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各向异性刚度梯度调节的机械导向驱动癌细胞的定向迁移。

Anisotropic stiffness gradient-regulated mechanical guidance drives directional migration of cancer cells.

机构信息

Academy for Advanced Interdisciplinary Studies, Peking University, Beijing 100871, China.

Department of Mechanics and Engineering Science, College of Engineering, Peking University, Beijing 100871, PR China.

出版信息

Acta Biomater. 2020 Apr 1;106:181-192. doi: 10.1016/j.actbio.2020.02.004. Epub 2020 Feb 8.

Abstract

Interfacial interactions between cancer cells and surrounding microenvironment involve complex mechanotransduction mechanisms that are directly associated with tumor invasion and metastasis. Matrix remodeling triggers heterogeneity of stiffness in tumor microenvironment and thus generates anisotropic stiffness gradient (ASG). The migration of cancer cells mediated by ASG, however, still remains elusive. Based on a multi-layer polymerization method of microstructured hydrogels with surface topology, we develop an in vitro experimental platform for mechanical interactions of cancer cells with ASG matrix microenvironment. We show that mechanical guidance of mesenchymal cells is essentially modulated by ASG, leading to a spontaneous directional migration along the orientation parallel to the maximum stiffness although there is no stiffness gradient in the direction. The ASG-regulated mechanical guidance presents an alternative way of cancer cell directional migration. Further, our findings indicate that the mechanical guidance occurs only in mesenchymal cancer cells, but not in epithelial cancer cells, implying that cell contractility may contribute to ASG-regulated migration of cells. This work is not only helpful for elucidating the role of matrix remodeling in mediating tumor cell invasion and metastasis, but has potential implications for developing specific cancer treatments. STATEMENT OF SIGNIFICANCE: Local extracellular matrix (ECM) stiffening triggers mechanical heterogeneity in tumor microenvironment, which can exert a crucial impact on interfacial interactions between tumor cells and surrounding ECM. The underlying mechanobiological mechanism that tumor cells are modulated by mechanically heterogeneous ECM, however, still remains mysterious to a great extent. Through our established in vitro platform and analysis, we have demonstrated that anisotropic stiffness gradient (ASG) has the ability to elicit directional migration of cells, essentially depending on local stiffness gradients and the corresponding absolute stiffness values. This study is not only crucial for revealing the role of matrix remodeling in regulating tumor invasion and metastasis, but also offers a valuable guidance for developing anti-tumor therapies from the biomechanical perspective.

摘要

癌细胞与周围微环境的相互作用涉及复杂的力学转导机制,这些机制与肿瘤的侵袭和转移直接相关。基质重塑触发肿瘤微环境硬度的异质性,从而产生各向异性硬度梯度(ASG)。然而,由 ASG 介导的癌细胞迁移仍然难以捉摸。基于具有表面拓扑结构的微结构化水凝胶的多层聚合方法,我们开发了一种用于癌症细胞与 ASG 基质微环境机械相互作用的体外实验平台。我们表明,间质细胞的机械引导本质上是由 ASG 调节的,导致自发的定向迁移,沿与最大硬度平行的方向,尽管在该方向上没有硬度梯度。ASG 调节的机械引导为癌细胞的定向迁移提供了另一种方式。此外,我们的发现表明,机械引导仅发生在间质癌细胞中,而不在上皮癌细胞中,这表明细胞收缩性可能有助于 ASG 调节的细胞迁移。这项工作不仅有助于阐明基质重塑在介导肿瘤细胞侵袭和转移中的作用,而且对开发特定的癌症治疗方法具有潜在意义。

意义陈述

局部细胞外基质(ECM)变硬会引发肿瘤微环境中的力学异质性,这对肿瘤细胞与周围 ECM 的界面相互作用会产生至关重要的影响。然而,肿瘤细胞受力学异质 ECM 调节的潜在力学生物学机制在很大程度上仍然神秘。通过我们建立的体外平台和分析,我们已经证明各向异性硬度梯度(ASG)能够引发细胞的定向迁移,这主要取决于局部硬度梯度和相应的绝对硬度值。这项研究不仅对于揭示基质重塑在调节肿瘤侵袭和转移中的作用至关重要,而且从生物力学的角度为开发抗肿瘤治疗方法提供了有价值的指导。

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