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用于体外肝脏供应的海藻酸钠-聚-L-赖氨酸包封HepaRG细胞的临床前特性研究

Preclinical characterization of alginate-poly-L-lysine encapsulated HepaRG for extracorporeal liver supply.

作者信息

Pasqua Mattia, Pereira Ulysse, de Lartigue Claire, Nicolas Jonathan, Vigneron Pascale, Dermigny Quentin, Legallais Cécile

机构信息

Université de technologie de Compiègne, CNRS, Laboratoire de Biomécanique et Bioingénierie, Centre de recherche de Royallieu, Compiègne, France.

DHU Hépatinov, Villejuif, France.

出版信息

Biotechnol Bioeng. 2021 Jan;118(1):453-464. doi: 10.1002/bit.27583. Epub 2020 Oct 9.

Abstract

We recently demonstrated that HepaRG cells encapsulated into 1.5% alginate beads are capable of self-assembling into spheroids. They adequately differentiate into hepatocyte-like cells, with hepatic features observed at Day 14 post-encapsulation required for external bioartificial liver applications. Preliminary investigations performed within a bioreactor under shear stress conditions and using a culture medium mimicking acute liver failure (ALF) highlighted the need to reinforce beads with a polymer coating. We demonstrated in a first step that a poly-l-lysine coating improved the mechanical stability, without altering the metabolic activities necessary for bioartificial liver applications (such as ammonia and lactate elimination). In a second step, we tested the optimized biomass in a newly designed perfused dynamic bioreactor, in the presence of the medium model for pathological plasma for 6 h. Performances of the biomass were enhanced as compared to the steady configuration, demonstrating its efficacy in decreasing the typical toxins of ALF. This type of bioreactor is easy to scale up as it relies on the number of micro-encapsulated cells, and could provide an adequate hepatic biomass for liver supply. Its design allows it to be integrated into a hybrid artificial/bioartificial liver setup for further clinical studies regarding its impact on ALF animal models.

摘要

我们最近证明,封装在1.5%海藻酸钠珠中的HepaRG细胞能够自组装成球体。它们能充分分化为肝细胞样细胞,在封装后第14天观察到具有肝脏特征,这是外部生物人工肝应用所必需的。在生物反应器中,在剪切应力条件下并使用模拟急性肝衰竭(ALF)的培养基进行的初步研究强调了用聚合物涂层增强珠子的必要性。我们在第一步中证明,聚-L-赖氨酸涂层提高了机械稳定性,同时不改变生物人工肝应用所需的代谢活性(如氨和乳酸的清除)。在第二步中,我们在新设计的灌注动态生物反应器中,在存在病理血浆培养基模型的情况下,对优化后的生物量进行了6小时的测试。与稳定配置相比,生物量的性能得到了提高,证明了其在降低ALF典型毒素方面的功效。这种类型的生物反应器易于扩大规模,因为它依赖于微囊化细胞的数量,并且可以为肝脏供应提供足够的肝脏生物量。其设计使其能够集成到人工/生物人工肝混合装置中,以便就其对ALF动物模型的影响进行进一步的临床研究。

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