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通过介电谱对 3D 培养中的 hiPSC 扩增和肝向分化进行在线监测。

Online monitoring of hiPSC expansion and hepatic differentiation in 3D culture by dielectric spectroscopy.

机构信息

iBET, Instituto de Biologia Experimental e Tecnológica, Oeiras, Portugal.

Instituto de Tecnologia Química e Biológica António Xavier, Universidade Nova de Lisboa, Oeiras, Portugal.

出版信息

Biotechnol Bioeng. 2021 Sep;118(9):3610-3617. doi: 10.1002/bit.27751. Epub 2021 Mar 25.

Abstract

Hepatocyte-like cells derived from human-induced pluripotent stem cells (hiPSC-HLC) are expected to have important applications in drug screening and regenerative medicine. However, hiPSC-HLC are difficult to produce on a large-scale to obtain relevant numbers for such applications. The aim of this study was to implement a novel integrated strategy for scalable production of hiPSC-HLC and demonstrate the applicability of dielectric spectroscopy to monitor hiPSC expansion/differentiation processes. We cultured hiPSC as three-dimensional (3D) aggregates in stirred-tank bioreactors (STB) operated in perfusion with an in situ capacitance probe. Dissolved oxygen concentration and dilution rate were controlled along the process and after 5 days of cell expansion, the hepatic differentiation was integrated in sequential steps for 28 days. The hiPSC were able to grow as 3D aggregates and the expression of hepatic markers and albumin production after differentiation confirmed that hepatocyte differentiation improved when compared to 2D culture. These hiPSC-HLC exhibited functional characteristics of hepatocytes including glycogen storage and drug metabolization capacity. Our results also show a good correlation between the cell permittivity measured online and the aggregate biovolume measured by standard offline methods, demonstrating for the first time the potential of dielectric spectroscopy to monitor hiPSC expansion and differentiation in STB.

摘要

人诱导多能干细胞(hiPSC)来源的肝细胞样细胞(hiPSC-HLC)有望在药物筛选和再生医学中具有重要应用。然而,hiPSC-HLC 难以大规模生产,无法获得此类应用所需的相关数量。本研究旨在实施一种新型的规模化生产 hiPSC-HLC 的综合策略,并证明介电谱可用于监测 hiPSC 扩增/分化过程。我们将 hiPSC 作为三维(3D)聚集体在搅拌罐生物反应器(STB)中进行培养,该生物反应器以灌注方式运行,并配备原位电容探头。在整个过程中控制溶解氧浓度和稀释率,细胞扩增 5 天后,以顺序步骤进行 28 天的肝分化。hiPSC 能够作为 3D 聚集体生长,分化后的肝标志物表达和白蛋白产生证实与 2D 培养相比,肝分化得到改善。这些 hiPSC-HLC 表现出肝细胞的功能特性,包括糖原储存和药物代谢能力。我们的结果还表明,在线测量的细胞介电常数与通过标准离线方法测量的聚集体生物量之间存在良好的相关性,首次证明介电谱在 STB 中监测 hiPSC 扩增和分化的潜力。

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