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基质硬度对人肝细胞迁移和功能的影响——一项体外研究

The Effect of Matrix Stiffness on Human Hepatocyte Migration and Function-An In Vitro Research.

作者信息

Xia Tingting, Zhao Runze, Feng Fan, Yang Li

机构信息

Key Laboratory of Biorheological Science and Ministry of Education, Bioengineering College, Chongqing University, Chongqing 400044, China.

出版信息

Polymers (Basel). 2020 Aug 24;12(9):1903. doi: 10.3390/polym12091903.

Abstract

The extracellular matrix (ECM) regulates cellular function through the dynamic biomechanical and biochemical interplay between the resident cells and their microenvironment. Pathologically stiff ECM promotes phenotype changes in hepatocytes during liver fibrosis. To investigate the effect of ECM stiffness on hepatocyte migration and function, we designed an easy fabricated polyvinyl alcohol (PVA) hydrogel in which stiffness can be controlled by changing the concentration of glutaraldehyde. Three stiffnesses of hydrogels corresponding to the health of liver tissue, early stage, and end stage of fibrosis were selected. These were 4.8 kPa (soft), 21 kPa (moderate), and 45 kPa (stiff). For hepatocytes attachment, the hydrogel was coated with fibronectin. To evaluate the optimal concentration of fibronectin, hydrogel was coated with 0.1 mg/mL, 0.01 mg/mL, 0.005 mg/mL, or 0.003 mg/mL fibronectin, and the migratory behavior of single hepatocyte cultured on different concentrations of fibronectin was analyzed. To further explore the effect of ubstrate stiffness on hepatocyte migration, we used a stiffness controllable commercial 3D collagen gel, which has similar substrate stiffness to that of PVA hydrogel. Our result confirmed the PVA hydrogel biocompatibility with high hepatocytes survival. Fibronectin (0.01 mg/mL) promoted optimal migratory behavior for single hepatocytes. However, for confluent hepatocytes, a stiff substrate promoted hepatocellular migration compared with the soft and moderate groups via enhancing the formation of actin- and tubulin-rich structures. The gene expression analysis and protein expression analysis showed that the stiff substrate altered the phenotype of hepatocytes and induced apoptosis. Hepatocytes in stiff 3D hydrogel showed a higher proportion of cell death and expression of filopodia.

摘要

细胞外基质(ECM)通过驻留细胞与其微环境之间动态的生物力学和生化相互作用来调节细胞功能。病理性僵硬的ECM在肝纤维化过程中促进肝细胞表型改变。为了研究ECM硬度对肝细胞迁移和功能的影响,我们设计了一种易于制备的聚乙烯醇(PVA)水凝胶,其硬度可通过改变戊二醛浓度来控制。选择了三种对应于肝组织健康状态、纤维化早期和晚期的水凝胶硬度。分别为4.8 kPa(软)、21 kPa(中等)和45 kPa(硬)。为了使肝细胞附着,水凝胶用纤连蛋白包被。为了评估纤连蛋白的最佳浓度,水凝胶分别用0.1 mg/mL、0.01 mg/mL、0.005 mg/mL或0.003 mg/mL的纤连蛋白包被,并分析在不同浓度纤连蛋白上培养的单个肝细胞的迁移行为。为了进一步探索底物硬度对肝细胞迁移的影响,我们使用了一种硬度可控的商用3D胶原凝胶,其底物硬度与PVA水凝胶相似。我们的结果证实了PVA水凝胶与高肝细胞存活率的生物相容性。纤连蛋白(0.01 mg/mL)促进单个肝细胞的最佳迁移行为。然而,对于汇合的肝细胞,与软质和中等硬度组相比,硬质底物通过增强富含肌动蛋白和微管蛋白结构的形成促进肝细胞迁移。基因表达分析和蛋白质表达分析表明,硬质底物改变了肝细胞的表型并诱导细胞凋亡。在硬质3D水凝胶中的肝细胞显示出更高比例的细胞死亡和丝状伪足的表达。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7c7f/7564768/c7217773b6af/polymers-12-01903-g001.jpg

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