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基于同步辐射 X 射线相衬的微计算机断层扫描的全心详细定量解剖、肌纤维结构和脉管系统。

Whole heart detailed and quantitative anatomy, myofibre structure and vasculature from X-ray phase-contrast synchrotron radiation-based micro computed tomography.

机构信息

Fetal i+D Fetal Medicine Research Center, BCNatal-Barcelona Center for Maternal-Fetal and Neonatal Medicine (Hospital Clínic and Hospital Sant Joan de Deu), IDIBAPS, University of Barcelona, and Centre for Biomedical Research on Rare Diseases (CIBER-ER), Barcelona, Spain.

PhySense, DTIC, Universitat Pompeu Fabra, Barcelona, Spain.

出版信息

Eur Heart J Cardiovasc Imaging. 2017 Jul 1;18(7):732-741. doi: 10.1093/ehjci/jew314.

DOI:10.1093/ehjci/jew314
PMID:28329054
Abstract

BACKGROUND

While individual cardiac myocytes only have a limited ability to shorten, the heart efficiently pumps a large volume-fraction thanks to a cell organization in a complex 3D fibre structure. Subclinical subtle cardiac structural remodelling is often present before symptoms arise. Understanding and early detection of these subtle changes is crucial for diagnosis and prevention. Additionally, personalized computational modelling requires knowledge on the multi-scale structure of the whole heart and vessels.

METHODS AND RESULTS

We developed a rapid acquisition together with visualization and quantification methods of the integrated microstructure of whole in-vitro rodents hearts using synchrotron based X-ray phase-contrast tomography. These images are formed not only by X-ray absorption by the tissue but also by wave propagation phenomena, enhancing structural information, thus allowing to raise tissue contrast to an unprecedented level. We used a (ex-vivo) normal rat heart and fetal rabbit hearts suffering intrauterine growth restriction as a model of subclinical cardiac remodelling to illustrate the strengths and potential of the technique. For comparison, histology and diffusion tensor magnetic resonance imaging was performed.

CONCLUSIONS

We have developed a novel, high resolution, image acquisition, and quantification approach to study a whole in-vitro heart at myofibre resolution, providing integrated 3D structural information at microscopic level without any need of tissue slicing and processing. This superior imaging approach opens up new possibilities for a systems approach towards analysing cardiac structure and function, providing rapid acquisition of quantitative microstructure of the heart in a near native state.

摘要

背景

虽然单个心肌细胞缩短的能力有限,但由于心脏在复杂的 3D 纤维结构中组织成细胞,因此心脏能够有效地泵出大量的分数体积。在出现症状之前,通常存在亚临床微妙的心脏结构重塑。了解和早期发现这些细微变化对于诊断和预防至关重要。此外,个性化计算模型需要了解整个心脏和血管的多尺度结构。

方法和结果

我们使用基于同步加速器的 X 射线相衬层析成像技术,开发了一种快速获取、可视化和量化整个体外啮齿动物心脏整体微观结构的方法。这些图像不仅由组织对 X 射线的吸收形成,还由波传播现象形成,增强了结构信息,从而可以将组织对比度提高到前所未有的水平。我们使用(离体)正常大鼠心脏和宫内生长受限的胎兔心脏作为亚临床心脏重塑的模型,说明了该技术的优势和潜力。为了进行比较,还进行了组织学和扩散张量磁共振成像。

结论

我们开发了一种新颖的、高分辨率的图像采集和量化方法,可在肌纤维分辨率下研究整个体外心脏,提供微观水平的集成 3D 结构信息,而无需任何组织切片和处理。这种优越的成像方法为分析心脏结构和功能的系统方法开辟了新的可能性,可快速获取近自然状态下心脏的定量微观结构。

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