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首页> 外文期刊>Medical Imaging, IEEE Transactions on >Multiple Nuclei Tracking Using Integer Programming for Quantitative Cancer Cell Cycle Analysis
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Multiple Nuclei Tracking Using Integer Programming for Quantitative Cancer Cell Cycle Analysis

机译:使用整数编程进行多核跟踪以定量癌细胞周期分析

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摘要

Automated cell segmentation and tracking are critical for quantitative analysis of cell cycle behavior using time-lapse fluorescence microscopy. However, the complex, dynamic cell cycle behavior poses new challenges to the existing image segmentation and tracking methods. This paper presents a fully automated tracking method for quantitative cell cycle analysis. In the proposed tracking method, we introduce a neighboring graph to characterize the spatial distribution of neighboring nuclei, and a novel dissimilarity measure is designed based on the spatial distribution, nuclei morphological appearance, migration, and intensity information. Then, we employ the integer programming and division matching strategy, together with the novel dissimilarity measure, to track cell nuclei. We applied this new tracking method for the tracking of HeLa cancer cells over several cell cycles, and the validation results showed that the high accuracy for segmentation and tracking at 99.5% and 90.0%, respectively. The tracking method has been implemented in the cell–cycle analysis software package, DCELLIQ, which is freely available.
机译:使用延时荧光显微镜对细胞周期行为进行定量分析对于细胞周期行为的自动分析至关重要。然而,复杂,动态的细胞周期行为对现有的图像分割和跟踪方法提出了新的挑战。本文提出了一种用于定量细胞周期分析的全自动跟踪方法。在提出的跟踪方法中,我们引入了一个相邻图来表征相邻原子核的空间分布,并基于空间分布,原子核形态,迁移和强度信息设计了一种新的相异性度量。然后,我们采用整数规划和除法匹配策略,以及新颖的相异性测度,来跟踪细胞核。我们将这种新的跟踪方法应用于多个细胞周期中的HeLa癌细胞跟踪,验证结果表明,分割和跟踪的准确率分别为99.5%和90.0%。跟踪方法已在细胞周期分析软件包DCELLIQ中实现,该软件包可免费获得。

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