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通过微流控中的动态压缩和松弛将乳腺癌球体的转移潜能与粘弹性特性联系起来

Linking Metastatic Potential and Viscoelastic Properties of Breast Cancer Spheroids via Dynamic Compression and Relaxation in Microfluidics.

作者信息

Tavasso Margherita, Bordoloi Ankur D, Tanré Elsa, Dekker Sanne A H, Garbin Valeria, Boukany Pouyan E

机构信息

Department of Chemical Engineering, Delft University of Technology, Delft, 2629 HZ, The Netherlands.

École Polytechnique, Institut Polytechnique de Paris, Palaiseau, 91120, France.

出版信息

Adv Healthc Mater. 2025 Mar;14(6):e2402715. doi: 10.1002/adhm.202402715. Epub 2024 Oct 14.

Abstract

The growth and invasion of solid tumors are associated with changes in their viscoelastic properties, influenced by both internal cellular factors and physical forces in the tumor microenvironment. Due to the lack of a comprehensive investigation of tumor tissue viscoelasticity, the relationship between such physical properties and cancer malignancy remains poorly understood. Here, the viscoelastic properties of breast cancer spheroids, 3D (in vitro) tumor models, are studied in relation to their metastatic potentials by imposing controlled, dynamic compression within a microfluidic constriction, and subsequently monitoring the relaxation of the imposed deformation. By adopting a modified Maxwell model to extract viscoelastic properties from the compression data, the benign (MCF-10A) spheroids are found to have higher bulk elastic modulus and viscosity compared to malignant spheroids (MCF-7 and MDA-MB-231). The relaxation is characterized by two timescales, captured by a double exponential fitting function, which reveals a similar fast rebound for MCF-7 and MCF-10A. Both the malignant spheroids exhibit similar long-term relaxation and display residual deformation. However, they differ significantly in morphology, particularly in intercellular movements. These differences between malignant spheroids are demonstrated to be linked to their cytoskeletal organization, by microscopic imaging of F-actin within the spheroids, together with cell-cell adhesion strength.

摘要

实体瘤的生长和侵袭与它们的粘弹性特性变化相关,这些变化受肿瘤微环境中的内部细胞因素和物理力影响。由于缺乏对肿瘤组织粘弹性的全面研究,这种物理性质与癌症恶性程度之间的关系仍知之甚少。在此,通过在微流体收缩通道内施加可控的动态压缩,并随后监测施加变形的松弛情况,研究了乳腺癌球体(三维(体外)肿瘤模型)的粘弹性特性与其转移潜能之间的关系。通过采用改进的麦克斯韦模型从压缩数据中提取粘弹性特性,发现良性(MCF - 10A)球体与恶性球体(MCF - 7和MDA - MB - 231)相比具有更高的体积弹性模量和粘度。松弛由两个时间尺度表征,通过双指数拟合函数捕捉,这揭示了MCF - 7和MCF - 10A具有相似的快速回弹。两种恶性球体都表现出相似的长期松弛并显示出残余变形。然而,它们在形态上有显著差异,特别是在细胞间运动方面。通过对球体内部F - 肌动蛋白的显微镜成像以及细胞间粘附强度,证明了恶性球体之间的这些差异与其细胞骨架组织有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a835/11874651/945dfe5de6d0/ADHM-14-0-g003.jpg

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