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Characterization of primary human hepatocyte spheroids as a model system for drug-induced liver injury, liver function and disease

  • Catherine C. Bell
  • , Delilah F.G. Hendriks
  • , Sabrina M.L. Moro
  • , Ewa Ellis
  • , Joanne Walsh
  • , Anna Renblom
  • , Lisa Fredriksson Puigvert
  • , Anita C.A. Dankers
  • , Frank Jacobs
  • , Jan Snoeys
  • , Rowena L. Sison-Young
  • , Rosalind E. Jenkins
  • , Åsa Nordling
  • , Souren Mkrtchian
  • , B. Kevin Park
  • , Neil R. Kitteringham
  • , Christopher E.P. Goldring
  • , Volker M. Lauschke
  • , Magnus Ingelman-Sundberg

Research output: Contribution to journalArticlepeer-review

614 Citations (Scopus)

Abstract

Liver biology and function, drug-induced liver injury (DILI) and liver diseases are difficult to study using current in vitro models such as primary human hepatocyte (PHH) monolayer cultures, as their rapid de-differentiation restricts their usefulness substantially. Thus, we have developed and extensively characterized an easily scalable 3D PHH spheroid system in chemically-defined, serum-free conditions. Using whole proteome analyses, we found that PHH spheroids cultured this way were similar to the liver in vivo and even retained their inter-individual variability. Furthermore, PHH spheroids remained phenotypically stable and retained morphology, viability, and hepatocyte-specific functions for culture periods of at least 5 weeks. We show that under chronic exposure, the sensitivity of the hepatocytes drastically increased and toxicity of a set of hepatotoxins was detected at clinically relevant concentrations. An interesting example was the chronic toxicity of fialuridine for which hepatotoxicity was mimicked after repeated-dosing in the PHH spheroid model, not possible to detect using previous in vitro systems. Additionally, we provide proof-of-principle that PHH spheroids can reflect liver pathologies such as cholestasis, steatosis and viral hepatitis. Combined, our results demonstrate that the PHH spheroid system presented here constitutes a versatile and promising in vitro system to study liver function, liver diseases, drug targets and long-term DILI.

Original languageEnglish
Article number25187
JournalScientific Reports
Volume6
DOIs
Publication statusPublished - 4 May 2016
Externally publishedYes

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