599 research outputs found

    Model-based Curvilinear Network Extraction and Tracking toward Quantitative Analysis of Biopolymer Networks

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    Curvilinear biopolymer networks pervade living systems. They are routinely imaged by fluorescence microscopy to gain insight into their structural, mechanical, and dynamic properties. Image analysis can facilitate understanding the mechanisms of their formation and their biological functions from a quantitative viewpoint. Due to the variability in network geometry, topology and dynamics as well as often low resolution and low signal-to-noise ratio in images, segmentation and tracking networks from these images is challenging. In this dissertation, we propose a complete framework for extracting the geometry and topology of curvilinear biopolymer networks, and also tracking their dynamics from multi-dimensional images. The proposed multiple Stretching Open Active Contours (SOACs) can identify network centerlines and junctions, and infer plausible network topology. Combined with a kk-partite matching algorithm, temporal correspondences among all the detected filaments can be established. This work enables statistical analysis of structural parameters of biopolymer networks as well as their dynamics. Quantitative evaluation using simulated and experimental images demonstrate its effectiveness and efficiency. Moreover, a principled method of optimizing key parameters without ground truth is proposed for attaining the best extraction result for any type of images. The proposed methods are implemented into a usable open source software ``SOAX\u27\u27. Besides network extraction and tracking, SOAX provides a user-friendly cross-platform GUI for interactive visualization, manual editing and quantitative analysis. Using SOAX to analyze several types of biopolymer networks demonstrates the potential of the proposed methods to help answer key questions in cell biology and biophysics from a quantitative viewpoint

    A survey of visual preprocessing and shape representation techniques

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    Many recent theories and methods proposed for visual preprocessing and shape representation are summarized. The survey brings together research from the fields of biology, psychology, computer science, electrical engineering, and most recently, neural networks. It was motivated by the need to preprocess images for a sparse distributed memory (SDM), but the techniques presented may also prove useful for applying other associative memories to visual pattern recognition. The material of this survey is divided into three sections: an overview of biological visual processing; methods of preprocessing (extracting parts of shape, texture, motion, and depth); and shape representation and recognition (form invariance, primitives and structural descriptions, and theories of attention)

    Contour integration: Psychophysical, neurophysiological, and computational perspectives

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    One of the important roles of our visual system is to detect and segregate objects. Neurons in the early visual system extract local image features from the visual scene. To combine these features into separate, global objects, the visual system must perform some kind of grouping operation. One such operation is contour integration. Contours form the outlines of objects, and are the first step in shape perception. We discuss the mechanism of contour integration from psychophysical, neurophysiological, and computational perspectives

    Retinal Fundus Image Analysis for Diagnosis of Glaucoma: A Comprehensive Survey

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    © 2016 IEEE. The rapid development of digital imaging and computer vision has increased the potential of using the image processing technologies in ophthalmology. Image processing systems are used in standard clinical practices with the development of medical diagnostic systems. The retinal images provide vital information about the health of the sensory part of the visual system. Retinal diseases, such as glaucoma, diabetic retinopathy, age-related macular degeneration, Stargardt's disease, and retinopathy of prematurity, can lead to blindness manifest as artifacts in the retinal image. An automated system can be used for offering standardized large-scale screening at a lower cost, which may reduce human errors, provide services to remote areas, as well as free from observer bias and fatigue. Treatment for retinal diseases is available; the challenge lies in finding a cost-effective approach with high sensitivity and specificity that can be applied to large populations in a timely manner to identify those who are at risk at the early stages of the disease. The progress of the glaucoma disease is very often quiet in the early stages. The number of people affected has been increasing and patients are seldom aware of the disease, which can cause delay in the treatment. A review of how computer-aided approaches may be applied in the diagnosis and staging of glaucoma is discussed here. The current status of the computer technology is reviewed, covering localization and segmentation of the optic nerve head, pixel level glaucomatic changes, diagonosis using 3-D data sets, and artificial neural networks for detecting the progression of the glaucoma disease

    Anatomy Segmentation of Breast Ultrasound images

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    Breast cancer is one of the most common cancers in women, affecting hundreds of women. Even though the detection of cancer has been largely studied, the decision of which strategy to take concerning oncoplastic surgery still relies almost exclusively on the surgeon's perception of post-surgical aesthetic result, which sometime leads to unsatisfactory outcomes. In order to empower the patients on the joint decision process there needs to exist a better communication between the parts. This can be achieved by developing medical grade 3D models of the breast and explaining better the surgical options and their results. In order to obtain such models, some effort has been made concerning multi-modality radiological imaging combination. This line of research has yet to mature. In turn, the modality alignment requires accurate landmarks to be produced. 2D Ultrasound imaging has not been sufficiently studied for multimodal registration due to the image characteristics and thus, landmark segmentation is of utmost importance. This task can be challenging since US data presents high specular noise levels and the presence of some tissues alters the perception of other tissues. Objectives: ● Study and evaluation of different techniques for anatomical landmark segmentation, such as Skin, Fat and Glandular tissue, Lesions (masses and cysts), Pectoral muscle; ● Development of Ultrasound segmentation methods for acquiring landmarks; ● Evaluation of the developed methods with manual annotations and comparison of results with the current algorithm alternatives.Breast cancer is one of the most common cancers in women, affecting hundreds of women. Even though the detection of cancer has been largely studied, the decision of which strategy to take concerning oncoplastic surgery still relies almost exclusively on the surgeon's perception of post-surgical aesthetic result, which sometime leads to unsatisfactory outcomes. In order to empower the patients on the joint decision process there needs to exist a better communication between the parts. This can be achieved by developing medical grade 3D models of the breast and explaining better the surgical options and their results. In order to obtain such models, some effort has been made concerning multi-modality radiological imaging combination. This line of research has yet to mature. In turn, the modality alignment requires accurate landmarks to be produced. 2D Ultrasound imaging has not been sufficiently studied for multimodal registration due to the image characteristics and thus, landmark segmentation is of utmost importance. This task can be challenging since US data presents high specular noise levels and the presence of some tissues alters the perception of other tissues. Objectives: ● Study and evaluation of different techniques for anatomical landmark segmentation, such as Skin, Fat and Glandular tissue, Lesions (masses and cysts), Pectoral muscle; ● Development of Ultrasound segmentation methods for acquiring landmarks; ● Evaluation of the developed methods with manual annotations and comparison of results with the current algorithm alternatives

