4.7 Article

Morphological features of single cells enable accurate automated classification of cancer from non-cancer cell lines

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SCIENTIFIC REPORTS
卷 11, 期 1, 页码 -

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NATURE PORTFOLIO
DOI: 10.1038/s41598-021-03813-8

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  1. National Cancer Institute of the National Institutes of Health [U54CA199091]
  2. Robert R. McCormick School of Engineering and Applied Science at Northwestern University

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This research successfully introduced an algorithm that could distinguish cancer from non-cancer cells in high-resolution single cell images by exploiting structural differences in the cytoskeleton. Overcoming the barrier of insufficient data in machine learning methodologies, the study identified the most discriminatory features to predict cell type accurately with as few as 100 cells per line. Furthermore, normalizing cell shape improved discrimination of cell lines with difficult-to-distinguish phenotypes, demonstrating the generalizability of the algorithm across various tissue origins.
Accurate cancer detection and diagnosis is of utmost importance for reliable drug-response prediction. Successful cancer characterization relies on both genetic analysis and histological scans from tumor biopsies. It is known that the cytoskeleton is significantly altered in cancer, as cellular structure dynamically remodels to promote proliferation, migration, and metastasis. We exploited these structural differences with supervised feature extraction methods to introduce an algorithm that could distinguish cancer from non-cancer cells presented in high-resolution, single cell images. In this paper, we successfully identified the features with the most discriminatory power to successfully predict cell type with as few as 100 cells per cell line. This trait overcomes a key barrier of machine learning methodologies: insufficient data. Furthermore, normalizing cell shape via microcontact printing on self-assembled monolayers enabled better discrimination of cell lines with difficult-to-distinguish phenotypes. Classification accuracy remained robust as we tested dissimilar cell lines across various tissue origins, which supports the generalizability of our algorithm.

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