Stochastic severing of actin filaments by ADF/cofilin controls the emergence of a steady dynamical regime
Actin dynamics (ie: polymerization/depolymerization) powers a large number of cellular processes. However, a great deal remains to be learned in order to explain the rapid actin filament turnover observed in vivo. Here, we developed a minimal kinetic model that describes key details of actin filamen...
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Veröffentlicht in: | Biophysical journal 2008, Vol.94, p.2082-2094 |
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creator | Roland, Jeremy Berro, Julien Michelot, Alphee Blanchoin, Laurent Martiel, Jean-Louis |
description | Actin dynamics (ie: polymerization/depolymerization) powers a large number of cellular processes. However, a great deal remains to be learned in order to explain the rapid actin filament turnover observed in vivo. Here, we developed a minimal kinetic model that describes key details of actin filament dynamics in the presence of ADF/cofilin. We limited the molecular mechanism to (1) the spontaneous growth of filaments by polymerization of actin monomers, (2) the ageing of actin subunits in filaments, (3) the cooperative binding of ADF/cofilin to actin filament subunits, and (4) filament severing by ADF/cofilin. First, from numerical simulations and mathematical analysis, we find that the average filament length, < L >, is controlled by the concentration of actin monomers (power law: 5/6) and ADF/cofilin (power law: -2/3). We also showed that the average subunit residence time inside the filament, < T >, depends on the actin monomer (power law: -1/6) and ADF/cofilin (power law: -2/3) concentrations. In addition, filament length fluctuations are ~ 20% of the average filament length. Moreover, ADF/cofilin fragmentation while modulating filament length keeps filaments in a high molar ratio of ATP- or ADP-Pi- versus ADP-bound subunits. This latter property has a protecting effect against a too high severing activity of ADF/cofilin. We propose that the activity of ADF/cofilin in vivo is under the control of an affinity gradient that builds up dynamically along growing actin filaments. Our analysis shows that ADF/cofilin regulation maintains actin filaments in a highly dynamical state compatible with the cytoskeleton dynamics observed in vivo. |
doi_str_mv | 10.1529/biophysj.107.121988 |
format | Article |
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However, a great deal remains to be learned in order to explain the rapid actin filament turnover observed in vivo. Here, we developed a minimal kinetic model that describes key details of actin filament dynamics in the presence of ADF/cofilin. We limited the molecular mechanism to (1) the spontaneous growth of filaments by polymerization of actin monomers, (2) the ageing of actin subunits in filaments, (3) the cooperative binding of ADF/cofilin to actin filament subunits, and (4) filament severing by ADF/cofilin. First, from numerical simulations and mathematical analysis, we find that the average filament length, < L >, is controlled by the concentration of actin monomers (power law: 5/6) and ADF/cofilin (power law: -2/3). We also showed that the average subunit residence time inside the filament, < T >, depends on the actin monomer (power law: -1/6) and ADF/cofilin (power law: -2/3) concentrations. In addition, filament length fluctuations are ~ 20% of the average filament length. Moreover, ADF/cofilin fragmentation while modulating filament length keeps filaments in a high molar ratio of ATP- or ADP-Pi- versus ADP-bound subunits. This latter property has a protecting effect against a too high severing activity of ADF/cofilin. We propose that the activity of ADF/cofilin in vivo is under the control of an affinity gradient that builds up dynamically along growing actin filaments. 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Moreover, ADF/cofilin fragmentation while modulating filament length keeps filaments in a high molar ratio of ATP- or ADP-Pi- versus ADP-bound subunits. This latter property has a protecting effect against a too high severing activity of ADF/cofilin. We propose that the activity of ADF/cofilin in vivo is under the control of an affinity gradient that builds up dynamically along growing actin filaments. 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However, a great deal remains to be learned in order to explain the rapid actin filament turnover observed in vivo. Here, we developed a minimal kinetic model that describes key details of actin filament dynamics in the presence of ADF/cofilin. We limited the molecular mechanism to (1) the spontaneous growth of filaments by polymerization of actin monomers, (2) the ageing of actin subunits in filaments, (3) the cooperative binding of ADF/cofilin to actin filament subunits, and (4) filament severing by ADF/cofilin. First, from numerical simulations and mathematical analysis, we find that the average filament length, < L >, is controlled by the concentration of actin monomers (power law: 5/6) and ADF/cofilin (power law: -2/3). We also showed that the average subunit residence time inside the filament, < T >, depends on the actin monomer (power law: -1/6) and ADF/cofilin (power law: -2/3) concentrations. In addition, filament length fluctuations are ~ 20% of the average filament length. Moreover, ADF/cofilin fragmentation while modulating filament length keeps filaments in a high molar ratio of ATP- or ADP-Pi- versus ADP-bound subunits. This latter property has a protecting effect against a too high severing activity of ADF/cofilin. We propose that the activity of ADF/cofilin in vivo is under the control of an affinity gradient that builds up dynamically along growing actin filaments. Our analysis shows that ADF/cofilin regulation maintains actin filaments in a highly dynamical state compatible with the cytoskeleton dynamics observed in vivo.</abstract><pub>Biophysical Society</pub><pmid>18065447</pmid><doi>10.1529/biophysj.107.121988</doi><orcidid>https://orcid.org/0000-0001-8146-9254</orcidid><orcidid>https://orcid.org/0000-0003-2023-8094</orcidid><orcidid>https://orcid.org/0000-0003-2023-8094</orcidid><orcidid>https://orcid.org/0000-0001-8146-9254</orcidid></addata></record> |
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source | Cell Press Free Archives; Elsevier ScienceDirect Journals; Elektronische Zeitschriftenbibliothek - Frei zugängliche E-Journals; PubMed Central |
subjects | Biochemistry, Molecular Biology Life Sciences |
title | Stochastic severing of actin filaments by ADF/cofilin controls the emergence of a steady dynamical regime |
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