Anisotropic 3D confinement of MCF-7 cells induces directed cell-migration and viscoelastic anisotropy of cell-membrane.

IF 2 4区生物学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY

Physical biology Pub Date : 2022-11-09 DOI:10.1088/1478-3975/ac9bc1

Privita Edwina Rayappan George Edwin, Sumeet Kumar, Srestha Roy, Basudev Roy, Saumendra Kumar Bajpai

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Abstract

Tumor-associated collagen signature-3 (TACS-3) is a prognostic indicator for breast cancer survival. It is characterized by highly organized, parallel bundles of collagen fibers oriented perpendicular to the tumor boundary, serving as directional, confining channels for cancer cell invasion. Here we design a TACS-3-mimetic anisotropic, confined collagen I matrix and examine the relation between anisotropy of matrix, directed cellular migration, and anisotropy of cell membrane-the first direct contact between TACS-3 and cell-using Michigan Cancer Foundation-7 (MCF-7) cells as cancer-model. Using unidirectional freezing, we generated ∼50μm-wide channels filled with collagen I. Optical tweezer (OT) microrheology shows that anisotropic confinement increases collagen viscoelasticity by two orders of magnitude, and the elastic modulus is significantly greater along the direction of anisotropic confinement compared to that along the orthogonal direction, thus establishing matrix anisotropy. Furthermore, MCF-7 cells embedded in anisotropic collagen I, exhibit directionality in cellular morphology and migration. Finally, using customized OT to trap polystyrene probes bound to cell-membrane (and not to ECM) of either free cells or cells under anisotropic confinement, we quantified the effect of matrix anisotropy on membrane viscoelasticity, both in-plane and out-of-plane, vis-à-vis the membrane. Both bulk and viscous modulus of cell-membrane of MCF-7 cells exhibit significant anisotropy under anisotropic confinement. Moreover, the cell membrane of MCF-7 cells under anisotropic confinement is significantly softer (both in-plane and out-of-plane moduli) despite their local environment being five times stiffer than free cells. In order to test if the coupling between anisotropy of extracellular matrix and anisotropy of cell-membrane is regulated by cell-cytoskeleton, actin cytoskeleton was depolymerized for both free and confined cells. Results show that cell membrane viscoelasticity of confined MCF-7 cells is unaffected by actin de-polymerization, in contrast to free cells. Together, these findings suggest that anisotropy of ECM induces directed migration and correlates with anisotropy of cell-membrane viscoelasticity of the MCF-7 cells in an actin-independent manner.

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MCF-7细胞的各向异性三维约束诱导细胞定向迁移和细胞膜的粘弹性各向异性。

肿瘤相关胶原标记-3 (TACS-3)是乳腺癌生存的预后指标。它的特点是高度组织化的，平行的胶原纤维束垂直于肿瘤边界，作为癌细胞入侵的定向限制通道。在这里，我们设计了一个模拟TACS-3的各向异性，限制性胶原I基质，并研究了基质的各向异性，定向细胞迁移和细胞膜的各向异性之间的关系- TACS-3和细胞之间的第一次直接接触，使用密歇根癌症基金会-7 (MCF-7)细胞作为癌症模型。通过单向冻结，我们生成了约50μm宽的填充胶原i的通道。光镊(OT)微流变学研究表明，各向异性约束使胶原的粘弹性提高了两个数量级，且各向异性约束方向的弹性模量明显大于正交方向，从而建立了基质的各向异性。此外，嵌入在各向异性胶原I中的MCF-7细胞在细胞形态和迁移方面表现出方向性。最后，在各向异性约束下，我们使用定制的OT捕获与自由细胞或细胞的细胞膜(而不是ECM)结合的聚苯乙烯探针，量化了基质各向异性对膜粘弹性的影响，包括面内和面外，-à-vis膜。在各向异性约束下，MCF-7细胞的细胞膜体积模量和黏性模量均表现出显著的各向异性。此外，在各向异性约束下，MCF-7细胞的细胞膜明显更软(面内和面外模量)，尽管它们的局部环境比自由细胞硬5倍。为了检验细胞外基质各向异性与细胞膜各向异性之间的耦合是否受到细胞-细胞骨架的调节，我们对自由细胞和受限细胞进行了肌动蛋白细胞骨架的解聚。结果表明，与自由细胞相比，受约束的MCF-7细胞的细胞膜粘弹性不受肌动蛋白解聚的影响。总之，这些发现表明，ECM的各向异性诱导定向迁移，并以不依赖于动作蛋白的方式与MCF-7细胞的细胞膜粘弹性的各向异性相关。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Physical biology 生物-生物物理

CiteScore

4.20

自引率

0.00%

发文量

审稿时长

3 months

期刊介绍： Physical Biology publishes articles in the broad interdisciplinary field bridging biology with the physical sciences and engineering. This journal focuses on research in which quantitative approaches – experimental, theoretical and modeling – lead to new insights into biological systems at all scales of space and time, and all levels of organizational complexity. Physical Biology accepts contributions from a wide range of biological sub-fields, including topics such as: molecular biophysics, including single molecule studies, protein-protein and protein-DNA interactions subcellular structures, organelle dynamics, membranes, protein assemblies, chromosome structure intracellular processes, e.g. cytoskeleton dynamics, cellular transport, cell division systems biology, e.g. signaling, gene regulation and metabolic networks cells and their microenvironment, e.g. cell mechanics and motility, chemotaxis, extracellular matrix, biofilms cell-material interactions, e.g. biointerfaces, electrical stimulation and sensing, endocytosis cell-cell interactions, cell aggregates, organoids, tissues and organs developmental dynamics, including pattern formation and morphogenesis physical and evolutionary aspects of disease, e.g. cancer progression, amyloid formation neuronal systems, including information processing by networks, memory and learning population dynamics, ecology, and evolution collective action and emergence of collective phenomena.