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未染色病理组织样本的 X 射线显微断层摄影术。

X-ray microtomosynthesis of unstained pathology tissue samples.

机构信息

National Heart, Lung and Blood Institute, National Institutes of Health, Bethesda, Maryland.

College of Medicine, University of Arizona, Tucson, Arizona.

出版信息

J Microsc. 2021 Jul;283(1):9-20. doi: 10.1111/jmi.13003. Epub 2021 Feb 18.

Abstract

In pathology protocols, a tissue block, such as one containing a mouse brain or a biopsy sample from a patient, can produce several hundred thin sections. Substantial time may be required to analyse all sections. In cases of uncertainty regarding which sections to focus on, noninvasive scout imaging of intact blocks can help in guiding the pathology procedure. The scouting step is ideally done in a time window of minutes without special sample preparation that may interfere with the pathology procedures. The challenge is to obtain some visibility of unstained tissue structures at sub-10 µm resolution. We explored a novel x-ray tomosynthesis method as a way to maximise contrast-to-noise ratio, a determinant of tissue visibility. It provided a z-stack of thousands of images at 7.3 μm resolution (10% contrast, half-period of 68.5 line pairs/mm), in scans of 5-15 minutes. When compared with micro-CT scans, the straight-line tomosynthesis scan did not need to rotate the sample, which allowed flat samples, such as paraffin blocks, to be kept as close as possible to the x-ray source. Thus, given the same hardware, scan time and resolution, this mode maximised the photon flux density through the sample, which helped in maximising the contrast-to-noise ratio. The tradeoff of tomosynthesis is incomplete 3D information. The microtomosynthesis scanner has scanned 110 unstained human and animal tissue samples as part of their respective pathology protocols. In all cases, the z-stack of images showed tissue structures that guided sectioning or provided correlative structural information. We describe six examples that presented different levels of visibility of soft tissue structures. Additionally, in a set of coronary artery samples from an HIV patient donor, microtomosynthesis made a new discovery of isolated focal calcification in the internal elastic lamina of coronary wall, which was the onset of medial calcific sclerosis in the arteries.

摘要

在病理学方案中,组织块(例如包含小鼠大脑或患者活检样本的组织块)可以产生数百个薄片。分析所有切片可能需要大量时间。在不确定要关注哪些切片的情况下,对完整块进行非侵入性的侦察成像可以帮助指导病理学程序。侦察步骤的理想时间窗口是几分钟,而无需进行可能干扰病理学程序的特殊样本准备。挑战在于以亚 10µm 的分辨率获得未染色组织结构的一些可见性。我们探索了一种新的 X 射线断层合成方法,以最大限度地提高对比度噪声比,这是组织可见度的决定因素。它在 5-15 分钟的扫描中以 7.3µm 的分辨率(10%对比度,半周期为 68.5 线对/mm)提供了数千张图像的 z 堆叠。与微计算机断层扫描相比,直线断层合成扫描不需要旋转样品,这允许将石蜡块等扁平样品尽可能靠近 X 射线源放置。因此,在相同的硬件、扫描时间和分辨率下,这种模式最大限度地增加了通过样品的光子通量密度,有助于最大限度地提高对比度噪声比。断层合成的缺点是三维信息不完整。微断层合成扫描仪已经扫描了 110 个未染色的人类和动物组织样本,作为其各自病理学方案的一部分。在所有情况下,图像的 z 堆叠都显示了指导切片或提供相关结构信息的组织结构。我们描述了六个示例,这些示例显示了软组织结构的不同可见度。此外,在来自 HIV 患者供体的一组冠状动脉样本中,微断层合成发现了冠状动脉壁内弹性膜中孤立的焦点钙化,这是动脉中层钙化硬化的开始。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/83ea/8248055/9f510590bcea/JMI-283-9-g001.jpg

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