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Single-cell biophysical study reveals deformability and internal ordering relationship in T cells.

Blanca González-BermúdezHikaru KobayashiÁlvaro NavarreteCésar NybladMónica González-SánchezMónica de la FuenteGonzalo FuentesGustavo V GuineaClaudio GarcíaGustavo R Plaza
Published in: Soft matter (2021)
Deformability and internal ordering are key features related to cell function, particularly critical for cells that routinely undergo large deformations, like T cells during extravasation and migration. In the measurement of cell deformability, a considerable variability is typically obtained, masking the identification of possible interrelationships between deformability, internal ordering and cell function. We report the development of a single-cell methodology that combines measurements of living-cell deformability, using micropipette aspiration, and three-dimensional confocal analysis of the nucleus and cytoskeleton. We show that this single-cell approach can serve as a powerful tool to identify appropriate parameters that characterize deformability within a population of cells, not readably discernable in population-averaged data. By applying this single-cell methodology to mouse CD4+ T cells, our results demonstrate that the relative size of the nucleus, better than other geometrical or cytoskeletal features, effectively determines the overall deformability of the cells within the population.
Keyphrases
  • single cell
  • rna seq
  • induced apoptosis
  • cell cycle arrest
  • high throughput
  • endoplasmic reticulum stress
  • stem cells
  • cell death
  • oxidative stress
  • cell therapy
  • machine learning
  • electronic health record