4.7 Article

Mathematical imaging methods for mitosis analysis in live-cell phase contrast microscopy

Journal

METHODS
Volume 115, Issue -, Pages 91-99

Publisher

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.ymeth.2017.02.001

Keywords

Phase contrast microscopy; Mitosis analysis; Circular Hough transform; Cell tracking; Variational methods; Level-set methods

Funding

  1. NIHR Cambridge Biomedical Research Centre
  2. ERC [615216 LifeInverse]
  3. German Science Foundation DFG via Cells-in-Motion Cluster of Excellence
  4. EPSRC [EP/M00483X/1]
  5. Leverhulme grant Breaking the non-convexity barrier
  6. EPSRC Centre for Mathematical And Statistical Analysis Of Multimodal Clinical Imaging grant [EP/N014588/1]
  7. Cantab Capital Institute for the Mathematics of Information
  8. Cancer Research UK
  9. University of Cambridge
  10. Hutchison Whampoa Ltd.
  11. Pancreatic Cancer UK
  12. EPSRC [EP/N014588/1, EP/M00483X/1] Funding Source: UKRI
  13. Alan Turing Institute [TU/B/000071] Funding Source: researchfish
  14. Cancer Research UK [22310, 15678] Funding Source: researchfish
  15. Engineering and Physical Sciences Research Council [EP/N014588/1, 1000413, EP/M00483X/1, 1130198] Funding Source: researchfish
  16. Pancreatic Cancer UK [FLF2015_03_Cambridge] Funding Source: researchfish

Ask authors/readers for more resources

In this paper we propose a workflow to detect and track mitotic cells in time-lapse microscopy image,sequences. In order to avoid the requirement for cell lines expressing fluorescent markers and the associated phototoxicity, phase contrast microscopy is often preferred over fluorescence microscopy in live cell imaging. However, common specific image characteristics complicate image processing and impede use of standard methods. Nevertheless, automated analysis is desirable due to manual analysis being subjective, biased and extremely time-consuming for large data sets. Here, we present the following workflow based on mathematical imaging methods. In the first step, mitosis detection is performed by means of the circular Hough transform. The obtained circular contour subsequently serves as an initialisation for the tracking algorithm based on variational methods. It is sub-divided into two parts: in order to determine the beginning of the whole mitosis cycle, a backwards tracking procedure is performed. After that, the cell is tracked forwards in time until the end of mitosis. As a result, the average of mitosis duration and ratios of different cell fates (cell death, no division, division into two or more daughter cells) can be measured and statistics on cell morphologies can be obtained. All of the tools are featured in the userfriendly MATLAB Graphical User Interface MitosisAnalyser. (C) 2017 The Authors. Published by Elsevier Inc.

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