正弦波
肝小叶
肝细胞
血管生成
功能(生物学)
材料科学
生物医学工程
纳米技术
生物
病理
细胞生物学
体外
医学
癌症研究
免疫学
生物化学
作者
Shengnan Ya,Weiping Ding,Shibo Li,Kun Du,Yuanyuan Zhang,Chengpan Li,Jing Liu,Fenfen Li,Ping Li,Tianzhi Luo,Liqun He,Ao Xu,Dayong Gao,Bensheng Qiu
标识
DOI:10.1021/acsami.1c00794
摘要
Although various liver chips have been developed using emerging organ-on-a-chip techniques, it remains an enormous challenge to replicate the liver lobules with self-assembled perfusable hepatic sinusoid networks. Herein we develop a lifelike bionic liver lobule chip (LLC), on which the perfusable hepatic sinusoid networks are achieved using a microflow-guided angiogenesis methodology; additionally, during and after self-assembly, oxygen concentration is regulated to mimic physiologically dissolved levels supplied by actual hepatic arterioles and venules. This liver lobule design thereby produces more bionic liver microstructures, higher metabolic abilities, and longer lasting hepatocyte function than other liver-on-a-chip techniques that are able to deliver. We found that the flow through the unique micropillar design in the cell coculture zone guides the radiating assembly of the hepatic sinusoid, the oxygen concentration affects the morphology of the sinusoid by proliferation, and the oxygen gradient plays a key role in prolonging hepatocyte function. The expected breadth of applications our LLC is suited to is demonstrated by means of preliminarily testing chronic and acute hepatotoxicity of drugs and replicating growth of tumors in situ. This work provides new insights into designing more extensive bionic vascularized liver chips, while achieving longer lasting ex-vivo hepatocyte function.
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