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MAP4K4 regulates forces at cell–cell and cell–matrix adhesions to promote collective cell migration

Collective cell migration is not only important for development and tissue homeostasis but can also promote cancer metastasis. To migrate collectively, cells need to coordinate cellular extensions and retractions, adhesion sites dynamics, and forces generation and transmission. Nevertheless, the reg...

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Autores principales: Alberici Delsin, Lara Elis, Plutoni, Cédric, Clouvel, Anna, Keil, Sarah, Marpeaux, Léa, Elouassouli, Lina, Khavari, Adele, Ehrlicher, Allen J, Emery, Gregory
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Life Science Alliance LLC 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10300198/
https://www.ncbi.nlm.nih.gov/pubmed/37369604
http://dx.doi.org/10.26508/lsa.202302196
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author Alberici Delsin, Lara Elis
Plutoni, Cédric
Clouvel, Anna
Keil, Sarah
Marpeaux, Léa
Elouassouli, Lina
Khavari, Adele
Ehrlicher, Allen J
Emery, Gregory
author_facet Alberici Delsin, Lara Elis
Plutoni, Cédric
Clouvel, Anna
Keil, Sarah
Marpeaux, Léa
Elouassouli, Lina
Khavari, Adele
Ehrlicher, Allen J
Emery, Gregory
author_sort Alberici Delsin, Lara Elis
collection PubMed
description Collective cell migration is not only important for development and tissue homeostasis but can also promote cancer metastasis. To migrate collectively, cells need to coordinate cellular extensions and retractions, adhesion sites dynamics, and forces generation and transmission. Nevertheless, the regulatory mechanisms coordinating these processes remain elusive. Using A431 carcinoma cells, we identify the kinase MAP4K4 as a central regulator of collective migration. We show that MAP4K4 inactivation blocks the migration of clusters, whereas its overexpression decreases cluster cohesion. MAP4K4 regulates protrusion and retraction dynamics, remodels the actomyosin cytoskeleton, and controls the stability of both cell–cell and cell–substrate adhesion. MAP4K4 promotes focal adhesion disassembly through the phosphorylation of the actin and plasma membrane crosslinker moesin but disassembles adherens junctions through a moesin-independent mechanism. By analyzing traction and intercellular forces, we found that MAP4K4 loss of function leads to a tensional disequilibrium throughout the cell cluster, increasing the traction forces and the tension loading at the cell–cell adhesions. Together, our results indicate that MAP4K4 activity is a key regulator of biomechanical forces at adhesion sites, promoting collective migration.
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spelling pubmed-103001982023-06-29 MAP4K4 regulates forces at cell–cell and cell–matrix adhesions to promote collective cell migration Alberici Delsin, Lara Elis Plutoni, Cédric Clouvel, Anna Keil, Sarah Marpeaux, Léa Elouassouli, Lina Khavari, Adele Ehrlicher, Allen J Emery, Gregory Life Sci Alliance Research Articles Collective cell migration is not only important for development and tissue homeostasis but can also promote cancer metastasis. To migrate collectively, cells need to coordinate cellular extensions and retractions, adhesion sites dynamics, and forces generation and transmission. Nevertheless, the regulatory mechanisms coordinating these processes remain elusive. Using A431 carcinoma cells, we identify the kinase MAP4K4 as a central regulator of collective migration. We show that MAP4K4 inactivation blocks the migration of clusters, whereas its overexpression decreases cluster cohesion. MAP4K4 regulates protrusion and retraction dynamics, remodels the actomyosin cytoskeleton, and controls the stability of both cell–cell and cell–substrate adhesion. MAP4K4 promotes focal adhesion disassembly through the phosphorylation of the actin and plasma membrane crosslinker moesin but disassembles adherens junctions through a moesin-independent mechanism. By analyzing traction and intercellular forces, we found that MAP4K4 loss of function leads to a tensional disequilibrium throughout the cell cluster, increasing the traction forces and the tension loading at the cell–cell adhesions. Together, our results indicate that MAP4K4 activity is a key regulator of biomechanical forces at adhesion sites, promoting collective migration. Life Science Alliance LLC 2023-06-27 /pmc/articles/PMC10300198/ /pubmed/37369604 http://dx.doi.org/10.26508/lsa.202302196 Text en © 2023 Alberici Delsin et al. https://creativecommons.org/licenses/by/4.0/This article is available under a Creative Commons License (Attribution 4.0 International, as described at https://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Articles
Alberici Delsin, Lara Elis
Plutoni, Cédric
Clouvel, Anna
Keil, Sarah
Marpeaux, Léa
Elouassouli, Lina
Khavari, Adele
Ehrlicher, Allen J
Emery, Gregory
MAP4K4 regulates forces at cell–cell and cell–matrix adhesions to promote collective cell migration
title MAP4K4 regulates forces at cell–cell and cell–matrix adhesions to promote collective cell migration
title_full MAP4K4 regulates forces at cell–cell and cell–matrix adhesions to promote collective cell migration
title_fullStr MAP4K4 regulates forces at cell–cell and cell–matrix adhesions to promote collective cell migration
title_full_unstemmed MAP4K4 regulates forces at cell–cell and cell–matrix adhesions to promote collective cell migration
title_short MAP4K4 regulates forces at cell–cell and cell–matrix adhesions to promote collective cell migration
title_sort map4k4 regulates forces at cell–cell and cell–matrix adhesions to promote collective cell migration
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10300198/
https://www.ncbi.nlm.nih.gov/pubmed/37369604
http://dx.doi.org/10.26508/lsa.202302196
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