Literature DB >> 20199920

Advanced level-set-based cell tracking in time-lapse fluorescence microscopy.

Oleh Dzyubachyk1, Wiggert A van Cappellen, Jeroen Essers, Wiro J Niessen, Erik Meijering.   

Abstract

Cell segmentation and tracking in time-lapse fluorescence microscopy images is a task of fundamental importance in many biological studies on cell migration and proliferation. In recent years, level sets have been shown to provide a very appropriate framework for this purpose, as they are well suited to capture topological changes occurring during mitosis, and they easily extend to higher dimensional image data. This model evolution approach has also been extended to deal with many cells concurrently. Notwithstanding its high potential, the multiple-level-set method suffers from a number of shortcomings, which limit its applicability to a larger variety of cell biological imaging studies. In this paper, we propose several modifications and extensions to the coupled-active-surfaces algorithm, which considerably improve its robustness and applicability. Our algorithm was validated by comparing it to the original algorithm and two other cell segmentation algorithms. For the evaluation, four real fluorescence microscopy image datasets were used, involving different cell types and labelings that are representative of a large range of biological experiments. Improved tracking performance in terms of precision (up to 11%), recall (up to 8%), ability to correctly capture all cell division events, and computation time (up to nine times reduction) is achieved.

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Year:  2010        PMID: 20199920     DOI: 10.1109/TMI.2009.2038693

Source DB:  PubMed          Journal:  IEEE Trans Med Imaging        ISSN: 0278-0062            Impact factor:   10.048


  48 in total

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Review 7.  Robust Nucleus/Cell Detection and Segmentation in Digital Pathology and Microscopy Images: A Comprehensive Review.

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9.  Automated Cell Segmentation for Quantitative Phase Microscopy.

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10.  Live imaging, identifying, and tracking single cells in complex populations in vivo and ex vivo.

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