| Literature DB >> 33308479 |
Erik S Welf1, Christopher E Miles2, Jaewon Huh3, Etai Sapoznik3, Joseph Chi3, Meghan K Driscoll3, Tadamoto Isogai3, Jungsik Noh3, Andrew D Weems3, Theresa Pohlkamp4, Kevin Dean5, Reto Fiolka3, Alex Mogilner6, Gaudenz Danuser7.
Abstract
Despite the well-established role of actin polymerization as a driving mechanism for cell protrusion, upregulated actin polymerization alone does not initiate protrusions. Using a combination of theoretical modeling and quantitative live-cell imaging experiments, we show that local depletion of actin-membrane links is needed for protrusion initiation. Specifically, we show that the actin-membrane linker ezrin is depleted prior to protrusion onset and that perturbation of ezrin's affinity for actin modulates protrusion frequency and efficiency. We also show how actin-membrane release works in concert with actin polymerization, leading to a comprehensive model for actin-driven shape changes. Actin-membrane release plays a similar role in protrusions driven by intracellular pressure. Thus, our findings suggest that protrusion initiation might be governed by a universal regulatory mechanism, whereas the mechanism of force generation determines the shape and expansion properties of the protrusion.Entities:
Keywords: Brownian ratchet model; actin dynamics; cytoskeleton; intracellular force; lamellipodium; morphology; polymerization; protrusion; shape change
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Year: 2020 PMID: 33308479 PMCID: PMC7908823 DOI: 10.1016/j.devcel.2020.11.024
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270