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Experimental determination of folding factor of benign breast cancer cell (MCF10A) and its effect on contact models and 3D manipulation of biological particles

机译:实验测定良性乳腺癌细胞(MCF10A)的折叠因子及其对生物粒子接触模型和3D操纵的影响

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摘要

Plasma membrane of most cells is not smooth. The surfaces of both small and large micropermeable cells are folded and corrugated which makes mammalian cells to have a larger membrane surface than the supposed ideal mode, that is, the smooth sphere of the same volume. Since cancer is an anthropic disease, cancer cells tend to have a larger membrane area than normal cells. Therefore, cancer cells have higher folding factor and larger radius than normal and healthy cells. On the other hand, the prevalence of breast cancer has prompted researchers to improve the treatment options raised for the disease in the past. In this paper, the impact of folding factor of the cell surface has been investigated. Considering that AFM is one of the most effective tools in performing the tests at micro- and nanoscales, it was used to determine the topography of MCF10 cells and then the resulting images and results were used to experimentally extract the folding factor of cells. By applying this factor in the Hertz, DMT and JKR contact models in the elastic and viscoelastic states, these models have been modified and the simulation of the three models shows that the simulation results are closer to the experimental results by considering the folding in the calculations. Additionally, the simulation of 3D manipulation has been done in both elastic and viscoelastic states with and without consideration of folding. Finally, the results were compared to investigate the effects of folding of the cell surface to the critical force and critical time of sliding and rolling in contact with the substrate and AFM tip in the 3D manipulation model.
机译:大多数细胞的血浆膜不是光滑的。小型和大微型细胞的表面折叠和波纹,其使哺乳动物细胞具有比假定的理想模式更大的膜表面,即相同体积的光滑球。由于癌症是一种人类疾病,癌细胞倾向于具有比正常细胞更大的膜面积。因此,癌细胞具有比正常和健康细胞更高的折叠因子和较大的半径。另一方面,乳腺癌的患病率促使研究人员改善过去疾病所提出的治疗选择。本文研究了细胞表面的折叠因子的影响。考虑到AFM是在微型和纳米级进行测试中最有效的工具之一,它用于确定MCF10细胞的形貌,然后使用所得的图像和结果来通过实验提取细胞的折叠因子。通过在弹性和粘弹性状态的赫兹,DMT和JKR接触型号中应用此因素,这些模型已经修改,三种模型的仿真表明,通过考虑计算中的折叠,模拟结果更接近实验结果。另外,在弹性和粘弹性状态下进行了3D操纵的模拟,并且不考虑折叠。最后,将结果进行比较,以研究折叠细胞表面与3D操纵模型中的基板和AFM尖端的滑动和滚动的临界力和临界时的影响。

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