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避免胶原蛋白支架微计算机断层扫描成像中的伪影:磷钨酸(PTA)染色和交联密度的影响

Avoiding artefacts in MicroCT imaging of collagen scaffolds: Effect of phosphotungstic acid (PTA)-staining and crosslink density.

作者信息

Kwon Kyung-Ah, Bax Daniel V, Shepherd Jennifer H, Cameron Ruth E, Best Serena M

机构信息

Cambridge Centre for Medical Materials, Department of Materials Science and Metallurgy, University of Cambridge, Cambridge, United Kingdom.

School of Engineering, University of Leicester, Leicester, United Kingdom.

出版信息

Bioact Mater. 2021 Jun 18;8:210-219. doi: 10.1016/j.bioactmat.2021.06.012. eCollection 2022 Feb.

Abstract

X-ray micro-computed tomography (μ-CT) can be used to provide both qualitative and quantitative information on the structure of three-dimensional (3D) bioactive scaffolds. When performed in a dry state, μ-CT accurately reflects the structure of collagen-based scaffolds, but imaging in a wet state offers challenges with radiolucency. Here we have used phosphotungstic acid (PTA) as a contrast agent to visualise fully hydrated collagen scaffolds in a physiologically relevant environment. A systematic investigation was performed to understand the effects of PTA on the results of μ-CT imaging by varying sample processing variables such as crosslinking density, hydration medium and staining duration. Immersing samples in 0.3% PTA solution overnight completely stained the samples and the treatment provided a successful route for μ-CT analysis of crosslinked samples. However, significant structural artefacts were observed for samples which were either non-crosslinked or had low levels of crosslinking, which had a heterogeneous interior architecture with collapsed pores at the scaffold periphery. This work highlights the importance of optimising the choice of processing and staining conditions to ensure accurate visualisation for hydrated 3D collagen scaffolds in an aqueous medium.

摘要

X射线显微计算机断层扫描(μ-CT)可用于提供有关三维(3D)生物活性支架结构的定性和定量信息。在干燥状态下进行时,μ-CT能准确反映基于胶原蛋白的支架结构,但在湿态下成像会面临射线透过性的挑战。在此,我们使用磷钨酸(PTA)作为造影剂,以在生理相关环境中可视化完全水合的胶原蛋白支架。通过改变诸如交联密度、水合介质和染色持续时间等样品处理变量,进行了系统研究以了解PTA对μ-CT成像结果的影响。将样品在0.3% PTA溶液中浸泡过夜可使样品完全染色,该处理为交联样品的μ-CT分析提供了一条成功途径。然而,对于未交联或交联程度低的样品,观察到显著的结构伪影,这些样品内部结构不均匀,支架周边有塌陷的孔隙。这项工作强调了优化处理和染色条件选择的重要性,以确保在水性介质中对水合3D胶原蛋白支架进行准确可视化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7e04/8424391/4dfccacbce6c/ga1.jpg

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