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A 3D alcoholic liver disease model on a chip

Authors
Lee, JaeSeoChoi, BongHwanNo, Da YoonLee, GeonHuiLee, Seung-riOh, HyunJikLee, Sang-Hoon
Issue Date
2016
Publisher
ROYAL SOC CHEMISTRY
Citation
INTEGRATIVE BIOLOGY, v.8, no.3, pp.302 - 308
Indexed
SCIE
SCOPUS
Journal Title
INTEGRATIVE BIOLOGY
Volume
8
Number
3
Start Page
302
End Page
308
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/90118
DOI
10.1039/c5ib00298b
ISSN
1757-9694
Abstract
Alcohol is one of the main causes of liver diseases, and the development of alcoholic liver disease (ALD) treatment methods has been one of the hottest issues. For this purpose, development of in vitro models mimicking the in vivo physiology is one of the critical requirements, and they help to determine the disease mechanisms and to discover the treatment method. Herein, a three-dimensional (3D) ALD model was developed and its superior features in mimicking the in vivo condition were demonstrated. A spheroid-based microfluidic chip was employed for the development of the 3D in vitro model of ALD progression. We co-cultured rat primary hepatocytes and hepatic stellate cells (HSCs) in a fluidic chip to investigate the role of HSCs in the recovery of liver with ALD. An interstitial level of flow derived by an osmotic pump was applied to the chip to provide in vivo mimicking of fluid activity. Using this in vitro tool, we were able to observe structural changes and decreased hepatic functions with the increase in ethanol concentration. The recovery process of liver injured by alcohol was observed by providing fresh culture medium to the damaged 3D liver tissue for few days. A reversibly- and irreversibly-injured ALD model was established. The proposed model can not only be used for the research of alcoholic disease mechanism, but also has the potential for use in studies of hepatotoxicity and drug screening applications.
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