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Substrate stiffness reduces particle uptake by epithelial cells and macrophages in a size-dependent manner through mechanoregulation

Cells continuously exert forces on their environment and respond to changes in mechanical forces by altering their behaviour. Many pathologies such as cancer and fibrosis are hallmarked by dysregulation in the extracellular matrix, driving aberrant behaviour through mechanotransduction pathways. We...

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Autores principales: Lee, Aaron, Sousa de Almeida, Mauro, Milinkovic, Daela, Septiadi, Dedy, Taladriz-Blanco, Patricia, Loussert-Fonta, Céline, Balog, Sandor, Bazzoni, Amelie, Rothen-Rutishauser, Barbara, Petri-Fink, Alke
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society of Chemistry 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9585528/
https://www.ncbi.nlm.nih.gov/pubmed/36205559
http://dx.doi.org/10.1039/d2nr03792k
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author Lee, Aaron
Sousa de Almeida, Mauro
Milinkovic, Daela
Septiadi, Dedy
Taladriz-Blanco, Patricia
Loussert-Fonta, Céline
Balog, Sandor
Bazzoni, Amelie
Rothen-Rutishauser, Barbara
Petri-Fink, Alke
author_facet Lee, Aaron
Sousa de Almeida, Mauro
Milinkovic, Daela
Septiadi, Dedy
Taladriz-Blanco, Patricia
Loussert-Fonta, Céline
Balog, Sandor
Bazzoni, Amelie
Rothen-Rutishauser, Barbara
Petri-Fink, Alke
author_sort Lee, Aaron
collection PubMed
description Cells continuously exert forces on their environment and respond to changes in mechanical forces by altering their behaviour. Many pathologies such as cancer and fibrosis are hallmarked by dysregulation in the extracellular matrix, driving aberrant behaviour through mechanotransduction pathways. We demonstrate that substrate stiffness can be used to regulate cellular endocytosis of particles in a size-dependent fashion. Culture of A549 epithelial cells and J774A.1 macrophages on polystyrene/glass (stiff) and polydimethylsiloxane (soft) substrates indicated that particle uptake is increased up to six times for A549 and two times for macrophages when cells are grown in softer environments. Furthermore, we altered surface characteristics through the attachment of submicron-sized particles as a method to locally engineer substrate stiffness and topography to investigate the biomechanical changes which occurred within adherent epithelial cells, i.e. characterization of A549 cell spreading and focal adhesion maturation. Consequently, decreasing substrate rigidity and particle-based topography led to a reduction of focal adhesion size. Moreover, expression levels of Yes-associated protein were found to correlate with the degree of particle endocytosis. A thorough appreciation of the mechanical cues may lead to improved solutions to optimize nanomedicine approaches for treatment of cancer and other diseases with abnormal mechanosignalling.
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spelling pubmed-95855282022-11-02 Substrate stiffness reduces particle uptake by epithelial cells and macrophages in a size-dependent manner through mechanoregulation Lee, Aaron Sousa de Almeida, Mauro Milinkovic, Daela Septiadi, Dedy Taladriz-Blanco, Patricia Loussert-Fonta, Céline Balog, Sandor Bazzoni, Amelie Rothen-Rutishauser, Barbara Petri-Fink, Alke Nanoscale Chemistry Cells continuously exert forces on their environment and respond to changes in mechanical forces by altering their behaviour. Many pathologies such as cancer and fibrosis are hallmarked by dysregulation in the extracellular matrix, driving aberrant behaviour through mechanotransduction pathways. We demonstrate that substrate stiffness can be used to regulate cellular endocytosis of particles in a size-dependent fashion. Culture of A549 epithelial cells and J774A.1 macrophages on polystyrene/glass (stiff) and polydimethylsiloxane (soft) substrates indicated that particle uptake is increased up to six times for A549 and two times for macrophages when cells are grown in softer environments. Furthermore, we altered surface characteristics through the attachment of submicron-sized particles as a method to locally engineer substrate stiffness and topography to investigate the biomechanical changes which occurred within adherent epithelial cells, i.e. characterization of A549 cell spreading and focal adhesion maturation. Consequently, decreasing substrate rigidity and particle-based topography led to a reduction of focal adhesion size. Moreover, expression levels of Yes-associated protein were found to correlate with the degree of particle endocytosis. A thorough appreciation of the mechanical cues may lead to improved solutions to optimize nanomedicine approaches for treatment of cancer and other diseases with abnormal mechanosignalling. The Royal Society of Chemistry 2022-10-03 /pmc/articles/PMC9585528/ /pubmed/36205559 http://dx.doi.org/10.1039/d2nr03792k Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by-nc/3.0/
spellingShingle Chemistry
Lee, Aaron
Sousa de Almeida, Mauro
Milinkovic, Daela
Septiadi, Dedy
Taladriz-Blanco, Patricia
Loussert-Fonta, Céline
Balog, Sandor
Bazzoni, Amelie
Rothen-Rutishauser, Barbara
Petri-Fink, Alke
Substrate stiffness reduces particle uptake by epithelial cells and macrophages in a size-dependent manner through mechanoregulation
title Substrate stiffness reduces particle uptake by epithelial cells and macrophages in a size-dependent manner through mechanoregulation
title_full Substrate stiffness reduces particle uptake by epithelial cells and macrophages in a size-dependent manner through mechanoregulation
title_fullStr Substrate stiffness reduces particle uptake by epithelial cells and macrophages in a size-dependent manner through mechanoregulation
title_full_unstemmed Substrate stiffness reduces particle uptake by epithelial cells and macrophages in a size-dependent manner through mechanoregulation
title_short Substrate stiffness reduces particle uptake by epithelial cells and macrophages in a size-dependent manner through mechanoregulation
title_sort substrate stiffness reduces particle uptake by epithelial cells and macrophages in a size-dependent manner through mechanoregulation
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9585528/
https://www.ncbi.nlm.nih.gov/pubmed/36205559
http://dx.doi.org/10.1039/d2nr03792k
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