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完整的死后幼年大鼠肺脏的微米分辨率X射线断层全容积重建

Micrometer-resolution X-ray tomographic full-volume reconstruction of an intact post-mortem juvenile rat lung.

作者信息

Borisova Elena, Lovric Goran, Miettinen Arttu, Fardin Luca, Bayat Sam, Larsson Anders, Stampanoni Marco, Schittny Johannes C, Schlepütz Christian M

机构信息

Swiss Light Source, Paul Scherrer Institute, 5232, Villigen PSI, Switzerland.

Institute of Anatomy, University of Bern, 3012, Bern, Switzerland.

出版信息

Histochem Cell Biol. 2021 Feb;155(2):215-226. doi: 10.1007/s00418-020-01868-8. Epub 2020 Mar 18.

Abstract

In this article, we present an X-ray tomographic imaging method that is well suited for pulmonary disease studies in animal models to resolve the full pathway from gas intake to gas exchange. Current state-of-the-art synchrotron-based tomographic phase-contrast imaging methods allow for three-dimensional microscopic imaging data to be acquired non-destructively in scan times of the order of seconds with good soft tissue contrast. However, when studying multi-scale hierarchically structured objects, such as the mammalian lung, the overall sample size typically exceeds the field of view illuminated by the X-rays in a single scan and the necessity for achieving a high spatial resolution conflicts with the need to image the whole sample. Several image stitching and calibration techniques to achieve extended high-resolution fields of view have been reported, but those approaches tend to fail when imaging non-stable samples, thus precluding tomographic measurements of large biological samples, which are prone to degradation and motion during extended scan times. In this work, we demonstrate a full-volume three-dimensional reconstruction of an intact rat lung under immediate post-mortem conditions and at an isotropic voxel size of (2.75 µm). We present the methodology for collecting multiple local tomographies with 360° extended field of view scans followed by locally non-rigid volumetric stitching. Applied to the lung, it allows to resolve the entire pulmonary structure from the trachea down to the parenchyma in a single dataset. The complete dataset is available online ( https://doi.org/10.16907/7eb141d3-11f1-47a6-9d0e-76f8832ed1b2 ).

摘要

在本文中,我们提出了一种X射线断层成像方法,该方法非常适合在动物模型中进行肺部疾病研究,以解析从气体吸入到气体交换的完整路径。当前基于同步加速器的先进断层相衬成像方法能够在几秒左右的扫描时间内无损获取三维微观成像数据,且软组织对比度良好。然而,在研究多尺度层次结构的物体(如哺乳动物的肺)时,单个扫描中样本的整体尺寸通常会超过X射线照亮的视野范围,并且实现高空间分辨率的必要性与对整个样本成像的需求相冲突。已经报道了几种用于实现扩展高分辨率视野的图像拼接和校准技术,但这些方法在对不稳定样本成像时往往会失败,从而排除了对大型生物样本的断层测量,因为在长时间扫描过程中,大型生物样本容易降解和移动。在这项工作中,我们展示了在刚死后的条件下对完整大鼠肺进行全容积三维重建,体素大小为各向同性的(2.75 µm)。我们介绍了通过360°扩展视野扫描收集多个局部断层图像,然后进行局部非刚性体积拼接的方法。应用于肺部时,它能够在单个数据集中解析从气管到实质的整个肺部结构。完整的数据集可在线获取(https://doi.org/10.16907/7eb141d3-11f1-47a6-9d0e-76f8832ed1b2)。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0dfa/7910225/5f4a6858863d/418_2020_1868_Fig1_HTML.jpg

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