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首页> 外文期刊>Molecular biology of the cell >The size-speed-force relationship governs migratory cell response to tumorigenic factors
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The size-speed-force relationship governs migratory cell response to tumorigenic factors

机译:大小-速度-力的关系控制迁移细胞对致瘤因子的反应

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Tumor development progresses through a complex path of biomechanical changes leading first to cell growth and contraction and then cell deadhesion, scattering, and invasion. Tumorigenic factors may act specifically on one of these steps or have a wider spectrum of actions, leading to a variety of effects and thus sometimes to apparent contradictory outcomes. Here we used micropatterned lines of collagen type I/fibronectin on deformable surfaces to standardize cell behavior and measure simultaneously cell size, speed of motion and magnitude of the associated traction forces at the level of a single cell. We analyzed and compared the normal human breast cell line MCF10A in control conditions and in response to various tumorigenic factors. In all conditions, a wide range of biomechanical properties was identified. Despite this heterogeneity, normal and transformed motile cells followed a common trend whereby size and contractile forces were negatively correlated with cell speed. Some tumorigenic factors, such as activation of ErbB2 or loss of the {beta}subunit of casein kinase 2, shifted the whole population toward a faster speed and lower contractility state. Treatment with transforming growth factor {beta} induced some cells to adopt opposing behaviors such as extremely high versus extremely low contractility. Thus tumor transformation amplified preexisting population heterogeneity and led some cells to exhibit biomechanical properties that were more extreme than those observed with normal cells.
机译:肿瘤的发展通过生物力学变化的复杂路径进行,首先导致细胞生长和收缩,然后导致细胞死亡,扩散和侵袭。致瘤因子可能专门作用于这些步骤之一,或者具有更广泛的作用范围,从而导致多种影响,因此有时会导致明显矛盾的结果。在这里,我们在可变形表面上使用了I型/纤连蛋白胶原蛋白的微型图案线来标准化细胞行为,并同时在单个细胞水平上测量细胞大小,运动速度和相关牵引力的大小。我们分析并比较了正常人乳腺癌细胞系MCF10A在控制条件下以及对各种致瘤因素的反应。在所有条件下,已确定了广泛的生物力学性能。尽管存在异质性,正常和转化的运动细胞仍遵循共同的趋势,即大小和收缩力与细胞速度呈负相关。一些致瘤因素,例如ErbB2的激活或酪蛋白激酶2的β亚基的丢失,使整个人群转向了更快的速度和更低的收缩状态。用转化生长因子β的处理诱导一些细胞采取相反的行为,例如极高的收缩力与极低的收缩力。因此,肿瘤转化会放大先前存在的种群异质性,并导致某些细胞表现出比正常细胞更为极端的生物力学特性。

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