Defined extracellular matrix compositions support stiffness-insensitive cell spreading and adhesion signaling

Author:

Conway James R. W.1ORCID,Isomursu Aleksi1ORCID,Follain Gautier1ORCID,Härmä Ville23ORCID,Jou-Ollé Eva1ORCID,Pasquier Nicolas1ORCID,Välimäki Eetu P. O.2ORCID,Rantala Juha K.23ORCID,Ivaska Johanna14567ORCID

Affiliation:

1. Turku Bioscience Centre, University of Turku and Åbo Akademi University, Turku FI-20520, Finland

2. Misvik Biology Oy, Turku FI-20520, Finland

3. Department of Oncology and Metabolism, University of Sheffield, Sheffield S10 2TN, United Kingdom

4. Department of Life Technologies, University of Turku, Turku FI-20520, Finland

5. InFLAMES Research Flagship, University of Turku, Turku FI-20520, Finland

6. Western Finnish Cancer Center, University of Turku, Turku FI-20520, Finland

7. Foundation for the Finnish Cancer Institute, Helsinki FI-00014, Finland

Abstract

Integrin-dependent adhesion to the extracellular matrix (ECM) mediates mechanosensing and signaling in response to altered microenvironmental conditions. In order to provide tissue- and organ-specific cues, the ECM is composed of many different proteins that temper the mechanical properties and provide the necessary structural diversity. Despite most human tissues being soft, the prevailing view from predominantly in vitro studies is that increased stiffness triggers effective cell spreading and activation of mechanosensitive signaling pathways. To address the functional coupling of ECM composition and matrix rigidity on compliant substrates, we developed a matrix spot array system to screen cell phenotypes against different ECM mixtures on defined substrate stiffnesses at high resolution. We applied this system to both cancer and normal cells and surprisingly identified ECM mixtures that support stiffness-insensitive cell spreading on soft substrates. Employing the motor-clutch model to simulate cell adhesion on biochemically distinct soft substrates, with varying numbers of available ECM–integrin–cytoskeleton (clutch) connections, we identified conditions in which spreading would be supported on soft matrices. Combining simulations and experiments, we show that cell spreading on soft is supported by increased clutch engagement on specific ECM mixtures and even augmented by the partial inhibition of actomyosin contractility. Thus, “stiff-like” spreading on soft is determined by a balance of a cell’s contractile and adhesive machinery. This provides a fundamental perspective for in vitro mechanobiology studies, identifying a mechanism through which cells spread, function, and signal effectively on soft substrates.

Funder

Academy of Finland

EC | Horizon Europe | Excellent Science | HORIZON EUROPE Marie Sklodowska-Curie Actions

SKR | Varsinais-Suomen Rahasto

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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