Intrinsic Dynamics of the ClpXP Proteolytic Machine Using Elastic Network Models

[Image: see text] ClpXP complex is an ATP-dependent mitochondrial matrix protease that binds, unfolds, translocates, and subsequently degrades specific protein substrates. Its mechanisms of operation are still being debated, and several have been proposed, including the sequential translocation of t...

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Autores principales: González-Paz, Lenin, Lossada, Carla, Hurtado-León, Maria Laura, Fernández-Materán, Francelys V., Paz, José Luis, Parvizi, Shayan, Cardenas Castillo, Rafael Eduardo, Romero, Freddy, Alvarado, Ysaias J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2023
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9979342/
https://www.ncbi.nlm.nih.gov/pubmed/36873006
http://dx.doi.org/10.1021/acsomega.2c04347
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author González-Paz, Lenin
Lossada, Carla
Hurtado-León, Maria Laura
Fernández-Materán, Francelys V.
Paz, José Luis
Parvizi, Shayan
Cardenas Castillo, Rafael Eduardo
Romero, Freddy
Alvarado, Ysaias J.
author_facet González-Paz, Lenin
Lossada, Carla
Hurtado-León, Maria Laura
Fernández-Materán, Francelys V.
Paz, José Luis
Parvizi, Shayan
Cardenas Castillo, Rafael Eduardo
Romero, Freddy
Alvarado, Ysaias J.
author_sort González-Paz, Lenin
collection PubMed
description [Image: see text] ClpXP complex is an ATP-dependent mitochondrial matrix protease that binds, unfolds, translocates, and subsequently degrades specific protein substrates. Its mechanisms of operation are still being debated, and several have been proposed, including the sequential translocation of two residues (SC/2R), six residues (SC/6R), and even long-pass probabilistic models. Therefore, it has been suggested to employ biophysical–computational approaches that can determine the kinetics and thermodynamics of the translocation. In this sense, and based on the apparent inconsistency between structural and functional studies, we propose to apply biophysical approaches based on elastic network models (ENM) to study the intrinsic dynamics of the theoretically most probable hydrolysis mechanism. The proposed models ENM suggest that the ClpP region is decisive for the stabilization of the ClpXP complex, contributing to the flexibility of the residues adjacent to the pore, favoring the increase in pore size and, therefore, with the energy of interaction of its residues with a larger portion of the substrate. It is predicted that the complex may undergo a stable configurational change once assembled and that the deformability of the system once assembled is oriented, to increase the rigidity of the domains of each region (ClpP and ClpX) and to gain flexibility of the pore. Our predictions could suggest under the conditions of this study the mechanism of the interaction of the system, of which the substrate passes through the unfolding of the pore in parallel with a folding of the bottleneck. The variations in the distance calculated by molecular dynamics could allow the passage of a substrate with a size equivalent to ∼3 residues. The theoretical behavior of the pore and the stability and energy of binding to the substrate based on ENM models suggest that in this system, there are thermodynamic, structural, and configurational conditions that allow a possible translocation mechanism that is not strictly sequential.
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spelling pubmed-99793422023-03-03 Intrinsic Dynamics of the ClpXP Proteolytic Machine Using Elastic Network Models González-Paz, Lenin Lossada, Carla Hurtado-León, Maria Laura Fernández-Materán, Francelys V. Paz, José Luis Parvizi, Shayan Cardenas Castillo, Rafael Eduardo Romero, Freddy Alvarado, Ysaias J. ACS Omega [Image: see text] ClpXP complex is an ATP-dependent mitochondrial matrix protease that binds, unfolds, translocates, and subsequently degrades specific protein substrates. Its mechanisms of operation are still being debated, and several have been proposed, including the sequential translocation of two residues (SC/2R), six residues (SC/6R), and even long-pass probabilistic models. Therefore, it has been suggested to employ biophysical–computational approaches that can determine the kinetics and thermodynamics of the translocation. In this sense, and based on the apparent inconsistency between structural and functional studies, we propose to apply biophysical approaches based on elastic network models (ENM) to study the intrinsic dynamics of the theoretically most probable hydrolysis mechanism. The proposed models ENM suggest that the ClpP region is decisive for the stabilization of the ClpXP complex, contributing to the flexibility of the residues adjacent to the pore, favoring the increase in pore size and, therefore, with the energy of interaction of its residues with a larger portion of the substrate. It is predicted that the complex may undergo a stable configurational change once assembled and that the deformability of the system once assembled is oriented, to increase the rigidity of the domains of each region (ClpP and ClpX) and to gain flexibility of the pore. Our predictions could suggest under the conditions of this study the mechanism of the interaction of the system, of which the substrate passes through the unfolding of the pore in parallel with a folding of the bottleneck. The variations in the distance calculated by molecular dynamics could allow the passage of a substrate with a size equivalent to ∼3 residues. The theoretical behavior of the pore and the stability and energy of binding to the substrate based on ENM models suggest that in this system, there are thermodynamic, structural, and configurational conditions that allow a possible translocation mechanism that is not strictly sequential. American Chemical Society 2023-02-14 /pmc/articles/PMC9979342/ /pubmed/36873006 http://dx.doi.org/10.1021/acsomega.2c04347 Text en © 2023 The Authors. Published by American Chemical Society https://creativecommons.org/licenses/by-nc-nd/4.0/Permits non-commercial access and re-use, provided that author attribution and integrity are maintained; but does not permit creation of adaptations or other derivative works (https://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle González-Paz, Lenin
Lossada, Carla
Hurtado-León, Maria Laura
Fernández-Materán, Francelys V.
Paz, José Luis
Parvizi, Shayan
Cardenas Castillo, Rafael Eduardo
Romero, Freddy
Alvarado, Ysaias J.
Intrinsic Dynamics of the ClpXP Proteolytic Machine Using Elastic Network Models
title Intrinsic Dynamics of the ClpXP Proteolytic Machine Using Elastic Network Models
title_full Intrinsic Dynamics of the ClpXP Proteolytic Machine Using Elastic Network Models
title_fullStr Intrinsic Dynamics of the ClpXP Proteolytic Machine Using Elastic Network Models
title_full_unstemmed Intrinsic Dynamics of the ClpXP Proteolytic Machine Using Elastic Network Models
title_short Intrinsic Dynamics of the ClpXP Proteolytic Machine Using Elastic Network Models
title_sort intrinsic dynamics of the clpxp proteolytic machine using elastic network models
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9979342/
https://www.ncbi.nlm.nih.gov/pubmed/36873006
http://dx.doi.org/10.1021/acsomega.2c04347
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