小鼠骨折愈伤组织组成及细胞特性的时空特征。

IF 9.6
Tobias M Ballhause, Ana Ocokoljic, Jan Sevecke, Alexander Simon, Anke Baranowsky, Assil-Ramin Alimy, Frank Timo Beil, Karl-Heinz Frosch, Johannes Keller, Tim Rolvien
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引用次数: 0

摘要

对骨愈合及其损伤(即骨不连)的生理过程的理解的进展需要适当的模型和精确的标准化。股骨截骨外固定小鼠模型满足这些要求,但骨愈合过程中骨痂矿化的全面时空特征尚未得到。在这里,我们在愈合骨内划分了三个区域,并检查了截骨后的八个时间点。我们能够证明随着软骨内成骨,骨痂矿化逐渐增加。我们进一步证明了血管化的暂时增加,随后增加了骨骼的建模和重塑活动。这可以通过h型血管的短暂高丰度、骨矿化异质性的增加和骨细胞数量的强烈增加来证明。值得注意的是,在骨折愈合级联结束时,骨折骨痂附近的皮质骨发生脱矿,表明前骨折附近有相当大的再骨折风险。综上所述,我们的研究结果在显微结构、细胞和骨质量水平上深入了解了愈伤组织矿化的进程,为在多个长度尺度下各自参数的量化提供了参考,可用于该领域的未来研究。意义声明:我们的数据通过对骨痂组织的多模态分析提供了第一个关于小鼠骨折愈合的综合观点,重点是矿化、细胞骨转换和纳米力学。从几个时间点(7、9、11、13、15、17、21和28天)获得的结果,以及愈合骨内和周围不同区域的包含,使我们能够提供证据,证明机械敏感骨细胞的短暂参与以及未骨折骨钙的动员。我们的数据也为科学家在解释小鼠骨折愈合数据时提供了有用的多维参考价值。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Spatio-temporal characterization of compositional and cellular properties in the murine fracture callus.

Advances in the understanding of the physiological process of bone healing and its impairment (i.e., nonunion) require appropriate models and precise standardization. The femoral osteotomy and external fixation mouse model meets these requirements, but a comprehensive spatio-temporal characterization of callus mineralization along the bone healing process has not been available. Here, we differentiated into three regions within the healing bone and examined eight time points post-osteotomy. We were able to demonstrate a gradual increase in callus mineralization alongside endochondral ossification. We further demonstrated a temporary increase in vascularization, followed by increased modeling and remodeling activity of the bone. This was evidenced by a transient high abundance of type-H vessels, increased bone mineralization heterogeneity, and a strong increase in osteocyte numbers. Notably, at the end of the fracture healing cascade, demineralization occurred in the cortical bone adjacent to the fracture callus, suggesting a considerable risk of refracture in the vicinity of the former fracture. In summary, our results provide insight into the progression of callus mineralization at the microstructural, cellular and bone quality levels, providing a reference for the quantification of respective parameters at multiple length scales, which can be used for future studies in this field. STATEMENT OF SIGNIFICANCE: Our data provide the first comprehensive view of murine fracture healing through the multimodal analysis of callus tissue focusing on mineralization, cellular bone turnover, and nanomechanics. The results obtained from several time points (7, 9, 11, 13, 15, 17, 21 and 28 days) and the inclusion of different regions in and around the healing bone allowed us to provide evidence for the transient involvement of mechanosensitive osteocytes as well as the mobilization of calcium from the unfractured bone. Our data also provide scientists with useful multidimensional reference values when interpreting data on fracture healing in mice.

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