A comprehensive transcriptomic comparison of hepatocyte model systems improves selection of models for experimental use

Publication date

2022-10-14

Authors

Ardisasmita, Ibrahim
Schene, Imre F.
Joore, Indi P
Kok, Gautam
Hendriks, Delilah
Artegiani, Benedetta
Mokry, MichalORCID 0000-0002-5298-4852ISNI 0000000387648231
Nieuwenhuis, Edward E.S.ISNI 0000000393345368
Fuchs, Sabine A

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Document Type

Article

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cc_by

Abstract

The myriad of available hepatocyte in vitro models provides researchers the possibility to select hepatocyte-like cells (HLCs) for specific research goals. However, direct comparison of hepatocyte models is currently challenging. We systematically searched the literature and compared different HLCs, but reported functions were limited to a small subset of hepatic functions. To enable a more comprehensive comparison, we developed an algorithm to compare transcriptomic data across studies that tested HLCs derived from hepatocytes, biliary cells, fibroblasts, and pluripotent stem cells, alongside primary human hepatocytes (PHHs). This revealed that no HLC covered the complete hepatic transcriptome, highlighting the importance of HLC selection. HLCs derived from hepatocytes had the highest transcriptional resemblance to PHHs regardless of the protocol, whereas the quality of fibroblasts and PSC derived HLCs varied depending on the protocol used. Finally, we developed and validated a web application (HLCompR) enabling comparison for specific pathways and addition of new HLCs. In conclusion, our comprehensive transcriptomic comparison of HLCs allows selection of HLCs for specific research questions and can guide improvements in culturing conditions.

Keywords

Cell Differentiation/genetics, Hepatocytes/metabolism, Humans, Induced Pluripotent Stem Cells/metabolism, Pluripotent Stem Cells, Transcriptome, Journal Article

Citation

Ardisasmita, A I, Schene, I F, Joore, I P, Kok, G, Hendriks, D, Artegiani, B, Mokry, M, Nieuwenhuis, E E S & Fuchs, S A 2022, 'A comprehensive transcriptomic comparison of hepatocyte model systems improves selection of models for experimental use', Communications biology, vol. 5, no. 1, 1094. https://doi.org/10.1038/s42003-022-04046-9