4.5 Article

Protein Signaling Networks from Single Cell Fluctuations and Information Theory Profiling

Journal

BIOPHYSICAL JOURNAL
Volume 100, Issue 10, Pages 2378-2386

Publisher

CELL PRESS
DOI: 10.1016/j.bpj.2011.04.025

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Funding

  1. National Cancer Institute [5U54 CA119347, 1K99 CA136759-01]
  2. Jean Perkins Foundation
  3. California Institute of Technology/University of California, Los Angeles, Joint Center for Translational Research
  4. Samsung Scholarship

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Protein signaling networks among cells play critical roles in a host of pathophysiological processes, from inflammation to tumorigenesis. We report on an approach that integrates microfluidic cell handling, in situ protein secretion profiling, and information theory to determine an extracellular protein-signaling network and the role of perturbations. We assayed 12 proteins secreted from human macrophages that were subjected to lipopolysaccharide challenge, which emulates the macrophage-based innate immune responses against Gram-negative bacteria. We characterize the fluctuations in protein secretion of single cells, and of small cell colonies (n = 2, 3, ... ), as a function of colony size. Measuring the fluctuations permits a validation of the conditions required for the application of a quantitative version of the Le Chatelier's principle, as derived using information theory. This principle provides a quantitative prediction of the role of perturbations and allows a characterization of a protein-protein interaction network.

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