Mechanical force is a fundamental regulator of cell phenotype. Myofibroblasts are central mediators of fibrosis, a major unmet clinical need characterised by the deposition of excessive matrix proteins. Traction forces of myofibroblasts play a key role in remodelling the matrix and modulate the activities of embedded stromal cells. Here, we employ a combination of unsupervised computational analysis, cytoskeletal profiling and single cell traction force microscopy as a functional readout to uncover how the complex spatiotemporal dynamics and mechanics of living human myofibroblast shape sub-cellular profiling of traction forces in fibrosis. We resolve distinct biophysical communities of myofibroblasts, and our results provide a new paradigm for studying functional heterogeneity in human stromal cells.
Single cell force profiling of human myofibroblasts reveals a biophysical spectrum of cell states.
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作者:Layton Thomas B, Williams Lynn, Colin-York Huw, McCann Fiona E, Cabrita Marisa, Feldmann Marc, Brown Cameron, Xie Weilin, Fritzsche Marco, Furniss Dominic, Nanchahal Jagdeep
| 期刊: | Biology Open | 影响因子: | 1.700 |
| 时间: | 2020 | 起止号: | 2020 Mar 24; 9(3):bio049809 |
| doi: | 10.1242/bio.049809 | ||
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