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Article

Elastomeric Pillar Cages Modulate Actomyosin Contractility of Epithelial Microtissues by Substrate Stiffness and Topography

Institute of Biological Information Processing 2 (IBI-2): Mechanobiology, Forschungszentrum Jülich, 52428 Jülich, Germany
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Cells 2023, 12(9), 1256; https://doi.org/10.3390/cells12091256
Submission received: 25 March 2023 / Revised: 19 April 2023 / Accepted: 21 April 2023 / Published: 26 April 2023
(This article belongs to the Special Issue Cellular Integrity under Mechanical Stress)

Abstract

Cell contractility regulates epithelial tissue geometry development and homeostasis. The underlying mechanobiological regulation circuits are poorly understood and experimentally challenging. We developed an elastomeric pillar cage (EPC) array to quantify cell contractility as a mechanoresponse of epithelial microtissues to substrate stiffness and topography. The spatially confined EPC geometry consisted of 24 circularly arranged slender pillars (1.2 MPa, height: 50 µm; diameter: 10 µm, distance: 5 µm). These high-aspect-ratio pillars were confined at both ends by planar substrates with different stiffness (0.15–1.2 MPa). Analytical modeling and finite elements simulation retrieved cell forces from pillar displacements. For evaluation, highly contractile myofibroblasts and cardiomyocytes were assessed to demonstrate that the EPC device can resolve static and dynamic cellular force modes. Human breast (MCF10A) and skin (HaCaT) cells grew as adherence junction-stabilized 3D microtissues within the EPC geometry. Planar substrate areas triggered the spread of monolayered clusters with substrate stiffness-dependent actin stress fiber (SF)-formation and substantial single-cell actomyosin contractility (150–200 nN). Within the same continuous microtissues, the pillar-ring topography induced the growth of bilayered cell tubes. The low effective pillar stiffness overwrote cellular sensing of the high substrate stiffness and induced SF-lacking roundish cell shapes with extremely low cortical actin tension (11–15 nN). This work introduced a versatile biophysical tool to explore mechanobiological regulation circuits driving low- and high-tensional states during microtissue development and homeostasis. EPC arrays facilitate simultaneously analyzing the impact of planar substrate stiffness and topography on microtissue contractility, hence microtissue geometry and function.
Keywords: mechanosensing; mechanotransduction; cell force measurement; cell-matrix adhesion; cell-cell adhesion; actomyosin; cell contractility; cortical actin; substrate stiffness; topography mechanosensing; mechanotransduction; cell force measurement; cell-matrix adhesion; cell-cell adhesion; actomyosin; cell contractility; cortical actin; substrate stiffness; topography

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MDPI and ACS Style

Esser, L.; Springer, R.; Dreissen, G.; Lövenich, L.; Konrad, J.; Hampe, N.; Merkel, R.; Hoffmann, B.; Noetzel, E. Elastomeric Pillar Cages Modulate Actomyosin Contractility of Epithelial Microtissues by Substrate Stiffness and Topography. Cells 2023, 12, 1256. https://doi.org/10.3390/cells12091256

AMA Style

Esser L, Springer R, Dreissen G, Lövenich L, Konrad J, Hampe N, Merkel R, Hoffmann B, Noetzel E. Elastomeric Pillar Cages Modulate Actomyosin Contractility of Epithelial Microtissues by Substrate Stiffness and Topography. Cells. 2023; 12(9):1256. https://doi.org/10.3390/cells12091256

Chicago/Turabian Style

Esser, Lisann, Ronald Springer, Georg Dreissen, Lukas Lövenich, Jens Konrad, Nico Hampe, Rudolf Merkel, Bernd Hoffmann, and Erik Noetzel. 2023. "Elastomeric Pillar Cages Modulate Actomyosin Contractility of Epithelial Microtissues by Substrate Stiffness and Topography" Cells 12, no. 9: 1256. https://doi.org/10.3390/cells12091256

APA Style

Esser, L., Springer, R., Dreissen, G., Lövenich, L., Konrad, J., Hampe, N., Merkel, R., Hoffmann, B., & Noetzel, E. (2023). Elastomeric Pillar Cages Modulate Actomyosin Contractility of Epithelial Microtissues by Substrate Stiffness and Topography. Cells, 12(9), 1256. https://doi.org/10.3390/cells12091256

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