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Multifactorial Optimization of Contrast-Enhanced Nanofocus Computed Tomography for Quantitative Analysis of Neo-Tissue Formation in Tissue Engineering Constructs

机译:对比度增强纳米聚焦计算机断层扫描的多因素优化用于组织工程构造中新组织形成的定量分析

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摘要

To progress the fields of tissue engineering (TE) and regenerative medicine, development of quantitative methods for non-invasive three dimensional characterization of engineered constructs (i.e. cells/tissue combined with scaffolds) becomes essential. In this study, we have defined the most optimal staining conditions for contrast-enhanced nanofocus computed tomography for three dimensional visualization and quantitative analysis of in vitro engineered neo-tissue (i.e. extracellular matrix containing cells) in perfusion bioreactor-developed Ti6Al4V constructs. A fractional factorial ‘design of experiments’ approach was used to elucidate the influence of the staining time and concentration of two contrast agents (Hexabrix and phosphotungstic acid) and the neo-tissue volume on the image contrast and dataset quality. Additionally, the neo-tissue shrinkage that was induced by phosphotungstic acid staining was quantified to determine the operating window within which this contrast agent can be accurately applied. For Hexabrix the staining concentration was the main parameter influencing image contrast and dataset quality. Using phosphotungstic acid the staining concentration had a significant influence on the image contrast while both staining concentration and neo-tissue volume had an influence on the dataset quality. The use of high concentrations of phosphotungstic acid did however introduce significant shrinkage of the neo-tissue indicating that, despite sub-optimal image contrast, low concentrations of this staining agent should be used to enable quantitative analysis. To conclude, design of experiments allowed us to define the most optimal staining conditions for contrast-enhanced nanofocus computed tomography to be used as a routine screening tool of neo-tissue formation in Ti6Al4V constructs, transforming it into a robust three dimensional quality control methodology.
机译:为了进步组织工程学(TE)和再生医学的领域,开发用于工程化构建体(即细胞/组织与支架相结合)的非侵入性三维表征的定量方法的开发变得至关重要。在这项研究中,我们为灌注生物反应器开发的Ti6Al4V构建体中的体外工程化新组织(即包含细胞外基质的细胞)进行三维可视化和定量分析,为对比度增强的纳米聚焦计算机断层扫描定义了最佳的染色条件。使用分数阶式“实验设计”方法来阐明两种造影剂(六溴化石蜡和磷钨酸)的染色时间和浓度以及新组织体积对图像对比度和数据集质量的影响。另外,对由磷钨酸染色引起的新组织收缩进行定量,以确定可以在其中准确地施加这种造影剂的手术窗口。对于Hexabrix,染色浓度是影响图像对比度和数据集质量的主要参数。使用磷钨酸,染色浓度对图像对比度有显着影响,而染色浓度和新组织体积都对数据集质量有影响。但是,使用高浓度的磷钨酸确实会引起新组织的明显收缩,这表明,尽管图像对比度欠佳,但应使用低浓度的这种染色剂进行定量分析。总而言之,实验设计使我们能够为对比增强的纳米聚焦计算机断层扫描定义最佳的染色条件,以用作Ti6Al4V构建体中新组织形成的常规筛查工具,并将其转化为可靠的三维质量控制方法。

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