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Monitoring in vivo (re)modeling: A computational approach using 4D microCT data to quantify bone surface movements

机译:监测体内(重新)建模:一种使用4D microCT数据量化骨表面运动的计算方法

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Bone undergoes continual damage repair and structural adaptation to changing external loads with the aim of maintaining skeletal integrity throughout life. The ability to monitor bone (re)modeling would allow for a better understanding in how various pathologies and interventions affect bone turnover and subsequent bone strength. To date, however, current methods to monitor bone (re)modeling over time and in space are limited. We propose a novel method to visualize and quantify bone turnover, based on in vivo microCT imaging and a 4D computational approach. By in vivo tracking of spatially correlated formation and resorption sites over time it classifies bone restructuring into (re)modeling sequences, the spatially and temporally linked sequences of formation, resorption and quiescent periods on the bone surface. The microCT based method was validated using experimental data from an in vivo mouse tibial loading model and ex vivo data of the mouse tibia. In this application, the method allows the visualization of time-resolved cortical (re)modeling and the quantification of short-term and long-term modeling on the endocortical and periosteal surface at the mid-diaphysis of loaded and control mice tibiae. Both short-term and long-term modeling processes, independent formation and resorption events, could be monitored and modeling (spatially not correlated formation and resorption) and remodeling (resorption followed by new formation at the same site) could be distinguished on the bone surface. This novel method that combines in vivo microCT with a computational approach is a powerful tool to monitor bone turnover in animal models now and is waiting to be applied to human patients in the near future. (C) 2015 Elsevier Inc. All rights reserved.
机译:骨骼经过不断的损伤修复和结构调整,以适应不断变化的外部载荷,目的是在整个生命中保持骨骼完整性。监视骨骼(重新建模)的能力将使人们更好地了解各种病理和干预如何影响骨骼更新和随后的骨骼强度。但是,迄今为止,用于监视随时间和空间变化的骨骼(重新)建模的当前方法受到限制。我们提出了一种基于体内microCT成像和4D计算方法的可视化和量化骨转换的新颖方法。通过随时间进行体内跟踪与空间相关的形成和吸收位点,它可以将骨重建分为(重新)建模序列,在骨表面上形成,吸收和静止期的空间和时间相关序列。使用来自体内小鼠胫骨加载模型的实验数据和小鼠胫骨的离体数据验证了基于microCT的方法。在此应用中,该方法可以可视化时间分辨的皮质(重塑)模型,并可以量化负荷和对照小鼠胫骨中骨干处皮质内膜和骨膜表面上短期和长期模型的数量。可以监测短期和长期的建模过程,独立的形成和吸收事件,并可以在骨表面上区分建模(空间上不相关的形成和吸收)和重塑(在同一部位吸收然后有新的形成) 。这种将体内microCT与计算方法结合起来的新颖方法现在是监视动物模型中骨骼更新的强大工具,并且正等待不久的将来应用于人类患者。 (C)2015 Elsevier Inc.保留所有权利。

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