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Publication : Extracellular rigidity sensing by talin isoform-specific mechanical linkages.

First Author  Austen K Year  2015
Journal  Nat Cell Biol Volume  17
Issue  12 Pages  1597-606
PubMed ID  26523364 Mgi Jnum  J:237578
Mgi Id  MGI:5816194 Doi  10.1038/ncb3268
Citation  Austen K, et al. (2015) Extracellular rigidity sensing by talin isoform-specific mechanical linkages. Nat Cell Biol 17(12):1597-606
abstractText  The ability of cells to adhere and sense differences in tissue stiffness is crucial for organ development and function. The central mechanisms by which adherent cells detect extracellular matrix compliance, however, are still unknown. Using two single-molecule-calibrated biosensors that allow the analysis of a previously inaccessible but physiologically highly relevant force regime in cells, we demonstrate that the integrin activator talin establishes mechanical linkages following cell adhesion, which are indispensable for cells to probe tissue stiffness. Talin linkages are exposed to a range of piconewton forces and bear, on average, 7-10 pN during cell adhesion depending on their association with F-actin and vinculin. Disruption of talin's mechanical engagement does not impair integrin activation and initial cell adhesion but prevents focal adhesion reinforcement and thus extracellular rigidity sensing. Intriguingly, talin mechanics are isoform specific so that expression of either talin-1 or talin-2 modulates extracellular rigidity sensing.
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