2010
DOI: 10.1016/j.actbio.2010.02.035
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A novel platform for in situ investigation of cells and tissues under mechanical strain

Abstract: The mechanical micro-environment influences cellular responses such as migration, proliferation, differentiation, and apoptosis. Cells are subjected to mechanical stretching in vivo, e.g., epithelial cells during embryogenesis. Current methodologies do not allow high resolution in situ observation of cells and tissues under applied strain, which may reveal intracellular dynamics and the origin of cell mechanosensitivity. We have developed a novel polydimethylsiloxane (PDMS) substrate capable of applying tensil… Show more

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Cited by 38 publications
(34 citation statements)
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“…Second, the regularly arranged PDMS microposts can be used automatically as high-precision fiducial markers to gauge the magnitude of cell stretch, eliminating the necessary step for continuous membranes to mark their surfaces for assessments of the stretch magnitude. 29, 5657 Third, the geometry of the PDMS micropost can be precisely controlled to regulate substrate rigidity and adhesive ECM pattern independently of effects on other surface properties. 15, 5154 Thus, the mPAM system can serve as a new class of the synthetic biointerfacial system in which cell stretch, substrate rigidity, adhesive ECM pattern, and surface chemistry and topography can be independently controlled to facilitate characterization and study of complex biointerfacial cellular phenomena.…”
Section: Resultsmentioning
confidence: 99%
“…Second, the regularly arranged PDMS microposts can be used automatically as high-precision fiducial markers to gauge the magnitude of cell stretch, eliminating the necessary step for continuous membranes to mark their surfaces for assessments of the stretch magnitude. 29, 5657 Third, the geometry of the PDMS micropost can be precisely controlled to regulate substrate rigidity and adhesive ECM pattern independently of effects on other surface properties. 15, 5154 Thus, the mPAM system can serve as a new class of the synthetic biointerfacial system in which cell stretch, substrate rigidity, adhesive ECM pattern, and surface chemistry and topography can be independently controlled to facilitate characterization and study of complex biointerfacial cellular phenomena.…”
Section: Resultsmentioning
confidence: 99%
“…Lastly, Franze and Guck (2010) recently published a comprehensive review on the biophysics of neuronal growth and the susceptibility of neurons to physical cues. In brief, the methods used to study the physical properties of neurons have innovatively utilized nanowires (Hallstrom et al, 2010), force calibrated glass needles (Bernal et al, 2007), microfabricated silicon-based micromechanical force sensors (Siechen et al, 2009), optical stretchers (Lu et al, 2006), stretchable polydimethylsiloxane (PDMS) substrates (Ahmed et al , 2010), and polyacrylamide gel-based compliant substrates (Chan and Odde, 2008). Using these approaches the significant findings have been that (1) tension generation by growth cones is higher on softer (i.e.…”
Section: Forces and Axonal Elongationmentioning
confidence: 99%
“…Using these approaches the significant findings have been that (1) tension generation by growth cones is higher on softer (i.e. < ~ 1 kiloPascal) substrates (Chan and Odde, 2008), (2) glial cells provide a soft substrate that may facilitate axonal elongation (Lu et al, 2006), (3) active force generation in neurons causes them to shorten when slackened (Ahmed et al , 2010; Bernal et al , 2007), and (4) the rest tension of axons both in vivo and in vitro is in the range of 1–10 nN (Hallstrom et al , 2010; Rajagopalan et al , 2010; Siechen et al , 2009). We think there is great promise in the application of these approaches to longstanding problems in the field of molecular cell biology, not only of neurons but cells in general.…”
Section: Forces and Axonal Elongationmentioning
confidence: 99%
“…The mechanical microenvironment can affect cell proliferation, migration, differentiation, and apoptosis, as well as tissue development. 19 Different types of mechanical stimuli have been widely applied to tissue engineering of tendons. 20, 21 We used custom-fabricated springs and PGA scaffolds modified from the previous work 22, 23 to apply static stretch to DPSCs in vitro .…”
Section: Discussionmentioning
confidence: 99%