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个体化循环机械加载可改善骨折愈合重塑阶段骨痂的特性,通过延迟活体成像评估。

Individualized cyclic mechanical loading improves callus properties during the remodelling phase of fracture healing in mice as assessed from time-lapsed in vivo imaging.

机构信息

Institute for Biomechanics, ETH Zurich, Leopold-Ruzicka-Weg 4, 8093, Zurich, Switzerland.

出版信息

Sci Rep. 2021 Nov 29;11(1):23037. doi: 10.1038/s41598-021-02368-y.

Abstract

Fracture healing is regulated by mechanical loading. Understanding the underlying mechanisms during the different healing phases is required for targeted mechanical intervention therapies. Here, the influence of individualized cyclic mechanical loading on the remodelling phase of fracture healing was assessed in a non-critical-sized mouse femur defect model. After bridging of the defect, a loading group (n = 10) received individualized cyclic mechanical loading (8-16 N, 10 Hz, 5 min, 3 × /week) based on computed strain distribution in the mineralized callus using animal-specific real-time micro-finite element analysis with 2D/3D visualizations and strain histograms. Controls (n = 10) received 0 N treatment at the same post-operative time-points. By registration of consecutive scans, structural and dynamic callus morphometric parameters were followed in three callus sub-volumes and the adjacent cortex showing that the remodelling phase of fracture healing is highly responsive to cyclic mechanical loading with changes in dynamic parameters leading to significantly larger formation of mineralized callus and higher degree of mineralization. Loading-mediated maintenance of callus remodelling was associated with distinct effects on Wnt-signalling-associated molecular targets Sclerostin and RANKL in callus sub-regions and the adjacent cortex (n = 1/group). Given these distinct local protein expression patterns induced by cyclic mechanical loading during callus remodelling, the femur defect loading model with individualized load application seems suitable to further understand the local spatio-temporal mechano-molecular regulation of the different fracture healing phases.

摘要

骨折愈合受机械加载调控。为了实现针对机械干预疗法的目标,需要了解不同愈合阶段的潜在机制。在这里,我们在非关键性大小的小鼠股骨缺损模型中评估了个体化循环机械加载对骨折愈合重塑阶段的影响。在缺损桥接后,加载组(n=10)根据使用动物特异性实时微有限元分析的二维/三维可视化和应变直方图对矿化骨痂中的计算应变分布,接受基于个体化的循环机械加载(8-16 N,10 Hz,5 分钟,3×/周)。对照组(n=10)在相同的术后时间点接受 0 N 处理。通过连续扫描的注册,在三个骨痂子体积和相邻皮质中跟踪结构和动态骨痂形态计量参数,结果表明骨折愈合的重塑阶段对循环机械加载高度敏感,动态参数的变化导致矿化骨痂形成显著增加和矿化程度显著提高。加载介导的骨痂重塑维持与骨痂子区域和相邻皮质中的 Wnt 信号相关的分子靶标 Sclerostin 和 RANKL 明显相关(n=1/组)。鉴于在骨痂重塑过程中循环机械加载引起的这些明显的局部蛋白表达模式,具有个体化负荷应用的股骨缺损加载模型似乎适合进一步了解不同骨折愈合阶段的局部时空机械分子调控。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/202d/8630002/2a674d4a9f89/41598_2021_2368_Fig1_HTML.jpg

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