PLoS ONE (Jan 2014)

Exploiting cell-to-cell variability to detect cellular perturbations.

  • Gautam Dey,
  • Gagan D Gupta,
  • Balaji Ramalingam,
  • Mugdha Sathe,
  • Satyajit Mayor,
  • Mukund Thattai

DOI
https://doi.org/10.1371/journal.pone.0090540
Journal volume & issue
Vol. 9, no. 3
p. e90540

Abstract

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Any single-cell-resolved measurement generates a population distribution of phenotypes, characterized by a mean, a variance, and a shape. Here we show that changes in the shape of a phenotypic distribution can signal perturbations to cellular processes, providing a way to screen for underlying molecular machinery. We analyzed images of a Drosophila S2R+ cell line perturbed by RNA interference, and tracked 27 single-cell features which report on endocytic activity, and cell and nuclear morphology. In replicate measurements feature distributions had erratic means and variances, but reproducible shapes; RNAi down-regulation reliably induced shape deviations in at least one feature for 1072 out of 7131 genes surveyed, as revealed by a Kolmogorov-Smirnov-like statistic. We were able to use these shape deviations to identify a spectrum of genes that influenced cell morphology, nuclear morphology, and multiple pathways of endocytosis. By preserving single-cell data, our method was even able to detect effects invisible to a population-averaged analysis. These results demonstrate that cell-to-cell variability contains accessible and useful biological information, which can be exploited in existing cell-based assays.