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使用单细胞计算机断层扫描和三维核型计量学对癌前病变进展进行定量描述。

Quantitative characterization of preneoplastic progression using single-cell computed tomography and three-dimensional karyometry.

机构信息

School of Electrical, Computer, and Energy Engineering, Arizona State University, Tempe, Arizona, USA.

出版信息

Cytometry A. 2011 Jan;79(1):25-34. doi: 10.1002/cyto.a.20997.

Abstract

The development of morphological biosignatures to precisely characterize preneoplastic progression necessitates high-resolution three-dimensional (3D) cell imagery and robust image processing algorithms. We report on the quantitative characterization of nuclear structure alterations associated with preneoplastic progression in human esophageal epithelial cells using single-cell optical tomography and fully automated 3D karyometry. We stained cultured cells with hematoxylin and generated 3D images of individual cells by mathematically reconstructing 500 projection images acquired using optical absorption tomographic imaging. For 3D karyometry, we developed novel, fully automated algorithms to robustly segment the cellular, nuclear, and subnuclear components in the acquired cell images, and computed 41 quantitative morphological descriptors from these segmented volumes. In addition, we developed algorithms to quantify the spatial distribution and texture of the nuclear DNA. We applied our methods to normal, metaplastic, and dysplastic human esophageal epithelial cell lines, analyzing 100 cells per line. The 3D karyometric descriptors elucidated quantitative differences in morphology and enabled robust discrimination between cell lines on the basis of extracted morphological features. The morphometric hallmarks of cancer progression such as increased nuclear size, elevated nuclear content, and anomalous chromatin texture and distribution correlated with this preneoplastic progression model, pointing to the clinical use of our method for early cancer detection.

摘要

为了精确地描述肿瘤前进展,需要发展形态学生物标志物,这需要高分辨率的三维(3D)细胞成像和强大的图像处理算法。我们报告了使用单细胞光学层析成像和全自动 3D 核型计量学对人食管上皮细胞肿瘤前进展相关核结构改变的定量特征分析。我们用苏木精对培养的细胞进行染色,并通过数学重建使用光学吸收层析成像获取的 500 个投影图像,生成单个细胞的 3D 图像。对于 3D 核型计量学,我们开发了新的、全自动的算法,以稳健地分割获取的细胞图像中的细胞、核和亚核成分,并从这些分割的体积中计算了 41 个定量形态描述符。此外,我们开发了算法来量化核 DNA 的空间分布和纹理。我们将我们的方法应用于正常、化生和异型增生的人食管上皮细胞系,每条线分析 100 个细胞。3D 核型计量学描述符阐明了形态上的定量差异,并能够基于提取的形态特征稳健地区分细胞系。癌症进展的形态特征,如核增大、核含量升高以及异常染色质纹理和分布,与这个肿瘤前进展模型相关,这表明我们的方法可用于早期癌症检测。

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