Human chemically-derived hepatic progenitors (hCdHs) as a source of liver organoid generation: Application in regenerative medicine, disease modeling, and toxicology testing

类有机物 诱导多能干细胞 再生医学 重编程 胚胎干细胞 祖细胞 干细胞 细胞生物学 生物 酒精性肝病 化学 癌症研究 分子生物学 细胞 生物化学 医学 肝硬化 内科学 基因
作者
Soraya Salas‐Silva,Yohan Kim,Tae Hun Kim,Myounghoi Kim,Daekwan Seo,Jeonghoon Choi,Valentina M. Factor,Haeng Ran Seo,Yeonhwa Song,Gyu Sung Choi,Yun Kyung Jung,K.-S. Kim,Kyeong Geun Lee,Jaemin Jeong,Ji Hyun Shin,Dongho Choi
出处
期刊:Biomaterials [Elsevier]
卷期号:303: 122360-122360 被引量:3
标识
DOI:10.1016/j.biomaterials.2023.122360
摘要

Several types of human stem cells from embryonic (ESCs) and induced pluripotent (iPSCs) to adult tissue-specific stem cells are commonly used to generate 3D liver organoids for modeling tissue physiology and disease. We have recently established a protocol for direct conversion of primary human hepatocytes (hPHs) from healthy donor livers into bipotent progenitor cells (hCdHs). Here we extended this culture system to generate hCdH-derived liver organoids for diverse biomedical applications. To obtain hCdHs, hPHs were cultured in reprogramming medium containing A83-01 and CHIR99021 for 7 days. Liver organoids were established from hCdHs (hCdHOs) and human liver cells (hLOs) using the same donor livers for direct comparison, as well as from hiPSCs. Organoid properties were analyzed by standard in vitro assays. Molecular changes were determined by RT-qPCR and RNA-seq. Clinical relevance was evaluated by transplantation into FRG mice, modeling of alcohol-related liver disease (ARLD) and in vitro drug-toxicity tests. hCdHs were clonally expanded as organoid cultures with low variability between starting hCdH lines. Similar to the hLOs, hCdHOs stably maintained stem cell phenotype based on accepted criteria. However, hCdHOs had an advantage over hLOs in terms of EpCAM expression, efficiency of organoid generation and capacity for directed hepatic differentiation as judged by molecular profiling, albumin secretion, glycogen accumulation, and CYP450 activities. Accordingly, FRG mice transplanted with hCdHOs survived longer than mice injected with hLOs. When exposed to ethanol, hCdHOs developed stronger ALD phenotype than hLOs as evidenced by transcriptional profiling, lipid accumulation and mitochondrial dysfunction. In drug-induced injury assays in vitro, hCdHOs showed a similar or higher sensitivity response than hPHs. hCdHOs provide a novel patient-specific stem cell-based platform for regenerative medicine, toxicology testing and modeling liver diseases.
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