重度骨关节炎患者骨对骨磨损沟下硬化软骨下骨的高分辨率显微ct分析。

Bone Pub Date : 2025-01-04 DOI:10.1016/j.bone.2024.117388
Meret Keiser, Stefan Preiss, Stephen J Ferguson, Vincent A Stadelmann
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引用次数: 0

摘要

骨关节炎(OA)与硬化症(软骨下骨板增厚)有关,但对严重膝关节OA患者全层软骨缺损周围的骨适应知之甚少,特别是骨对骨磨损槽下的骨适应。这项高分辨率微计算机断层扫描(microCT)研究旨在量化软骨下骨微观结构与软骨缺损位置、关节间隙距离和凹槽深度的关系。对10例全层软骨缺损的胫骨平台进行显微ct扫描以确定缺损的位置和大小。磨损槽深度估计为从其最深点到从缺陷边缘插值的表面的厚度。分别从三个区域(缺损区、边缘区和软骨覆盖区)和对侧髁上取样2个5 × 5 mm标本,然后进行高分辨率扫描。骨密度曲线作为距离关节空间的函数进行分析,以识别感兴趣的皮质和小梁区域,并计算它们各自的骨密度和微观结构。缺损下皮质骨在磨损沟下的厚度是软骨下的4倍。在深度达5毫米处,三种标本类型的骨密度分布显著不同。缺损以下,皮质孔隙率比软骨覆盖标本高85%,小梁密度高14%。一些骨小梁间隙被编织的骨样组织填充,形成新的皮质层。这些变化局限于缺陷区域,并在缺陷边缘突然停止。骨显微结构指标与估计的骨沟深度之间没有相关性。我们的研究结果表明,在沟的形成过程中,皮质层从其原始位置持续迁移到下面的小梁骨,这一过程我们称之为“小梁皮质化”。在更深的磨损槽下,新的皮质层显示出连接骨髓和关节间隙的大孔隙,表明皮质化的生理限制。这些结果突出了严重骨关节炎软骨缺损下的特定骨适应,并为骨与骨接触区域下软骨下骨变化的进展提供了见解。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
High-resolution microCT analysis of sclerotic subchondral bone beneath bone-on-bone wear grooves in severe osteoarthritis.

Osteoarthritis (OA) is associated with sclerosis, a thickening of the subchondral bone plate, yet little is known about bone adaptations around full-thickness cartilage defects in severe knee OA, particularly beneath bone-on-bone wear grooves. This high-resolution micro-computed tomography (microCT) study aimed to quantify subchondral bone microstructure relative to cartilage defect location, distance from the joint space, and groove depth. Ten tibial plateaus with full-thickness cartilage defects were microCT-scanned to determine defect location and size. Wear groove depth was estimated as the thickness from its deepest point to a surface interpolated from the defect edges. Two 5 × 5 mm specimens were sampled from three regions (defect, edge, and cartilage-covered areas) and two from the contralateral condyle, then scanned at higher resolution. Bone density profiles were analyzed as a function of distance from the joint space to identify cortical and trabecular regions of interest and and compute their respective bone density and microstructure. Cortical bone beneath defects was four times thicker under wear grooves than beneath cartilage. Bone density profiles significantly differed between the three specimen types at depths up to 5 mm. Below defects, cortical porosity was 85 % higher, and trabecular density 14 % higher, than in cartilage-covered specimens. Some trabecular spaces were filled with woven bone-like tissue, forming a new cortical layer. These changes were confined to the defect region and ceased abruptly at the defect edge. No correlation was found between bone microstructural indices and the estimated groove depth. Our findings suggest an ongoing migration of the cortical layer during formation of the groove from its original position into the underlying trabecular bone, a process we termed "trabecular corticalization." Under deeper wear grooves, the new cortical layer exhibited large pores connecting bone marrow to the joint space, suggesting physiological limits to corticalization. These results highlight specific bone adaptations beneath cartilage defects in severe OA and provide insights into the progression of subchondral bone changes under bone-on-bone contact areas.

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