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首页> 外文期刊>Tissue engineering, Part C. Methods >Three-Dimensional Spheroid Primary Human Hepatocytes in Monoculture and Coculture with Nonparenchymal Cells
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Three-Dimensional Spheroid Primary Human Hepatocytes in Monoculture and Coculture with Nonparenchymal Cells

机译:单培养和与非正良细胞的三维球形原代人肝细胞和共核细胞

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Recent advances in the development of various culture platforms are promising for achieving more physiologically relevant in vitro hepatic models using primary human hepatocytes (PHHs). Previous studies have shown the value of PHHs three-dimensional (3D) spheroid models, cultured in low cell number (1330-2000 cells/3D spheroid), to study long-term liver function as well as pharmacological drug effects and toxicity. In this study, we report that only plateable PHHs aggregate and form compact 3D spheroids with a success rate of 79%, and 96% reproducibility. Out of 3D spheroid forming PHH lots, 65% were considered stable (50% ATP decrease) over the subsequent 14 days of culture, with reproducibility of a given PHH lot being 82%. We also report successful coculturing of PHHs with human liver nonparenchymal cells (NPCs). Crude P1(c)-NPC fractions were obtained by low centrifugation of the PHH supernatant fraction followed by a few days of culture before harvesting and cryopreservation. At aggregation of PHHs/P1(c)-NPCs (2:1 ratio 3D spheroids), liver sinusoidal endothelial cells, Kupffer cells, and hepatic stellate cells were successfully integrated and remained present throughout the subsequent 14-day culture period as revealed by mRNA expression markers and immunostaining. Increased mRNA expression of albumin (ALB), apolipoprotein B (APOB), cytochrome P450 3A4 (CYP3A4), and increased albumin secretion compared to PHH 3D spheroid monocultures highlighted that in a 3D spheroid coculture, configuration with NPCs, PHH functionality is increased. We thus achieved the development of a more integrated coculture model system requiring low cell numbers, of particular interest due to the scarcity of human liver NPCs.
机译:各种文化平台发展的最新进展是使用原代人肝细胞(PHHS)实现更生理相关的体外肝脏模型。以前的研究表明,在低细胞数(1330-2000个细胞/ 3D球状体)中培养的PHHS三维(3D)球状模型的值,以研究长期肝功能以及药理药物作用和毒性。在这项研究中,我们报告说,只有相块性的PHHS骨料和形成紧凑的3D球状体,成功率为79%和96%的重现性。除了3D球体形成PHH批次中,在随后的14天内被认为是稳定的(& 50%的ATP减少),具有给定的鼠标的再现性为82%。我们还报告了用人肝非正生细胞(NPC)的PHHS成功的PHHS。通过低离心PHH上清液馏分随后在收获和冷冻保存之前,通过低离心而获得粗P1(c)-NPC级分。在PHHS / P1(c)的聚集下 - NPC(2:1比率3D球状体),肝正弦内皮细胞,kupffer细胞和肝星状细胞成功整合并保持在随后的14天培养期内,如mRNA所显示的表达标记和免疫染色。与PHH 3D球形单体形式相比,白蛋白(ALB),载脂蛋白B(APOB),细胞色素P450 3A4(CYP3A4),细胞色素P450 3A4(CYP3A4)和随着白蛋白分泌的增加的增加,增加了NPC,PHH功能的配置。因此,我们实现了一种更加综合的共培养模型系统,需要低细胞数,由于人肝NPC的稀缺而特别兴趣。

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