Abstract:Articular chondrocytes experience a variety of mechanical stimuli during daily activity. One such stimulus, direct shear, is known to affect chondrocyte homeostasis and induce catabolic or anabolic pathways. Understanding how single chondrocytes respond biomechanically and morphologically to various levels of applied shear is an important first step toward elucidating tissue level responses and disease etiology. To this end, a novel videocapture method was developed in this study to examine the effect of direc… Show more
“…a unique set of passive material properties cannot be identified for a cell. The significant contribution of the actin cytoskeleton to the mechanical response of cells has been demonstrated in numerous experimental studies [17,18]. It has recently been demonstrated that a computational cell model must include the key features of remodelling and contractility of the actin cytoskeleton in order to provide a realistic prediction of cell biomechanical response to physical stimuli [18][19][20][21][22].…”
Section: Previous Studies Have Assumed Simple Viscoelastic Constitutimentioning
Publication InformationReynolds, NH,Ronan, W,Dowling, EP,Owens, P,McMeeking, RM,McGarry, JP (2014) 'On the role of the actin cytoskeleton and nucleus in the biomechanical response of spread cells '. Biomaterials,.
“…a unique set of passive material properties cannot be identified for a cell. The significant contribution of the actin cytoskeleton to the mechanical response of cells has been demonstrated in numerous experimental studies [17,18]. It has recently been demonstrated that a computational cell model must include the key features of remodelling and contractility of the actin cytoskeleton in order to provide a realistic prediction of cell biomechanical response to physical stimuli [18][19][20][21][22].…”
Section: Previous Studies Have Assumed Simple Viscoelastic Constitutimentioning
Publication InformationReynolds, NH,Ronan, W,Dowling, EP,Owens, P,McMeeking, RM,McGarry, JP (2014) 'On the role of the actin cytoskeleton and nucleus in the biomechanical response of spread cells '. Biomaterials,.
“…The glass substrate containing the cells was then placed in a Petri dish on an inverted microscope. A shear deformation was applied to individual cells by a tungsten probe [22]. Initially, the probe was positioned adjacent to the cell, 4 mm above the substrate (figure 1a).…”
The biomechanisms that govern the response of chondrocytes to mechanical stimuli are poorly understood. In this study, a series of in vitro tests are performed, in which single chondrocytes are subjected to shear deformation by a horizontally moving probe. Dramatically different probe force -indentation curves are obtained for untreated cells and for cells in which the actin cytoskeleton has been disrupted. Untreated cells exhibit a rapid increase in force upon probe contact followed by yielding behaviour. Cells in which the contractile actin cytoskeleton was removed exhibit a linear force -indentation response. In order to investigate the mechanisms underlying this behaviour, a three-dimensional active modelling framework incorporating stress fibre (SF) remodelling and contractility is used to simulate the in vitro tests. Simulations reveal that the characteristic force -indentation curve observed for untreated chondrocytes occurs as a result of two factors: (i) yielding of SFs due to stretching of the cytoplasm near the probe and (ii) dissociation of SFs due to reduced cytoplasm tension at the front of the cell. In contrast, a passive hyperelastic model predicts a linear force -indentation curve similar to that observed for cells in which the actin cytoskeleton has been disrupted. This combined modelling -experimental study offers a novel insight into the role of the active contractility and remodelling of the actin cytoskeleton in the response of chondrocytes to mechanical loading.
“…These microarrays have been used to study the adhesion and contractility of static cells [8,10] cells subjected to local [11] and global applied deformation [12], cell migration [13,14], and cell -cell adhesion [15]. Micropost arrays provide detailed quantitative data about the contractility of cells and measure tractions at a number of points on the cell [8], in contrast to whole-cell measurements obtained from atomic force microscopy or cell probing [16][17][18]. Numerous different designs of these arrays exist, with variations in the length and diameter of the pillars, the spacing between pillars, and the arrangement in square or triangular patterns.…”
Experimental studies where cells are seeded on micropost arrays in order to quantify their contractile behaviour are becoming increasingly common. Interpretation of the data generated by this experimental technique is difficult, due to the complexity of the processes underlying cellular contractility and mechanotransduction. In the current study, a coupled framework that considers strain rate dependent contractility and remodelling of the cytoskeleton is used in tandem with a thermodynamic model of tension dependent focal adhesion formation to investigate the
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