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用于研究微环境介导的对细胞核机械刺激的3D细胞培养:癌症研究的重要一步。

3D Cell Culture for the Study of Microenvironment-Mediated Mechanostimuli to the Cell Nucleus: An Important Step for Cancer Research.

作者信息

Chhetri Apekshya, Rispoli Joseph V, Lelièvre Sophie A

机构信息

Biomedical Engineering, Purdue University, West Lafayette, IN, United States.

Department of Basic Medical Sciences, Purdue University, West Lafayette, IN, United States.

出版信息

Front Mol Biosci. 2021 Feb 10;8:628386. doi: 10.3389/fmolb.2021.628386. eCollection 2021.

Abstract

The discovery that the stiffness of the tumor microenvironment (TME) changes during cancer progression motivated the development of cell culture involving extracellular mechanostimuli, with the intent of identifying mechanotransduction mechanisms that influence cell phenotypes. Collagen I is a main extracellular matrix (ECM) component used to study mechanotransduction in three-dimensional (3D) cell culture. There are also models with interstitial fluid stress that have been mostly focusing on the migration of invasive cells. We argue that a major step for the culture of tumors is to integrate increased ECM stiffness and fluid movement characteristic of the TME. Mechanotransduction is based on the principles of tensegrity and dynamic reciprocity, which requires measuring not only biochemical changes, but also physical changes in cytoplasmic and nuclear compartments. Most techniques available for cellular rheology were developed for a 2D, flat cell culture world, hence hampering studies requiring proper cellular architecture that, itself, depends on 3D tissue organization. New and adapted measuring techniques for 3D cell culture will be worthwhile to study the apparent increase in physical plasticity of cancer cells with disease progression. Finally, evidence of the physical heterogeneity of the TME, in terms of ECM composition and stiffness and of fluid flow, calls for the investigation of its impact on the cellular heterogeneity proposed to control tumor phenotypes. Reproducing, measuring and controlling TME heterogeneity should stimulate collaborative efforts between biologists and engineers. Studying cancers in well-tuned 3D cell culture platforms is paramount to bring mechanomedicine into the realm of oncology.

摘要

肿瘤微环境(TME)的硬度在癌症进展过程中会发生变化,这一发现推动了涉及细胞外机械刺激的细胞培养技术的发展,目的是确定影响细胞表型的机械转导机制。I型胶原蛋白是用于研究三维(3D)细胞培养中机械转导的主要细胞外基质(ECM)成分。也有一些针对间质液压力的模型,这些模型大多聚焦于侵袭性细胞的迁移。我们认为,肿瘤培养的一个主要步骤是整合TME中增加的ECM硬度和流体运动特性。机械转导基于张拉整体和动态互易原理,这不仅需要测量生化变化,还需要测量细胞质和细胞核区室中的物理变化。大多数现有的细胞流变学技术是为二维平面细胞培养环境开发的,因此阻碍了对需要适当细胞结构(其本身依赖于三维组织结构)的研究。用于3D细胞培养的新型适配测量技术对于研究癌细胞随着疾病进展而出现的物理可塑性增加将是有价值的。最后,TME在ECM组成、硬度和流体流动方面的物理异质性证据,要求研究其对控制肿瘤表型的细胞异质性的影响。再现、测量和控制TME异质性应促进生物学家和工程师之间的合作。在经过良好调节的3D细胞培养平台上研究癌症对于将机械医学引入肿瘤学领域至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cb53/7902798/094fb4d0a4db/fmolb-08-628386-g001.jpg

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