论文标题

自由包装的颗粒系统中的细胞反应

Cell response in free-packed granular systems

论文作者

Cunha, Ana F., Matias, André F. V., Dias, Cristóvão S., Oliveira, Mariana B., Araújo, Nuno A. M., Mano, João F.

论文摘要

研究活细胞与机械稳定(Visco)弹性材料的相互作用的研究,可以理解和利用由细胞 - 纤维细胞通信介导的生理现象。但是,对细胞和周围物体具有不同稳定性模式的相互作用的洞察力可能会揭示可能针对创新应用设计的细胞反应。在这里,假设细胞附着,散布和运动在微粒的颗粒床上的效率取决于微粒直径,这增加了对细胞颗粒键增强必要的最小牵引力的可能性,以及长期的细胞粘附。结果表明,具有14-20μM的微粒易于细胞介导的迁移率,具有诱导早期细胞脱离的潜力,而直径为38-85μm的物体可实现长期持久的细胞粘附和增殖。提出了一种解决细胞粘附时间依赖时间的生物学机制的基于Silico混合粒子的模型,为工程平台提供了启发,以应对与医疗保健相关的挑战。

The study of the interactions of living adherent cells with mechanically stable (visco)elastic materials enables understanding and exploiting physiological phenomena mediated by cell-extracellular communication. However, insight on the interaction of cells and surrounding objects with different stability patterns upon cell contact might unveil cell responses that may be engineered for innovative applications. Here, it is hypothesized that the efficiency of cell attachment, spreading and movement across a free-packed granular bed of microparticles depend on microparticle diameter, raising the possibility of a necessary minimum traction force for the reinforcement of cell-particle bonds, and long-term cell adhesion. The results suggest that microparticles with 14-20 μm are prone to cell-mediated mobility, holding the potential of inducing early cell detachment, while objects with diameters from 38-85 μm enable long-lasting cell adhesion and proliferation. An in-silico hybrid particle-based model that addresses time-dependent biological mechanisms of cell adhesion is proposed, providing inspiration for engineering platforms to address healthcare-related challenges.

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