Author:
Park JinSeok,Holmes William R.,Lee Sung Hoon,Kim Hong-Nam,Kim Deok-Ho,Kwak Moon Kyu,Wang Chiaochun Joanne,Edelstein-Keshet Leah,Levchenko Andre
Abstract
Cell polarization and directional cell migration can display random, persistent, and oscillatory dynamic patterns. However, it is not clear whether these polarity patterns can be explained by the same underlying regulatory mechanism. Here, we show that random, persistent, and oscillatory migration accompanied by polarization can simultaneously occur in populations of melanoma cells derived from tumors with different degrees of aggressiveness. We demonstrate that all of these patterns and the probabilities of their occurrence are quantitatively accounted for by a simple mechanism involving a spatially distributed, mechanochemical feedback coupling the dynamically changing extracellular matrix (ECM)–cell contacts to the activation of signaling downstream of the Rho-family small GTPases. This mechanism is supported by a predictive mathematical model and extensive experimental validation, and can explain previously reported results for diverse cell types. In melanoma, this mechanism also accounts for the effects of genetic and environmental perturbations, including mutations linked to invasive cell spread. The resulting mechanistic understanding of cell polarity quantitatively captures the relationship between population variability and phenotypic plasticity, with the potential to account for a wide variety of cell migration states in diverse pathological and physiological conditions.
Funder
HHS | NIH | National Cancer Institute
NSF | MPS | Division of Mathematical Sciences
Publisher
Proceedings of the National Academy of Sciences
Cited by
53 articles.
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