A cytoskeletal clutch mediates cellular force transmission in a soft, three-dimensional extracellular matrix

The ability of cells to impart forces and deformations on their surroundings underlies cell migration and extracellular matrix (ECM) remodeling and is thus an essential aspect of complex, metazoan life. Previous work has resulted in a refined understanding, commonly termed the molecular clutch model...

Descripción completa

Detalles Bibliográficos
Autores principales: Owen, Leanna M., Adhikari, Arjun S., Patel, Mohak, Grimmer, Peter, Leijnse, Natascha, Kim, Min Cheol, Notbohm, Jacob, Franck, Christian, Dunn, Alexander R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The American Society for Cell Biology 2017
Materias:
Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5541846/
https://www.ncbi.nlm.nih.gov/pubmed/28592635
http://dx.doi.org/10.1091/mbc.E17-02-0102
_version_ 1783254890872569856
author Owen, Leanna M.
Adhikari, Arjun S.
Patel, Mohak
Grimmer, Peter
Leijnse, Natascha
Kim, Min Cheol
Notbohm, Jacob
Franck, Christian
Dunn, Alexander R.
author_facet Owen, Leanna M.
Adhikari, Arjun S.
Patel, Mohak
Grimmer, Peter
Leijnse, Natascha
Kim, Min Cheol
Notbohm, Jacob
Franck, Christian
Dunn, Alexander R.
author_sort Owen, Leanna M.
collection PubMed
description The ability of cells to impart forces and deformations on their surroundings underlies cell migration and extracellular matrix (ECM) remodeling and is thus an essential aspect of complex, metazoan life. Previous work has resulted in a refined understanding, commonly termed the molecular clutch model, of how cells adhering to flat surfaces such as a microscope coverslip transmit cytoskeletally generated forces to their surroundings. Comparatively less is known about how cells adhere to and exert forces in soft, three-dimensional (3D), and structurally heterogeneous ECM environments such as occur in vivo. We used time-lapse 3D imaging and quantitative image analysis to determine how the actin cytoskeleton is mechanically coupled to the surrounding matrix for primary dermal fibroblasts embedded in a 3D fibrin matrix. Under these circumstances, the cytoskeletal architecture is dominated by contractile actin bundles attached at their ends to large, stable, integrin-based adhesions. Time-lapse imaging reveals that α-actinin-1 puncta within actomyosin bundles move more quickly than the paxillin-rich adhesion plaques, which in turn move more quickly than the local matrix, an observation reminiscent of the molecular clutch model. However, closer examination did not reveal a continuous rearward flow of the actin cytoskeleton over slower moving adhesions. Instead, we found that a subset of stress fibers continuously elongated at their attachment points to integrin adhesions, providing stable, yet structurally dynamic coupling to the ECM. Analytical modeling and numerical simulation provide a plausible physical explanation for this result and support a picture in which cells respond to the effective stiffness of local matrix attachment points. The resulting dynamic equilibrium can explain how cells maintain stable, contractile connections to discrete points within ECM during cell migration, and provides a plausible means by which fibroblasts contract provisional matrices during wound healing.
format Online
Article
Text
id pubmed-5541846
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher The American Society for Cell Biology
record_format MEDLINE/PubMed
spelling pubmed-55418462017-09-22 A cytoskeletal clutch mediates cellular force transmission in a soft, three-dimensional extracellular matrix Owen, Leanna M. Adhikari, Arjun S. Patel, Mohak Grimmer, Peter Leijnse, Natascha Kim, Min Cheol Notbohm, Jacob Franck, Christian Dunn, Alexander R. Mol Biol Cell Articles The ability of cells to impart forces and deformations on their surroundings underlies cell migration and extracellular matrix (ECM) remodeling and is thus an essential aspect of complex, metazoan life. Previous work has resulted in a refined understanding, commonly termed the molecular clutch model, of how cells adhering to flat surfaces such as a microscope coverslip transmit cytoskeletally generated forces to their surroundings. Comparatively less is known about how cells adhere to and exert forces in soft, three-dimensional (3D), and structurally heterogeneous ECM environments such as occur in vivo. We used time-lapse 3D imaging and quantitative image analysis to determine how the actin cytoskeleton is mechanically coupled to the surrounding matrix for primary dermal fibroblasts embedded in a 3D fibrin matrix. Under these circumstances, the cytoskeletal architecture is dominated by contractile actin bundles attached at their ends to large, stable, integrin-based adhesions. Time-lapse imaging reveals that α-actinin-1 puncta within actomyosin bundles move more quickly than the paxillin-rich adhesion plaques, which in turn move more quickly than the local matrix, an observation reminiscent of the molecular clutch model. However, closer examination did not reveal a continuous rearward flow of the actin cytoskeleton over slower moving adhesions. Instead, we found that a subset of stress fibers continuously elongated at their attachment points to integrin adhesions, providing stable, yet structurally dynamic coupling to the ECM. Analytical modeling and numerical simulation provide a plausible physical explanation for this result and support a picture in which cells respond to the effective stiffness of local matrix attachment points. The resulting dynamic equilibrium can explain how cells maintain stable, contractile connections to discrete points within ECM during cell migration, and provides a plausible means by which fibroblasts contract provisional matrices during wound healing. The American Society for Cell Biology 2017-07-07 /pmc/articles/PMC5541846/ /pubmed/28592635 http://dx.doi.org/10.1091/mbc.E17-02-0102 Text en © 2017 Owen et al. This article is distributed by The American Society for Cell Biology under license from the author(s). Two months after publication it is available to the public under an Attribution–Noncommercial–Share Alike 3.0 Unported Creative Commons License (http://creativecommons.org/licenses/by-nc-sa/3.0). “ASCB®,” “The American Society for Cell Biology®,” and “Molecular Biology of the Cell®” are registered trademarks of The American Society for Cell Biology.
spellingShingle Articles
Owen, Leanna M.
Adhikari, Arjun S.
Patel, Mohak
Grimmer, Peter
Leijnse, Natascha
Kim, Min Cheol
Notbohm, Jacob
Franck, Christian
Dunn, Alexander R.
A cytoskeletal clutch mediates cellular force transmission in a soft, three-dimensional extracellular matrix
title A cytoskeletal clutch mediates cellular force transmission in a soft, three-dimensional extracellular matrix
title_full A cytoskeletal clutch mediates cellular force transmission in a soft, three-dimensional extracellular matrix
title_fullStr A cytoskeletal clutch mediates cellular force transmission in a soft, three-dimensional extracellular matrix
title_full_unstemmed A cytoskeletal clutch mediates cellular force transmission in a soft, three-dimensional extracellular matrix
title_short A cytoskeletal clutch mediates cellular force transmission in a soft, three-dimensional extracellular matrix
title_sort cytoskeletal clutch mediates cellular force transmission in a soft, three-dimensional extracellular matrix
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5541846/
https://www.ncbi.nlm.nih.gov/pubmed/28592635
http://dx.doi.org/10.1091/mbc.E17-02-0102
work_keys_str_mv AT owenleannam acytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT adhikariarjuns acytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT patelmohak acytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT grimmerpeter acytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT leijnsenatascha acytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT kimmincheol acytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT notbohmjacob acytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT franckchristian acytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT dunnalexanderr acytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT owenleannam cytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT adhikariarjuns cytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT patelmohak cytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT grimmerpeter cytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT leijnsenatascha cytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT kimmincheol cytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT notbohmjacob cytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT franckchristian cytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix
AT dunnalexanderr cytoskeletalclutchmediatescellularforcetransmissioninasoftthreedimensionalextracellularmatrix

Ejemplares similares