The laminin–keratin link shields the nucleus from mechanical deformation and signalling

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Abstract

The mechanical properties of the extracellular matrix dictate tissue behaviour. In epithelial tissues, laminin is a very abundant extracellular matrix component and a key supporting element. Here we show that laminin hinders the mechanoresponses of breast epithelial cells by shielding the nucleus from mechanical deformation. Coating substrates with laminin-111—unlike fibronectin or collagen I—impairs cell response to substrate rigidity and YAP nuclear localization. Blocking the laminin-specific integrin β4 increases nuclear YAP ratios in a rigidity-dependent manner without affecting the cell forces or focal adhesions. By combining mechanical perturbations and mathematical modelling, we show that β4 integrins establish a mechanical linkage between the substrate and keratin cytoskeleton, which stiffens the network and shields the nucleus from actomyosin-mediated mechanical deformation. In turn, this affects the nuclear YAP mechanoresponses, chromatin methylation and cell invasion in three dimensions. Our results demonstrate a mechanism by which tissues can regulate their sensitivity to mechanical signals.

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CITATION STYLE

APA

Kechagia, Z., Sáez, P., Gómez-González, M., Canales, B., Viswanadha, S., Zamarbide, M., … Roca-Cusachs, P. (2023). The laminin–keratin link shields the nucleus from mechanical deformation and signalling. Nature Materials, 22(11), 1409–1420. https://doi.org/10.1038/s41563-023-01657-3

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