用微流控压缩装置和修正幂律模型揭示肿瘤球体的粘弹性特性。

ArXiv Pub Date : 2025-09-22
Mrinal Pandey, Bangguo Zhu, Kaitlyn Roach, Young Joon Suh, Jeffrey E Segall, Chung-Yuen Hui, Mingming Wu
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引用次数: 0

摘要

在临床上,触诊是评估肿瘤恶性程度的重要诊断方法之一。在实验室研究中,人们普遍认为肿瘤及周围组织的体刚度与肿瘤的恶性状态密切相关。在这里,我们假设除了肿瘤的刚度,肿瘤的粘弹性——即肿瘤组织受压后反弹所需的时间——也可以用来评估肿瘤的恶性状态。在这项工作中,我们利用最近开发的微流体压缩装置和理论幂律模型表征了乳腺肿瘤球体的粘弹性特性。不同恶性程度的乳腺肿瘤细胞;使用非致瘤性上皮细胞(MCF10A)、中度恶性肿瘤细胞(MCF7)和三阴性转移性肿瘤细胞(MDA-MB-231)。嵌入在三维细胞外基质中的球体被周期性压缩,并使用显微成像记录它们的应变响应。结果表明,测量的应变松弛曲线可以用修正的幂律模型描述,表明非致瘤性肿瘤球体比致瘤性肿瘤球体更具弹性,具有更短的松弛时间和更小的塑性。总之,这些结果强调,除了肿瘤球体的总体刚度外,粘弹性特性还可以作为肿瘤恶性的补充力学生物标志物,并证明了用于活体组织力学表征的修正幂律模型的有效性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Viscoelastic properties of tumor spheroids revealed by a microfluidic compression device and a modified power law model.

Viscoelastic properties of tumor spheroids revealed by a microfluidic compression device and a modified power law model.

Viscoelastic properties of tumor spheroids revealed by a microfluidic compression device and a modified power law model.

Viscoelastic properties of tumor spheroids revealed by a microfluidic compression device and a modified power law model.

Clinically, palpation is one of the important diagnostic methods to assess tumor malignancy. In laboratory research, it is well accepted that the bulk stiffness of the tumor and the surrounding tissue is closely correlated with the malignant state of the tumor. Here, we postulate that, in addition to tumor stiffness, tumor viscoelasticity - the fact that tumor tissue takes time to bounce back after compression, can also be used to evaluate the tumor malignancy state. In this work, we characterized the viscoelastic properties of breast tumor spheroids using a recently developed microfluidic compression device and a theoretical power law model. Breast tumor cells at varying malignant levels; a non-tumorigenic epithelial (MCF10A), moderately malignant tumor (MCF7) and triple negative metastatic tumor (MDA-MB-231) cells were used. Spheroids embedded within a 3D extracellular matrix were periodically compressed, and their strain responses were recorded using microscopic imaging. Our results revealed that the measured strain relaxation curves can be successfully described by a modified power law model, demonstrated that non-tumorigenic tumor spheroids were more elastic, exhibited shorter relaxation time and less plasticity than those of tumorigenic spheroids. Together, these results highlight that viscoelastic properties in addition to bulk stiffness of the tumor spheroids can serve as a complementary mechanical biomarker of tumor malignancy and demonstrate the validity of a modified power law model for the mechanical characterization of a living tissue.

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