihood of bone formation increased by 1.9 ± 0.2 %, totalling 38.3 ± 1.1 % of strain-driven remodelling events across the entire trabecular compartment. This work provides novel robust bone mechanoregulation markers and their precision for designing future clinical studies.

摘要

局部机械刺激是骨骼维持内稳态和适应环境的必要条件,有证据表明,破坏机械驱动的骨重塑过程可能导致骨丢失。纵向临床研究表明,高分辨率外周定量计算机断层扫描(HR-pQCT)和微有限元分析的联合使用可用于测量体内负荷驱动的骨重塑;然而,骨机械调节的定量标志物及其分析方法的精度尚未在人体受试者中得到验证。因此,本研究利用来自两个队列的参与者。同一天队列(n=33)用于开发一种过滤策略,以最大程度地减少 HR-pQCT 扫描中存在的噪声和运动伪影对骨重塑部位的假检测。一个纵向队列(n=19)用于开发小梁骨机械调节的骨成像标志物,并描述检测到受试者纵向变化的精度。具体来说,我们使用患者特异性比值比(OR)和 99%置信区间独立描述局部负荷驱动的形成和吸收部位。条件概率曲线用于将机械环境与骨表面检测到的重塑事件联系起来。为了量化整体机械调节,我们计算了一个正确分类率,该比率衡量机械信号正确识别重塑事件的比例。精度是通过基线扫描-扫描对与一年后随访扫描相结合的重复测量的均方根标准偏差(RMS-SD)来计算的。我们发现扫描-扫描条件概率之间没有显著的平均差异(p<0.01)。吸收比值的 RMS-SD 为 10.5%,形成比值的 RMS-SD 为 6.3%,正确分类率的 RMS-SD 为 1.3%。对于所有参与者,骨最有可能在高应变区形成,在低应变区吸收,这表明对机械刺激有一致的、受调节的反应。对于应变的每增加 1%,骨吸收的可能性降低 2.0±0.2%,骨形成的可能性增加 1.9±0.2%,总计整个小梁腔中应变驱动的重塑事件为 38.3±1.1%。这项工作为设计未来的临床研究提供了新的稳健的骨机械调节标志物及其精度。

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