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基于水凝胶微流控的肝芯片:模拟肝脏的质量传递和结构特征。

Hydrogel microfluidic-based liver-on-a-chip: Mimicking the mass transfer and structural features of liver.

机构信息

College of Chemical and Biological Engineering, Zhejiang University, Hangzhou, Zhejiang, China.

出版信息

Biotechnol Bioeng. 2021 Feb;118(2):612-621. doi: 10.1002/bit.27589. Epub 2020 Oct 15.

Abstract

Liver is fed by nutrition via diffusion across the vascular wall from blood flow. However, hepatocytes in liver models are directly exposed to the perfusion culture medium, where the shear stress reduces the cell viability and liver-specific functions. By mimicking the mass transfer and structural features of hepatic lobule, we designed a microfluidic liver-on-a-chip based on the di-acrylated pluronic F127 hydrogel. In the hydrogel chip, hepatocellular carcinoma HepG2 and human hepatic stellate cell LX-2 were statically cultured inside the microwells on the outer channel. These hepatic cells were fed by the diffused medium from the adjacent but separated inner channel with endothelial cell monolayers, which was perfused by the medium with physiologically relevant shear stress. As found, the hepatic cells in the liver-on-a-chip rapidly formed spheroids within 1-day incubation and expressed about one to two-fold higher viability/liver-specific functions than the corresponding static culture for at least 8 days. Moreover, the presence of endothelial cells also contributed to the expression of liver-specific functions in the liver-on-a-chip. Therefore, the proposed liver-on-a-chip provides a new concept for construction of 3D liver models in vitro, and shows the potential value for a variety of applications including bio-artificial livers and drug toxicity screening.

摘要

肝脏通过血管壁的扩散从血流中获得营养。然而,肝脏模型中的肝细胞直接暴露于灌流培养液中,其中切变应力会降低细胞活力和肝脏特异性功能。通过模拟肝小叶的质量传递和结构特征,我们基于二丙烯酸化 pluronic F127 水凝胶设计了一种基于微流控的肝芯片。在水凝胶芯片中,肝癌 HepG2 和人肝星状细胞 LX-2 在外部通道的微孔内静态培养。这些肝细胞通过与具有生理相关切变应力的培养基一起灌流的相邻但分开的内部通道中的扩散培养基进行喂养。结果发现,在孵育 1 天内,肝芯片中的肝细胞迅速形成球体,并且其活力/肝脏特异性功能表达比相应的静态培养至少高 1 至 2 倍,持续至少 8 天。此外,内皮细胞的存在也有助于肝芯片中肝脏特异性功能的表达。因此,所提出的肝芯片为体外构建 3D 肝模型提供了新概念,并显示出在生物人工肝脏和药物毒性筛选等多种应用中的潜在价值。

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