| Literature DB >> 34559943 |
Manon C Bouwmeester1, Paulina N Bernal2, Loes A Oosterhoff1, Monique E van Wolferen1, Vivian Lehmann1,3, Monique Vermaas1, Maj-Britt Buchholz1, Quentin C Peiffer2, Jos Malda1,2, Luc J W van der Laan4, Nynke I Kramer5,6, Kerstin Schneeberger1, Riccardo Levato1,2, Bart Spee1.
Abstract
There is a need for long-lived hepatic in vitro models to better predict drug induced liver injury (DILI). Human liver-derived epithelial organoids are a promising cell source for advanced in vitro models. Here, organoid technology is combined with biofabrication techniques, which holds great potential for the design of in vitro models with complex and customizable architectures. Here, porous constructs with human hepatocyte-like cells derived from organoids are generated using extrusion-based printing technology. Cell viability of bioprinted organoids remains stable for up to ten days (88-107% cell viability compared to the day of printing). The expression of hepatic markers, transporters, and phase I enzymes increased compared to undifferentiated controls, and is comparable to non-printed controls. Exposure to acetaminophen, a well-known hepatotoxic compound, decreases cell viability of bioprinted liver organoids to 21-51% (p < 0.05) compared to the start of exposure, and elevated levels of damage marker miR-122 are observed in the culture medium, indicating the potential use of the bioprinted constructs for toxicity testing. In conclusion, human liver-derived epithelial organoids can be combined with a biofabrication approach, thereby paving the way to create perfusable, complex constructs which can be used as toxicology- and disease-models.Entities:
Keywords: drug induced liver injury; extrusion-based bioprinting; in vitro modeling; organoids
Mesh:
Year: 2021 PMID: 34559943 DOI: 10.1002/mabi.202100327
Source DB: PubMed Journal: Macromol Biosci ISSN: 1616-5187 Impact factor: 4.979