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An Energy-Based Three-Dimensional Segmentation Approach for the Quantitative Interpretation of Electron Tomograms

机译:基于能量的三维分割方法用于电子断层图的定量解释

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Electron tomography allows for the determination of the three-dimensional structures of cells and tissues at resolutions significantly higher than that which is possible with optical microscopy. Electron tomograms contain, in principle, vast amounts of information on the locations and architectures of large numbers of subcellular assemblies and organelles. The development of reliable quantitative approaches for the analysis of features in tomograms is an important problem, and a challenging prospect due to the low signal-to-noise ratios that are inherent to biological electron microscopic images. This is, in part, a consequence of the tremendous complexity of biological specimens. We report on a new method for the automated segmentation of HIV particles and selected cellular compartments in electron tomograms recorded from fixed, plastic-embedded sections derived from HIV-infected human macrophages. Individual features in the tomogram are segmented using a novel robust algorithm that finds their boundaries as global minimal surfaces in a metric space defined by image features. The optimization is carried out in a transformed spherical domain with the center an interior point of the particle of interest, providing a proper setting for the fast and accurate minimization of the segmentation energy. This method provides tools for the semi-automated detection and statistical evaluation of HIV particles at different stages of assembly in the cells and presents opportunities for correlation with biochemical markers of HIV infection. The segmentation algorithm developed here forms the basis of the automated analysis of electron tomograms and will be especially useful given the rapid increases in the rate of data acquisition. It could also enable studies of much larger data sets, such as those which might be obtained from the tomographic analysis of HIV-infected cells from studies of large populations.
机译:电子断层扫描可以确定细胞和组织的三维结构,其分辨率明显高于光学显微镜所能达到的分辨率。电子断层图原则上包含有关大量亚细胞装配体和细胞器的位置和结构的大量信息。用于分析断层图像特征的可靠的定量方法是一个重要的问题,并且由于生物电子显微图像固有的低信噪比,因此具有挑战性的前景。部分原因是生物标本的高度复杂性。我们报告了一种新的方法,用于自动分割HIV颗粒和电子断层图中选定的细胞隔室,该电子断层图中记录了来自感染HIV的人类巨噬细胞的固定塑料包埋部分。使用新颖的鲁棒算法对断层图中的各个特征进行分割,该算法将其边界作为由图像特征定义的度量空间中的全局最小曲面来查找。优化是在一个变换的球面域中进行的,其中心是目标粒子的内部点,为快速准确地最小化分段能量提供了适当的设置。该方法提供了用于在细胞组装的不同阶段对HIV颗粒进行半自动检测和统计评估的工具,并为与HIV感染的生化标志物相关提供了机会。此处开发的分割算法构成了电子断层图自动分析的基础,鉴于数据采集速率的迅速提高,该算法将特别有用。它也可以用于研究更大的数据集,例如可以从对大批人群进行的HIV感染细胞的层析成像分析中获得的数据集。

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