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一种嵌入了 3D 层状人肝祖细胞的体外生物人工肝缓解了猪的急性肝衰竭。

An extracorporeal bioartificial liver embedded with 3D-layered human liver progenitor-like cells relieves acute liver failure in pigs.

机构信息

Department of Interventional Oncology, Renji Hospital, Jiaotong University School of Medicine, Shanghai 200127, China.

Shanghai Celliver Biotechnology Co. Ltd., Shanghai 210201, China.

出版信息

Sci Transl Med. 2020 Jul 8;12(551). doi: 10.1126/scitranslmed.aba5146.

DOI:10.1126/scitranslmed.aba5146
PMID:32641490
Abstract

Clinical advancement of the bioartificial liver is hampered by the lack of expandable human hepatocytes and appropriate bioreactors and carriers to encourage hepatic cells to function during extracorporeal circulation. We have recently developed an efficient approach for derivation of expandable liver progenitor-like cells from human primary hepatocytes (HepLPCs). Here, we generated immortalized and functionally enhanced HepLPCs by introducing , a hepatocyte nuclear factor that enables potentially complete hepatic function. When cultured on macroporous carriers in an air-liquid interactive bioartificial liver (Ali-BAL) support device, the integrated cells were alternately exposed to aeration and nutrition and grew to form high-density three-dimensional constructs. This led to highly efficient mass transfer and supported liver functions such as albumin biosynthesis and ammonia detoxification via ureagenesis. In a porcine model of drug overdose-induced acute liver failure (ALF), extracorporeal Ali-BAL treatment for 3 hours prevented hepatic encephalopathy and led to markedly improved survival (83%, = 6) compared to ALF control (17%, = 6, = 0.02) and device-only (no-cell) therapy (0%, = 6, = 0.003). The blood ammonia concentrations, as well as the biochemical and coagulation indices, were reduced in Ali-BAL-treated pigs. Ali-BAL treatment attenuated liver damage, ameliorated inflammation, and enhanced liver regeneration in the ALF porcine model and could be considered as a potential therapeutic avenue for patients with ALF.

摘要

生物人工肝的临床进展受到可扩展的人类肝细胞以及合适的生物反应器和载体的缺乏的阻碍,这些载体和生物反应器可在体外循环期间促进肝细胞发挥功能。我们最近开发了一种从人原代肝细胞(HepLPC)中获得可扩展的肝祖细胞样细胞的有效方法。在这里,我们通过引入一种能够实现潜在完全肝功能的肝核因子 4α (HNF4α),生成了永生化和功能增强的 HepLPC。当在气液交互式生物人工肝(Ali-BAL)支持装置的大孔载体上培养时,整合细胞被交替暴露于通气和营养中,并生长形成高密度的三维结构。这导致高效的质量传递,并支持白蛋白生物合成和氨解毒等肝功能,通过尿素生成。在药物过量诱导的急性肝衰竭(ALF)的猪模型中,体外 Ali-BAL 治疗 3 小时可预防肝性脑病,并导致存活率明显提高(83%, = 6),与 ALF 对照组(17%, = 6, = 0.02)和仅设备(无细胞)治疗(0%, = 6, = 0.003)相比。接受 Ali-BAL 治疗的猪的血氨浓度以及生化和凝血指数降低。Ali-BAL 治疗减轻了 ALF 猪模型中的肝损伤,改善了炎症,并增强了肝再生,可被视为 ALF 患者的一种潜在治疗途径。

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