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共培养细胞模型系统通过集体细胞迁移进行重排。

The rearrangement of co-cultured cellular model systems via collective cell migration.

机构信息

University of Belgrade, Faculty of Technology and Metallurgy, Department of Chemical Engineering, Serbia.

Laboratoire Mathematiques de Besançon, UMR-CNRS 6623, Université de Bourgogne Franche-Comte, 16 Route de Gray, Besançon 25000, France.

出版信息

Semin Cell Dev Biol. 2023 Sep 30;147:34-46. doi: 10.1016/j.semcdb.2022.10.002. Epub 2022 Oct 26.

Abstract

Cancer invasion through the surrounding epithelium and extracellular matrix (ECM) is the one of the main characteristics of cancer progression. While significant effort has been made to predict cancer cells response under various drug therapies, much less attention has been paid to understand the physical interactions between cancer cells and their microenvironment, which are essential for cancer invasion. Considering these physical interactions on various co-cultured in vitro model systems by emphasizing the role of viscoelasticity, the tissue surface tension, solid stress, and their inter-relations is a prerequisite for establishing the main factors that influence cancer cell spread and develop an efficient strategy to suppress it. This review focuses on the role of viscoelasticity caused by collective cell migration (CCM) in the context of mono-cultured and co-cultured cancer systems, and on the modeling approaches aimed at reproducing and understanding these biological systems. In this context, we do not only review previously-published biophysics models for collective cell migration, but also propose new extensions of those models to include solid stress accumulated within the spheroid core region and cell residual stress accumulation caused by CCM.

摘要

癌症通过周围上皮组织和细胞外基质(ECM)的侵袭是癌症进展的主要特征之一。虽然已经做出了很大的努力来预测癌症细胞在各种药物治疗下的反应,但对于理解癌症细胞与其微环境之间的物理相互作用关注较少,而这些相互作用对于癌症侵袭是至关重要的。考虑到各种共培养的体外模型系统中的这些物理相互作用,强调粘弹性、组织表面张力、固体应力及其相互关系的作用是确定影响癌症细胞扩散的主要因素并制定有效抑制策略的前提。本综述重点讨论了单细胞迁移(CCM)引起的粘弹性在单培养和共培养癌症系统中的作用,以及旨在再现和理解这些生物系统的建模方法。在这种情况下,我们不仅回顾了之前发表的用于单细胞迁移的生物物理模型,还提出了这些模型的新扩展,以包括球体核心区域内积累的固体应力和由 CCM 引起的细胞残余应力积累。

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