| Literature DB >> 25799384 |
Paolo Maiuri1, Jean-François Rupprecht2, Stefan Wieser3, Verena Ruprecht3, Olivier Bénichou2, Nicolas Carpi1, Mathieu Coppey4, Simon De Beco4, Nir Gov5, Carl-Philipp Heisenberg3, Carolina Lage Crespo6, Franziska Lautenschlaeger1, Maël Le Berre1, Ana-Maria Lennon-Dumenil7, Matthew Raab1, Hawa-Racine Thiam1, Matthieu Piel8, Michael Sixt9, Raphaël Voituriez10.
Abstract
Cell movement has essential functions in development, immunity, and cancer. Various cell migration patterns have been reported, but no general rule has emerged so far. Here, we show on the basis of experimental data in vitro and in vivo that cell persistence, which quantifies the straightness of trajectories, is robustly coupled to cell migration speed. We suggest that this universal coupling constitutes a generic law of cell migration, which originates in the advection of polarity cues by an actin cytoskeleton undergoing flows at the cellular scale. Our analysis relies on a theoretical model that we validate by measuring the persistence of cells upon modulation of actin flow speeds and upon optogenetic manipulation of the binding of an actin regulator to actin filaments. Beyond the quantitative prediction of the coupling, the model yields a generic phase diagram of cellular trajectories, which recapitulates the full range of observed migration patterns.Entities:
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Year: 2015 PMID: 25799384 DOI: 10.1016/j.cell.2015.01.056
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582