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Rho and F-actin self-organize within an artificial cell cortex

View ORCID ProfileJennifer Landino, View ORCID ProfileMarcin Leda, View ORCID ProfileAni Michaud, Zachary T. Swider, Mariah Prom, View ORCID ProfileChristine M. Field, View ORCID ProfileWilliam M. Bement, View ORCID ProfileAnthony G. Vecchiarelli, View ORCID ProfileAndrew B. Goryachev, View ORCID ProfileAnn L. Miller
doi: https://doi.org/10.1101/2021.04.09.438460
Jennifer Landino
1Department of Molecular, Cellular, and Developmental Biology, University of Michigan-Ann Arbor
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  • For correspondence: annlm@umich.edu landinoj@umich.edu
Marcin Leda
2Centre for Synthetic and Systems Biology, University of Edinburgh
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Ani Michaud
3Cellular and Molecular Biology Graduate Program, University of Wisconsin-Madison
4Center for Quantitative Cell Imaging, University of Wisconsin-Madison
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Zachary T. Swider
3Cellular and Molecular Biology Graduate Program, University of Wisconsin-Madison
4Center for Quantitative Cell Imaging, University of Wisconsin-Madison
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Mariah Prom
5Department of Pathology and Neuroscience Research Center, Medical College of Wisconsin
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Christine M. Field
6Department of Systems Biology, Harvard Medical School
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William M. Bement
3Cellular and Molecular Biology Graduate Program, University of Wisconsin-Madison
4Center for Quantitative Cell Imaging, University of Wisconsin-Madison
7Department of Integrative Biology, University of Wisconsin-Madison
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Anthony G. Vecchiarelli
1Department of Molecular, Cellular, and Developmental Biology, University of Michigan-Ann Arbor
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Andrew B. Goryachev
2Centre for Synthetic and Systems Biology, University of Edinburgh
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Ann L. Miller
1Department of Molecular, Cellular, and Developmental Biology, University of Michigan-Ann Arbor
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  • For correspondence: annlm@umich.edu landinoj@umich.edu
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Summary

The cell cortex, comprised of the plasma membrane and underlying cytoskeleton, undergoes dynamic reorganizations during a variety of essential biological processes including cell adhesion, cell migration, and cell division1,2. During cell division and cell locomotion, for example, waves of filamentous-actin (F-actin) assembly and disassembly develop in the cell cortex in a process termed “cortical excitability”3–7. In developing frog and starfish embryos, cortical excitability is generated through coupled positive and negative feedback, with rapid activation of Rho-mediated F-actin assembly followed in space and time by F-actin-dependent inhibition of Rho8,9. These feedback loops are proposed to serve as a mechanism for amplification of active Rho signaling at the cell equator to support furrowing during cytokinesis, while also maintaining flexibility for rapid error correction in response to movement of the mitotic spindle during chromosome segregation10. In this paper, we develop an artificial cortex based on Xenopus egg extract and supported lipid bilayers (SLBs), to investigate cortical Rho and F-actin dynamics11. This reconstituted system spontaneously develops two distinct dynamic patterns: singular excitable Rho and F-actin waves and non-traveling oscillatory Rho and F-actin patches. Both types of dynamic patterns have properties and dependencies similar to the cortical excitability previously characterized in vivo9. These findings directly support the longstanding speculation that the cell cortex is a self-organizing structure and present a novel approach for investigating mechanisms of Rho-GTPase-mediated cortical dynamics.

Highlights

  • An artificial cell cortex comprising Xenopus egg extract on a supported lipid bilayer self-organizes into complex, dynamic patterns of active Rho and F-actin

  • We identified two types of reconstituted cortical dynamics – excitable waves and coherent oscillations

  • Reconstituted waves and oscillations require Rho activity and F-actin polymerization

Competing Interest Statement

The authors have declared no competing interest.

  • Abbreviations

    (F-actin)
    Filamentous actin
    (SLB)
    supported lipid bilayer
    (rGBD)
    Rho binding domain of Rhotekin
    (UtrCH)
    Utrophin calponin homology domain
    (TIRF)
    Total Internal Reflection Fluorescence
    (PI(4,5)P2)
    Phosphatidylinositol 4,5-bisphosphate
    (GAP)
    GTPase activating protein
    (GTP)
    Guanosine triphosphate
  • Copyright 
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    Posted April 10, 2021.
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    Rho and F-actin self-organize within an artificial cell cortex
    Jennifer Landino, Marcin Leda, Ani Michaud, Zachary T. Swider, Mariah Prom, Christine M. Field, William M. Bement, Anthony G. Vecchiarelli, Andrew B. Goryachev, Ann L. Miller
    bioRxiv 2021.04.09.438460; doi: https://doi.org/10.1101/2021.04.09.438460
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    Rho and F-actin self-organize within an artificial cell cortex
    Jennifer Landino, Marcin Leda, Ani Michaud, Zachary T. Swider, Mariah Prom, Christine M. Field, William M. Bement, Anthony G. Vecchiarelli, Andrew B. Goryachev, Ann L. Miller
    bioRxiv 2021.04.09.438460; doi: https://doi.org/10.1101/2021.04.09.438460

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