Author:
Taïeb Hubert M.,Garske Daniela S.,Contzen Jörg,Gossen Manfred,Bertinetti Luca,Robinson Tom,Cipitria Amaia
Abstract
AbstractBiophysical cues such as osmotic pressure modulate proliferation and growth arrest of bacteria, yeast cells and seeds. In tissues, osmotic regulation takes place through blood and lymphatic capillaries and, at a single cell level, water and osmoregulation play a critical role. However, the effect of osmotic pressure on single cell cycle dynamics remains poorly understood. Here, we investigate the effect of osmotic pressure on single cell cycle dynamics, nuclear growth, proliferation, migration and protein expression, by quantitative time-lapse imaging of single cells genetically modified with fluorescent ubiquitination-based cell cycle indicator 2 (FUCCI2). Single cell data reveals that under hyperosmotic stress, distinct cell subpopulations emerge with impaired nuclear growth, delayed or growth arrested cell cycle and reduced migration. This state is reversible for mild hyperosmotic stress, where cells return to regular cell cycle dynamics, proliferation and migration. Thus, osmotic pressure can modulate the reversible growth arrest and reactivation of human metastatic cells.
Funder
International Max Planck Research School on Multiscale Bio-Systems
Deutsche Forschungsgemeinschaft
Berlin-Brandenburger Centrum für Regenerative Therapien
MaxSynBio consortium
Max Planck Institute for Colloids and Interfaces (MPIKG)
Publisher
Springer Science and Business Media LLC
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