    A 2D/3D image analysis system to track fluorescently labeled structures in rod-shaped cells: application to measure spindle pole asymmetry during mitosis.

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    BACKGROUND: The yeast Schizosaccharomyces pombe is frequently used as a model for studying the cell cycle. The cells are rod-shaped and divide by medial fission. The process of cell division, or cytokinesis, is controlled by a network of signaling proteins called the Septation Initiation Network (SIN); SIN proteins associate with the SPBs during nuclear division (mitosis). Some SIN proteins associate with both SPBs early in mitosis, and then display strongly asymmetric signal intensity at the SPBs in late mitosis, just before cytokinesis. This asymmetry is thought to be important for correct regulation of SIN signaling, and coordination of cytokinesis and mitosis. In order to study the dynamics of organelles or large protein complexes such as the spindle pole body (SPB), which have been labeled with a fluorescent protein tag in living cells, a number of the image analysis problems must be solved; the cell outline must be detected automatically, and the position and signal intensity associated with the structures of interest within the cell must be determined. RESULTS: We present a new 2D and 3D image analysis system that permits versatile and robust analysis of motile, fluorescently labeled structures in rod-shaped cells. We have designed an image analysis system that we have implemented as a user-friendly software package allowing the fast and robust image-analysis of large numbers of rod-shaped cells. We have developed new robust algorithms, which we combined with existing methodologies to facilitate fast and accurate analysis. Our software permits the detection and segmentation of rod-shaped cells in either static or dynamic (i.e. time lapse) multi-channel images. It enables tracking of two structures (for example SPBs) in two different image channels. For 2D or 3D static images, the locations of the structures are identified, and then intensity values are extracted together with several quantitative parameters, such as length, width, cell orientation, background fluorescence and the distance between the structures of interest. Furthermore, two kinds of kymographs of the tracked structures can be established, one representing the migration with respect to their relative position, the other representing their individual trajectories inside the cell. This software package, called "RodCellJ", allowed us to analyze a large number of S. pombe cells to understand the rules that govern SIN protein asymmetry. CONCLUSIONS: "RodCell" is freely available to the community as a package of several ImageJ plugins to simultaneously analyze the behavior of a large number of rod-shaped cells in an extensive manner. The integration of different image-processing techniques in a single package, as well as the development of novel algorithms does not only allow to speed up the analysis with respect to the usage of existing tools, but also accounts for higher accuracy. Its utility was demonstrated on both 2D and 3D static and dynamic images to study the septation initiation network of the yeast Schizosaccharomyces pombe. More generally, it can be used in any kind of biological context where fluorescent-protein labeled structures need to be analyzed in rod-shaped cells. AVAILABILITY: RodCellJ is freely available under http://bigwww.epfl.ch/algorithms.html, (after acceptance of the publication)

    Surface-guided computing to analyze subcellular morphology and membrane-associated signals in 3D

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    Signal transduction and cell function are governed by the spatiotemporal organization of membrane-associated molecules. Despite significant advances in visualizing molecular distributions by 3D light microscopy, cell biologists still have limited quantitative understanding of the processes implicated in the regulation of molecular signals at the whole cell scale. In particular, complex and transient cell surface morphologies challenge the complete sampling of cell geometry, membrane-associated molecular concentration and activity and the computing of meaningful parameters such as the cofluctuation between morphology and signals. Here, we introduce u-Unwrap3D, a framework to remap arbitrarily complex 3D cell surfaces and membrane-associated signals into equivalent lower dimensional representations. The mappings are bidirectional, allowing the application of image processing operations in the data representation best suited for the task and to subsequently present the results in any of the other representations, including the original 3D cell surface. Leveraging this surface-guided computing paradigm, we track segmented surface motifs in 2D to quantify the recruitment of Septin polymers by blebbing events; we quantify actin enrichment in peripheral ruffles; and we measure the speed of ruffle movement along topographically complex cell surfaces. Thus, u-Unwrap3D provides access to spatiotemporal analyses of cell biological parameters on unconstrained 3D surface geometries and signals.Comment: 49 pages, 10 figure
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