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Theory of cytoskeletal reorganization during crosslinker-mediated mitotic spindle assembly

A. R. Lamson, C. J. Edelmaier, M. A. Glaser, View ORCID ProfileM. D. Betterton
doi: https://doi.org/10.1101/419135
A. R. Lamson
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C. J. Edelmaier
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M. A. Glaser
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M. D. Betterton
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Abstract

Cells grow, move, and respond to outside stimuli by large-scale cytoskeletal reorganization. A prototypical example of cytoskeletal remodeling is mitotic spindle assembly, during which micro-tubules nucleate, undergo dynamic instability, bundle, and organize into a bipolar spindle. Key mechanisms of this process include regulated filament polymerization, crosslinking, and motor-protein activity. Remarkably, using passive crosslinkers, fission yeast can assemble a bipolar spindle in the absence of motor proteins. We develop a torque-balance model that describes this reorganization due to dynamic microtubule bundles, spindle-pole bodies, the nuclear envelope, and passive crosslinkers to predict spindle-assembly dynamics. We compare these results to those obtained with kinetic Monte Carlo-Brownian dynamics simulations, which include crosslinker-binding kinetics and other stochastic effects. Our results show that rapid crosslinker reorganization to microtubule overlaps facilitates crosslinker-driven spindle assembly, a testable prediction for future experiments. Combining these two modeling techniques, we illustrate a general method for studying cytoskeletal network reorganization.

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Posted March 01, 2019.
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Theory of cytoskeletal reorganization during crosslinker-mediated mitotic spindle assembly
A. R. Lamson, C. J. Edelmaier, M. A. Glaser, M. D. Betterton
bioRxiv 419135; doi: https://doi.org/10.1101/419135
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Theory of cytoskeletal reorganization during crosslinker-mediated mitotic spindle assembly
A. R. Lamson, C. J. Edelmaier, M. A. Glaser, M. D. Betterton
bioRxiv 419135; doi: https://doi.org/10.1101/419135

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