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首页> 外文期刊>Journal of tissue engineering and regenerative medicine >Multi-modal imaging for assessment of tissue-engineered bone in a critical-sized calvarial defect mouse model
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Multi-modal imaging for assessment of tissue-engineered bone in a critical-sized calvarial defect mouse model

机译:用于评估临界大小缺陷鼠标模型中组织工程骨的多模态成像

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Tissue-engineered bone (TEB) analysis in vivo relies heavily on tissue histological and end-point evaluations requiring the sacrifice of animals at specific time points. Due to differences in animal response to implanted tissues, the conventional analytical methods to evaluate TEB can introduce data inconsistencies. Additionally, the conventional methods increase the number of animals required to provide an acceptable statistical power for hypothesis testing. Alternatively, our non-invasive optical imaging allows for the longitudinal analysis of regenerating tissue, where each animal acts as its own control, thus reducing overall animal numbers. In our 6 month feasibility study, TEB, consisting of a silk protein scaffold with or without differentiated mesenchymal stem cells, was implanted in a critical-sized calvarial defect mouse model. Osteogenesis of the TEB was monitored through signal variation, using magnetic resonance imaging (MRI) and near-infrared (NIR) optical imaging with IRDye (R) 800CW BoneTag(TM) (800CW BT, a bone-specific marker used to label osteogenically differentiated mesenchymal stem cells and mineralization). Histological endpoint measurements and computed tomography (CT) were used to confirm imaging findings. Anatomical MRI revealed decreased signal intensity, indicating mineralization, in the TEB compared to the control (i.e. silk scaffold only) at various growth stages. NIR optical imaging results demonstrated a signal intensity increase of the TEB compared to control. Interpretation of the imaging results were confirmed by histological analysis. Specifically, haematoxylin and eosin staining revealing de novo bone in TEB showed that 80% of the defect was covered by TEB, while only 40% was covered for the control. Taken together, these results demonstrate the potential of multi-modal non-invasive imaging to visualize and quantify TEB for the assessment of regenerative medicine strategies. Copyright (c) 2015 John Wiley & Sons, Ltd.
机译:体内组织工程骨(TEB)分析严重依赖于需要在特定时间点牺牲动物的组织组织学和终点评估。由于动物反应对植入组织的差异,评估TEB的常规分析方法可以引入数据不一致。另外,传统方法增加了为假设检测提供可接受的统计功率所需的动物的数量。或者,我们的非侵入性光学成像允许再生组织的纵向分析,其中每只动物充当其自身的控制,从而减少了整体动物数。在我们的6个月可行性研究中,TEB,由具有或不具有分化的间充质干细胞的丝蛋白支架组成,植入临界大小的颅骨缺陷小鼠模型中。通过信号变化监测TEB的骨发生,使用磁共振成像(MRI)和近红外(NIR)光学成像与IRDYE(R)800cW Bonetag(TM)(800cW BT,用于标记骨开发的骨特异性标记物间充质干细胞和矿化)。组织学终点测量和计算断层扫描(CT)用于确认成像结果。与在各种生长阶段的控制(即丝绸支架仅)相比,解剖学MRI揭示了TEB中的信号强度下降,表明矿化,在TEB中。 NIR光学成像结果表明TEB的信号强度增加与控制相比。通过组织学分析证实了对成像结果的解释。具体而言,在TEB中揭示De Novo Bone的血红素和曙红染色表明TEB覆盖了80%的缺陷,而仅覆盖40%的控制。总之,这些结果证明了多模态非侵入性成像的潜力,以可视化和量化TEB以评估再生医学策略。版权所有(c)2015 John Wiley&Sons,Ltd。

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