Controlling T cells spreading, mechanics and activation by micropatterning
Abstract We designed a strategy, based on a careful examination of the activation capabilities of proteins and antibodies used as substrates for adhering T cells, coupled to protein microstamping to control at the same time the position, shape, spreading, mechanics and activation state of T cells. O...
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2021-03-01
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Series: | Scientific Reports |
Online Access: | https://doi.org/10.1038/s41598-021-86133-1 |
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doaj-ff1e48ef684a4b078137f5fce273a6b22021-03-28T11:31:34ZengNature Publishing GroupScientific Reports2045-23222021-03-0111111510.1038/s41598-021-86133-1Controlling T cells spreading, mechanics and activation by micropatterningAnaïs Sadoun0Martine Biarnes-Pelicot1Laura Ghesquiere-Dierickx2Ambroise Wu3Olivier Théodoly4Laurent Limozin5Yannick Hamon6Pierre-Henri Puech7Adhesion and Inflammation Lab (LAI), Aix Marseille University, LAI UM 61Adhesion and Inflammation Lab (LAI), Aix Marseille University, LAI UM 61Adhesion and Inflammation Lab (LAI), Aix Marseille University, LAI UM 61Centre d’Immunologie de Marseille Luminy (CIML), Aix-Marseille University, CNRS, Inserm, CIML MarseilleAdhesion and Inflammation Lab (LAI), Aix Marseille University, LAI UM 61Adhesion and Inflammation Lab (LAI), Aix Marseille University, LAI UM 61Centre d’Immunologie de Marseille Luminy (CIML), Aix-Marseille University, CNRS, Inserm, CIML MarseilleAdhesion and Inflammation Lab (LAI), Aix Marseille University, LAI UM 61Abstract We designed a strategy, based on a careful examination of the activation capabilities of proteins and antibodies used as substrates for adhering T cells, coupled to protein microstamping to control at the same time the position, shape, spreading, mechanics and activation state of T cells. Once adhered on patterns, we examined the capacities of T cells to be activated with soluble anti CD3, in comparison to T cells adhered to a continuously decorated substrate with the same density of ligands. We show that, in our hand, adhering onto an anti CD45 antibody decorated surface was not affecting T cell calcium fluxes, even adhered on variable size micro-patterns. Aside, we analyzed the T cell mechanics, when spread on pattern or not, using Atomic Force Microscopy indentation. By expressing MEGF10 as a non immune adhesion receptor in T cells we measured the very same spreading area on PLL substrates and Young modulus than non modified cells, immobilized on anti CD45 antibodies, while retaining similar activation capabilities using soluble anti CD3 antibodies or through model APC contacts. We propose that our system is a way to test activation or anergy of T cells with defined adhesion and mechanical characteristics, and may allow to dissect fine details of these mechanisms since it allows to observe homogenized populations in standardized T cell activation assays.https://doi.org/10.1038/s41598-021-86133-1 |
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DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Anaïs Sadoun Martine Biarnes-Pelicot Laura Ghesquiere-Dierickx Ambroise Wu Olivier Théodoly Laurent Limozin Yannick Hamon Pierre-Henri Puech |
spellingShingle |
Anaïs Sadoun Martine Biarnes-Pelicot Laura Ghesquiere-Dierickx Ambroise Wu Olivier Théodoly Laurent Limozin Yannick Hamon Pierre-Henri Puech Controlling T cells spreading, mechanics and activation by micropatterning Scientific Reports |
author_facet |
Anaïs Sadoun Martine Biarnes-Pelicot Laura Ghesquiere-Dierickx Ambroise Wu Olivier Théodoly Laurent Limozin Yannick Hamon Pierre-Henri Puech |
author_sort |
Anaïs Sadoun |
title |
Controlling T cells spreading, mechanics and activation by micropatterning |
title_short |
Controlling T cells spreading, mechanics and activation by micropatterning |
title_full |
Controlling T cells spreading, mechanics and activation by micropatterning |
title_fullStr |
Controlling T cells spreading, mechanics and activation by micropatterning |
title_full_unstemmed |
Controlling T cells spreading, mechanics and activation by micropatterning |
title_sort |
controlling t cells spreading, mechanics and activation by micropatterning |
publisher |
Nature Publishing Group |
series |
Scientific Reports |
issn |
2045-2322 |
publishDate |
2021-03-01 |
description |
Abstract We designed a strategy, based on a careful examination of the activation capabilities of proteins and antibodies used as substrates for adhering T cells, coupled to protein microstamping to control at the same time the position, shape, spreading, mechanics and activation state of T cells. Once adhered on patterns, we examined the capacities of T cells to be activated with soluble anti CD3, in comparison to T cells adhered to a continuously decorated substrate with the same density of ligands. We show that, in our hand, adhering onto an anti CD45 antibody decorated surface was not affecting T cell calcium fluxes, even adhered on variable size micro-patterns. Aside, we analyzed the T cell mechanics, when spread on pattern or not, using Atomic Force Microscopy indentation. By expressing MEGF10 as a non immune adhesion receptor in T cells we measured the very same spreading area on PLL substrates and Young modulus than non modified cells, immobilized on anti CD45 antibodies, while retaining similar activation capabilities using soluble anti CD3 antibodies or through model APC contacts. We propose that our system is a way to test activation or anergy of T cells with defined adhesion and mechanical characteristics, and may allow to dissect fine details of these mechanisms since it allows to observe homogenized populations in standardized T cell activation assays. |
url |
https://doi.org/10.1038/s41598-021-86133-1 |
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