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Real-time single-cell response to stiffness

机译:实时单细胞对刚度的响应

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摘要

Living cells adapt to the stiffness of their environment. However, cell response to stiffness is mainly thought to be initiated by the deformation of adhesion complexes under applied force. In order to determine whether cell response was triggered by stiffness or force, we have developed a unique method allowing us to tune, in real time, the effective stiffness experienced by a single living cell in a uniaxial traction geometry. In these conditions, the rate of traction force buildup dF/dt was adapted to stiffness in less than 0.1 s. This integrated fast response was unambiguously triggered by stiffness, and not by force. It suggests that early cell response could be mechanical in nature. In fact, local force-dependent signaling through adhesion complexes could be triggered and coordinated by the instantaneous cell-scale adaptation of dF/dt to stiffness. Remarkably, the effective stiffness method presented here can be implemented on any mechanical setup. Thus, beyond single-cell mechanosensing, this method should be useful to determine the role of rigidity in many fundamental phenomena such as morphogenesis and development.
机译:活细胞适应其环境的僵化。然而,细胞对刚度的反应主要被认为是由外加复合物在作用力作用下的变形引起的。为了确定细胞响应是由刚度还是由力触发的,我们开发了一种独特的方法,使我们可以实时调整单活细胞在单轴牵引几何中所经历的有效刚度。在这些条件下,牵引力累积速率dF / dt在不到0.1秒的时间内就适应了刚度。这种综合的快速响应无疑是由刚度而不是力量引起的。这表明早期细胞​​反应可能是机械性的。实际上,通过粘附力的瞬时细胞规模适应性,可以触发并协调通过粘附复合物产生的局部力依赖性信号。值得注意的是,此处介绍的有效刚度方法可以在任何机械装置上实施。因此,除了单细胞机械传感之外,该方法对于确定刚性在许多基本现象(例如形态发生和发育)中的作用应该是有用的。

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