Cell segmentation of in situ transcriptomics data using signed graph partitioning
December 07, 2023 Β· Declared Dead Β· π Workshop on Graph Based Representations in Pattern Recognition
"No code URL or promise found in abstract"
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Authors
Axel Andersson, Andrea Behanova, Carolina WΓ€hlby, Filip Malmberg
arXiv ID
2312.04181
Category
cs.IT: Information Theory
Cross-listed
q-bio.QM
Citations
0
Venue
Workshop on Graph Based Representations in Pattern Recognition
Last Checked
4 months ago
Abstract
The locations of different mRNA molecules can be revealed by multiplexed in situ RNA detection. By assigning detected mRNA molecules to individual cells, it is possible to identify many different cell types in parallel. This in turn enables investigation of the spatial cellular architecture in tissue, which is crucial for furthering our understanding of biological processes and diseases. However, cell typing typically depends on the segmentation of cell nuclei, which is often done based on images of a DNA stain, such as DAPI. Limiting cell definition to a nuclear stain makes it fundamentally difficult to determine accurate cell borders, and thereby also difficult to assign mRNA molecules to the correct cell. As such, we have developed a computational tool that segments cells solely based on the local composition of mRNA molecules. First, a small neural network is trained to compute attractive and repulsive edges between pairs of mRNA molecules. The signed graph is then partitioned by a mutex watershed into components corresponding to different cells. We evaluated our method on two publicly available datasets and compared it against the current state-of-the-art and older baselines. We conclude that combining neural networks with combinatorial optimization is a promising approach for cell segmentation of in situ transcriptomics data.
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