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对不同年龄小鼠干骺端的 3D 分析揭示了早期自发性骨关节炎新的潜在影像学生物标志物。

3D profiling of mouse epiphyses across ages reveals new potential imaging biomarkers of early spontaneous osteoarthritis.

机构信息

Palaeontological Institute & Museum, University of Zurich, Zurich, Switzerland.

Skeletal Biology Group, Comparative Biomedical Sciences, Royal Veterinary College, London, UK.

出版信息

J Anat. 2023 Jun;242(6):1037-1050. doi: 10.1111/joa.13834. Epub 2023 Feb 11.

Abstract

Worldwide research groups and funding bodies have highlighted the need for imaging biomarkers to predict osteoarthritis (OA) progression and treatment effectiveness. Changes in trabecular architecture, which can be detected with non-destructive high-resolution CT imaging, may reveal OA progression before apparent articular surface damage. Here, we analysed the tibial epiphyses of STR/Ort (OA-prone) and CBA (healthy, parental control) mice at different ages to characterise the effects of mouse age and strain on multiple bony parameters. We isolated epiphyseal components using a semi-automated method, and measured the total epiphyseal volume; cortical bone, trabecular bone and marrow space volumes; mean trabecular and cortical bone thicknesses; trabecular volume relative to cortical volume; trabecular volume relative to epiphyseal interior (trabecular BV/TV); and the trabecular degree of anisotropy. Using two-way ANOVA (significance level ≤0.05), we confirmed that all of these parameters change significantly with age, and that the two strains were significantly different in cortical and trabecular bone volumes, and trabecular degree of anisotropy. STR/Ort mice had higher cortical and trabecular volumes and a lower degree of anisotropy. As the two mouse strains reflect markedly divergent OA predispositions, these parameters have potential as bioimaging markers to monitor OA susceptibility and progression. Additionally, significant age/strain interaction effects were identified for total epiphyseal volume, marrow space volume and trabecular BV/TV. These interactions confirm that the two mouse strains have different epiphyseal growth patterns throughout life, some of which emerge prior to OA onset. Our findings not only propose valuable imaging biomarkers of OA, but also provide insight into ageing 3D epiphyseal architecture bone profiles and skeletal biology underlying the onset and development of age-related OA in STR/Ort mice.

摘要

全球研究团队和资助机构强调需要成像生物标志物来预测骨关节炎 (OA) 的进展和治疗效果。通过无损高分辨率 CT 成像可以检测到的小梁结构的变化,可能会在明显的关节表面损伤之前揭示 OA 的进展。在这里,我们分析了不同年龄的 STR/Ort(OA 易感)和 CBA(健康、亲代对照)小鼠的胫骨骺,以描述小鼠年龄和品系对多个骨参数的影响。我们使用半自动方法分离骺成分,并测量总骺体积;皮质骨、小梁骨和骨髓腔体积;平均小梁和皮质骨厚度;小梁体积与皮质体积比;小梁体积与骺内体积比(小梁 BV/TV);以及小梁各向异性程度。使用双因素方差分析(显著性水平≤0.05),我们证实所有这些参数都随年龄显著变化,并且两种品系在皮质骨和小梁骨体积以及小梁各向异性程度上有显著差异。STR/Ort 小鼠具有更高的皮质骨和小梁骨体积以及更低的各向异性程度。由于这两种小鼠品系反映了明显不同的 OA 易感性,因此这些参数有可能成为监测 OA 易感性和进展的生物成像标志物。此外,总骺体积、骨髓腔体积和小梁 BV/TV 还确定了显著的年龄/品系相互作用效应。这些相互作用证实,这两种小鼠品系在整个生命周期中具有不同的骺生长模式,其中一些在 OA 发病前就已经出现。我们的研究结果不仅提出了有价值的 OA 成像生物标志物,而且深入了解了 STR/Ort 小鼠中与年龄相关的 OA 发病和发展相关的 3D 骺结构骨骼生物学。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1f67/10184544/c09d8fb25401/JOA-242-1037-g003.jpg

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