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首页> 外文期刊>Lab on a chip >A new micropatterning method of soft substrates reveals that different tumorigenic signals can promote or reduce cell contraction levels
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A new micropatterning method of soft substrates reveals that different tumorigenic signals can promote or reduce cell contraction levels

机译:一种新的软底物微图案化方法揭示了不同的致瘤信号可以促进或降低细胞收缩水平

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摘要

In tissues, cell microenvironment geometry and mechanics strongly impact on cell physiology. Surface micropatterning allows the control of geometry while deformable substrates of tunable stiffness are well suited for the control of the mechanics. We developed a new method to micropattern extracellular matrix proteins on poly-acrylamide gels in order to simultaneously control cell geometry and mechanics. Microenvironment geometry and mechanics impinge on cell functions by regulating the development of intra-cellular forces. We measured these forces in micropatterned cells. Micropattern geometry was streamlined to orient forces and place cells in comparable conditions. Thereby force measurement method could be simplified and applied to large-scale experiment on chip. We applied this method to mammary epithelial cells with traction force measurements in various conditions to mimic tumoral transformation. We found that, contrary to the current view, all transformation phenotypes were not always associated to an increased level of cell contractility.
机译:在组织中,细胞微环境的几何形状和力学对细胞生理有很大影响。表面微图案化可以控制几何形状,而具有可调刚度的可变形基板非常适合于机械控制。我们开发了一种在聚丙烯酰胺凝胶上微模式化细胞外基质蛋白的新方法,以便同时控制细胞的几何形状和力学。微环境的几何和力学通过调节细胞内力的发展来影响细胞功能。我们在微模式细胞中测量了这些力。简化了微图案的几何形状,以定向力并将细胞放置在可比较的条件下。从而可以简化测力方法,并应用于大规模的芯片实验。我们将这种方法应用于乳腺上皮细胞,并在各种情况下通过牵引力测量来模拟肿瘤转化。我们发现,与当前观点相反,所有转化表型并不总是与细胞收缩性水平升高相关。

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