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肿瘤细胞细胞骨架组织对侵袭和迁移的影响:基于微流控通道的方法。

Impact of tumor cell cytoskeleton organization on invasiveness and migration: a microchannel-based approach.

机构信息

Department New Materials and Biosystems, Max Planck Institute for Metals Research, Stuttgart, Germany.

出版信息

PLoS One. 2010 Jan 15;5(1):e8726. doi: 10.1371/journal.pone.0008726.

Abstract

Cell migration is a fundamental feature of the interaction of cells with their surrounding. The cell's stiffness and ability to deform itself are two major characteristics that rule migration behavior especially in three-dimensional tissue. We simulate this situation making use of a micro-fabricated migration chip to test the active invasive behavior of pancreatic cancer cells (Panc-1) into narrow channels. At a channel width of 7 microm cell migration through the channels was significantly impeded due to size exclusion. A striking increase in cell invasiveness was observed once the cells were treated with the bioactive lipid sphingosylphosphorylcholine (SPC) that leads to a reorganization of the cell's keratin network, an enhancement of the cell's deformability, and also an increase in the cell's migration speed on flat surfaces. The migration speed of the highly deformed cells inside the channels was three times higher than of cells on flat substrates but was not affected upon SPC treatment. Cells inside the channels migrated predominantly by smooth sliding while maintaining constant cell length. In contrast, cells on adhesion mediating narrow lines moved in a stepwise way, characterized by fluctuations in cell length. Taken together, with our migration chip we demonstrate that the dimensionality of the environment strongly affects the migration phenotype and we suggest that the spatial cytoskeletal keratin organization correlates with the tumor cell's invasive potential.

摘要

细胞迁移是细胞与其周围环境相互作用的基本特征。细胞的刚性和自身变形的能力是控制迁移行为的两个主要特征,尤其是在三维组织中。我们利用微制造的迁移芯片模拟这种情况,以测试胰腺癌细胞(Panc-1)主动侵入狭窄通道的行为。在通道宽度为 7 微米的情况下,由于尺寸排阻,细胞穿过通道的迁移明显受到阻碍。一旦用生物活性脂质鞘磷脂磷酸胆碱 (SPC) 处理细胞,就会观察到细胞侵袭性显著增加,这导致细胞角质网络的重组、细胞变形性的增强,以及细胞在平面上的迁移速度的增加。高度变形细胞在通道内的迁移速度是细胞在平面底物上的三倍,但 SPC 处理后不受影响。细胞在通道内主要通过平滑滑动迁移,同时保持细胞长度不变。相比之下,在黏附介导的狭窄线内移动的细胞以逐步的方式移动,其特征是细胞长度波动。总之,我们通过迁移芯片证明了环境的维度强烈影响迁移表型,并且我们认为空间细胞骨架角蛋白组织与肿瘤细胞的侵袭潜力相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5989/2806915/d91a3f4f005f/pone.0008726.g001.jpg

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