3D-bioprinted cholangiocarcinoma-on-a-chip model for evaluating drug responses

被引:0
|
作者
Qiong Liu [1 ,2 ,3 ]
Luis SMille [1 ,4 ]
Cesar Villalobos [1 ,5 ]
Ingrid Anaya [1 ,5 ]
Matthias Vostatek [1 ,6 ]
Sili Yi [1 ]
Wanlu Li [1 ]
Junlong Liao [1 ]
Huanghui Wu [2 ,3 ]
Yongteng Song [2 ,7 ]
Lize Xiong [2 ,3 ]
Yu Shrike Zhang [1 ]
机构
[1] Division of Engineering in Medicine, Department of Medicine, Brigham and Women's Hospital, Harvard Medical School
[2] Translational Research Institute of Brain and Brain-Like Intelligence, Shanghai Fourth People's Hospital, School of Medicine, Tongji University
[3] Shanghai Key Laboratory of Anesthesiology and Brain Functional Modulation
[4] Department of Bioengineering, Stanford University
[5] Biotechnological Engineering Program, Monterrey Institute of Technology and Higher Education
[6] Molecular Biotechnology, University of Applied Sciences Campus Vienna 
[7] Rapid Manufacturing Engineering Center, School of Mechatronical Engineering and Automation, Shanghai
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暂无
中图分类号
R965.1 [药物筛选和实验模型]; TN40 [一般性问题];
学科分类号
摘要
Cholangiocarcinoma(CCA) is characterized by heterogeneous mutations and a refractory nature. Thus, the development of a model for effective drug screening is urgently needed. As the established therapeutic testing models for CCA are often ineffective, we fabricated an enabling three-dimensional(3D)-bioprinted CCA-on-a-chip model that to a good extent resembled the multicellular microenvironment and the anatomical microstructure of the hepato-vascular–biliary system to perform high-content antitumor drug screening. Specifically, cholangiocytes, hepatocytes, and vascular endotheliocytes were employed for 3D bioprinting of the models, allowing for a high degree of spatial and tube-like microstructural control.Interestingly, it was possible to observe CCA cells attached to the surfaces of the gelatin methacryloyl(Gel MA) hydrogelembedded microchannels and overgrown in a thickening manner, generating bile duct stenosis, which was expected to be analogous to the in vivo configuration. Over 4000 differentially expressed genes were detected in the CCA cells in our 3D coculture model compared to the traditional two-dimensional(2D) monoculture. Further screening revealed that the CCA cells grown in the 3D traditional model were more sensitive to the antitumoral prodrug than those in the 2D monoculture due to drug biotransformation by the neighboring functional hepatocytes. This study provides proof-of-concept validation of our bioprinted CCA-on-a-chip as a promising drug screening model for CCA treatment and paves the way for potential personalized medicine strategies for CCA patients in the future.
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页码:373 / 389
页数:17
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