Proteome-wide analyses of human hepatocytes during differentiation and dedifferentiation

Failure to predict hepatotoxic drugs in preclinical testing makes it imperative to develop better liver models with a stable phenotype in culture. Stem cell-derived models offer promise, with differentiated hepatocyte-like cells currently considered to be “fetal-like” in their maturity. However, thi...

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Autores principales: Rowe, Cliff, Gerrard, Dave T, Jenkins, Roz, Berry, Andrew, Durkin, Kesta, Sundstrom, Lars, Goldring, Chris E, Park, B Kevin, Kitteringham, Neil R, Hanley, Karen Piper, Hanley, Neil A
Formato: Online Artículo Texto
Lenguaje:English
Publicado: WILEY-VCH Verlag 2013
Materias:
Liver Biology/Pathobiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3842115/
https://www.ncbi.nlm.nih.gov/pubmed/23526496
http://dx.doi.org/10.1002/hep.26414
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author Rowe, Cliff
Gerrard, Dave T
Jenkins, Roz
Berry, Andrew
Durkin, Kesta
Sundstrom, Lars
Goldring, Chris E
Park, B Kevin
Kitteringham, Neil R
Hanley, Karen Piper
Hanley, Neil A
author_facet Rowe, Cliff
Gerrard, Dave T
Jenkins, Roz
Berry, Andrew
Durkin, Kesta
Sundstrom, Lars
Goldring, Chris E
Park, B Kevin
Kitteringham, Neil R
Hanley, Karen Piper
Hanley, Neil A
author_sort Rowe, Cliff
collection PubMed
description Failure to predict hepatotoxic drugs in preclinical testing makes it imperative to develop better liver models with a stable phenotype in culture. Stem cell-derived models offer promise, with differentiated hepatocyte-like cells currently considered to be “fetal-like” in their maturity. However, this judgment is based on limited biomarkers or transcripts and lacks the required proteomic datasets that directly compare fetal and adult hepatocytes. Here, we quantitatively compare the proteomes of human fetal liver, adult hepatocytes, and the HepG2 cell line. In addition, we investigate the proteome changes in human fetal and adult hepatocytes when cultured in a new air-liquid interface format compared to conventional submerged extracellular matrix sandwich culture. From albumin and urea secretion, and luciferase-based cytochrome P450 activity, adult hepatocytes were viable in either culture model over 2 weeks. The function of fetal cells was better maintained in the air-liquid interface system. Strikingly, the proteome was qualitatively similar across all samples but hierarchical clustering showed that each sample type had a distinct quantitative profile. HepG2 cells more closely resembled fetal than adult hepatocytes. Furthermore, clustering showed that primary adult hepatocytes cultured at the air-liquid interface retained a proteome that more closely mimicked their fresh counterparts than conventional culture, which acquired myofibroblast features. Principal component analysis extended these findings and identified a simple set of proteins, including cytochrome P450 2A6, glutathione S transferase P, and alcohol dehydrogenases as specialized indicators of hepatocyte differentiation. Conclusion: Our quantitative datasets are the first that directly compare multiple human liver cells, define a model for enhanced maintenance of the hepatocyte proteome in culture, and provide a new protein “toolkit” for determining human hepatocyte maturity in cultured cells. (Hepatology 2013;58:799–809)
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spelling pubmed-38421152013-12-02 Proteome-wide analyses of human hepatocytes during differentiation and dedifferentiation Rowe, Cliff Gerrard, Dave T Jenkins, Roz Berry, Andrew Durkin, Kesta Sundstrom, Lars Goldring, Chris E Park, B Kevin Kitteringham, Neil R Hanley, Karen Piper Hanley, Neil A Hepatology Liver Biology/Pathobiology Failure to predict hepatotoxic drugs in preclinical testing makes it imperative to develop better liver models with a stable phenotype in culture. Stem cell-derived models offer promise, with differentiated hepatocyte-like cells currently considered to be “fetal-like” in their maturity. However, this judgment is based on limited biomarkers or transcripts and lacks the required proteomic datasets that directly compare fetal and adult hepatocytes. Here, we quantitatively compare the proteomes of human fetal liver, adult hepatocytes, and the HepG2 cell line. In addition, we investigate the proteome changes in human fetal and adult hepatocytes when cultured in a new air-liquid interface format compared to conventional submerged extracellular matrix sandwich culture. From albumin and urea secretion, and luciferase-based cytochrome P450 activity, adult hepatocytes were viable in either culture model over 2 weeks. The function of fetal cells was better maintained in the air-liquid interface system. Strikingly, the proteome was qualitatively similar across all samples but hierarchical clustering showed that each sample type had a distinct quantitative profile. HepG2 cells more closely resembled fetal than adult hepatocytes. Furthermore, clustering showed that primary adult hepatocytes cultured at the air-liquid interface retained a proteome that more closely mimicked their fresh counterparts than conventional culture, which acquired myofibroblast features. Principal component analysis extended these findings and identified a simple set of proteins, including cytochrome P450 2A6, glutathione S transferase P, and alcohol dehydrogenases as specialized indicators of hepatocyte differentiation. Conclusion: Our quantitative datasets are the first that directly compare multiple human liver cells, define a model for enhanced maintenance of the hepatocyte proteome in culture, and provide a new protein “toolkit” for determining human hepatocyte maturity in cultured cells. (Hepatology 2013;58:799–809) WILEY-VCH Verlag 2013-08 2013-07-01 /pmc/articles/PMC3842115/ /pubmed/23526496 http://dx.doi.org/10.1002/hep.26414 Text en Copyright © 2013 by the American Association for the Study of Liver Diseases http://creativecommons.org/licenses/by/2.5/ Re-use of this article is permitted in accordance with the Creative Commons Deed, Attribution 2.5, which does not permit commercial exploitation.
spellingShingle Liver Biology/Pathobiology
Rowe, Cliff
Gerrard, Dave T
Jenkins, Roz
Berry, Andrew
Durkin, Kesta
Sundstrom, Lars
Goldring, Chris E
Park, B Kevin
Kitteringham, Neil R
Hanley, Karen Piper
Hanley, Neil A
Proteome-wide analyses of human hepatocytes during differentiation and dedifferentiation
title Proteome-wide analyses of human hepatocytes during differentiation and dedifferentiation
title_full Proteome-wide analyses of human hepatocytes during differentiation and dedifferentiation
title_fullStr Proteome-wide analyses of human hepatocytes during differentiation and dedifferentiation
title_full_unstemmed Proteome-wide analyses of human hepatocytes during differentiation and dedifferentiation
title_short Proteome-wide analyses of human hepatocytes during differentiation and dedifferentiation
title_sort proteome-wide analyses of human hepatocytes during differentiation and dedifferentiation
topic Liver Biology/Pathobiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3842115/
https://www.ncbi.nlm.nih.gov/pubmed/23526496
http://dx.doi.org/10.1002/hep.26414
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