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在具有可调硬度的 3D 层层微制造光交联 PEG 支架内的癌细胞迁移。

Cancer cell migration within 3D layer-by-layer microfabricated photocrosslinked PEG scaffolds with tunable stiffness.

机构信息

Department of NanoEngineering, University of California, San Diego, La Jolla, CA 92121, USA.

出版信息

Biomaterials. 2012 Oct;33(29):7064-70. doi: 10.1016/j.biomaterials.2012.06.012. Epub 2012 Jul 16.

Abstract

Our current understanding of 3-dimensional (3D) cell migration is primarily based on results from fibrous scaffolds with randomly organized internal architecture. Manipulations that change the stiffness of these 3D scaffolds often alter other matrix parameters that can modulate cell motility independently or synergistically, making observations less predictive of how cells behave when migrating in 3D. In order to decouple microstructural influences and stiffness effects, we have designed and fabricated 3D polyethylene glycol (PEG) scaffolds that permit orthogonal tuning of both elastic moduli and microstructure. Scaffolds with log-pile architectures were used to compare the 3D migration properties of normal breast epithelial cells (HMLE) and Twist-transformed cells (HMLET). Our results indicate that the nature of cell migration is significantly impacted by the ability of cells to migrate in the third dimension. 2D ECM-coated PEG substrates revealed no statistically significant difference in cell migration between HMLE and HMLET cells among substrates of different stiffness. However, when cells were allowed to move along the third dimension, substantial differences were observed for cell displacement, velocity and path straightness parameters. Furthermore, these differences were sensitive to both substrate stiffness and the presence of the Twist oncogene. Importantly, these 3D modes of migration provide insight into the potential for oncogene-transformed cells to migrate within and colonize tissues of varying stiffness.

摘要

我们目前对于三维(3D)细胞迁移的理解主要基于具有随机组织内部结构的纤维支架的结果。改变这些 3D 支架的刚度的操作常常改变其他可以独立或协同调节细胞迁移的基质参数,使得观察结果不太能预测细胞在 3D 中迁移时的行为。为了分离微观结构的影响和刚度效应,我们设计并制造了允许同时调整弹性模量和微观结构的 3D 聚乙二醇(PEG)支架。使用具有对数堆积结构的支架来比较正常乳腺上皮细胞(HMLE)和 Twist 转化细胞(HMLET)的 3D 迁移特性。我们的结果表明,细胞在第三维中迁移的能力显著影响细胞迁移的性质。在不同刚度的基底上,2D ECM 涂覆的 PEG 基底上 HMLE 和 HMLET 细胞的迁移没有统计学上的显著差异。然而,当允许细胞沿第三维移动时,细胞位移、速度和路径直度参数观察到显著差异。此外,这些差异对基底刚度和 Twist 癌基因的存在均敏感。重要的是,这些 3D 迁移模式为研究癌基因转化细胞在不同刚度的组织内迁移和定植的潜力提供了深入的见解。

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