Branching activity switches actin network between connected and fragmented states in a myosin-dependent manner

dc.contributor.advisorGiniger, Edward
dc.contributor.advisorPapoian, Garegin
dc.contributor.authorChandrasekaran, Aravind
dc.date.accessioned2021-09-03T12:44:17Z
dc.date.available2021-09-03T12:44:17Z
dc.date.issued2021
dc.descriptionThis repository contains the inputfiles for MEDYAN and the processed MATLAB files for three trials corresponding to M:A=0.1, 0.05 and 0.01 values. MEDYAN trajectories were converted into MATLAB files using the following code: https://github.com/achansek/readMEDYANtraj.git. Processed MATLAB files were analyzed to generate graphs for the manuscript. The codes for analyses can be found here: https://github.com/achansek/MEDYANArp23_2021.giten_US
dc.description.abstractActin networks rely on nucleation mechanisms to generate new filaments because de-novo nucleation is kinetically disfavored. Branching nucleation of actin filaments by Arp2/3, in particular, is critical for actin self-organization. In this study, we use the simulation platform for active matter, MEDYAN, to generate 2000s long stochastic trajectories of actin networks, under varying Arp2/3 concentrations, in reaction volumes of biologically meaningful size (> 20m3). We find that mechanosensitive dynamics of Arp2/3 increases the abundance of short filaments and increases network treadmilling rate. By analyzing the density-fields of F-actin, we find that at low Arp2/3 concentration, F-actin is organized into a single, connected and contractile domain, while at elevated Arp2/3 levels (10nM and above), such contractile actin domains fragment into smaller domains spanning a wide range of volumes. These fragmented domains are extremely dynamic, continuously merging and splitting, owing to the high treadmilling rate of the underlying actin network. Treating the domain dynamics as a drift-diffusion process, we find that the fragmented state is stochastically favored, and the network state slowly drifts towards the fragmented state with considerable diffusion (variability) in the number of domains. We suggest that tuning the Arp2/3 concentration enables cells to transition from a globally coherent cytoskeleton, whose response involves the entire cytoplasmic network, to a fragmented cytoskeleton where domains can respond independently to local varying signals.en_US
dc.description.sponsorshipNSF CHE-1800418, CHE-2102684 and by the Intramural Research Program of NINDS, NIH, grant Z01-NS003013 to EGen_US
dc.identifierhttps://doi.org/10.13016/kqog-283q
dc.identifier.urihttp://hdl.handle.net/1903/27673
dc.language.isoenen_US
dc.relation.isAvailableAtDigital Repository at the University of Marylanden_us
dc.relation.isAvailableAtChemistry & Biochemistryen_us
dc.relation.isAvailableAtCollege of Computer, Mathematical & Natural Sciencesen_us
dc.relation.isAvailableAtUniversity of Maryland (College Park, MD)en_us
dc.subjectactinen_US
dc.subjectactomyosinen_US
dc.subjectArp2/3en_US
dc.subjectdendriticen_US
dc.subjectcytoskeletonen_US
dc.titleBranching activity switches actin network between connected and fragmented states in a myosin-dependent manneren_US
dc.typeDataseten_US

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Input files to be used in MEDYAN to generate trajectories.
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