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MicroRNA-122: A Novel Hepatocyte-Enriched in vitro Marker of Drug-Induced Cellular Toxicity

Emerging hepatic models for the study of drug-induced toxicity include pluripotent stem cell-derived hepatocyte-like cells (HLCs) and complex hepatocyte-non-parenchymal cellular coculture to mimic the complex multicellular interactions that recapitulate the niche environment in the human liver. Howe...

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Autores principales: Kia, Richard, Kelly, Lorna, Sison-Young, Rowena L. C., Zhang, Fang, Pridgeon, Chris S., Heslop, James A., Metcalfe, Pete, Kitteringham, Neil R., Baxter, Melissa, Harrison, Sean, Hanley, Neil A., Burke, Zoë D., Storm, Mike P., Welham, Melanie J., Tosh, David, Küppers-Munther, Barbara, Edsbagge, Josefina, Starkey Lewis, Philip J., Bonner, Frank, Harpur, Ernie, Sidaway, James, Bowes, Joanne, Fenwick, Stephen W., Malik, Hassan, Goldring, Chris E. P., Park, B. Kevin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4349141/
https://www.ncbi.nlm.nih.gov/pubmed/25527335
http://dx.doi.org/10.1093/toxsci/kfu269
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author Kia, Richard
Kelly, Lorna
Sison-Young, Rowena L. C.
Zhang, Fang
Pridgeon, Chris S.
Heslop, James A.
Metcalfe, Pete
Kitteringham, Neil R.
Baxter, Melissa
Harrison, Sean
Hanley, Neil A.
Burke, Zoë D.
Storm, Mike P.
Welham, Melanie J.
Tosh, David
Küppers-Munther, Barbara
Edsbagge, Josefina
Starkey Lewis, Philip J.
Bonner, Frank
Harpur, Ernie
Sidaway, James
Bowes, Joanne
Fenwick, Stephen W.
Malik, Hassan
Goldring, Chris E. P.
Park, B. Kevin
author_facet Kia, Richard
Kelly, Lorna
Sison-Young, Rowena L. C.
Zhang, Fang
Pridgeon, Chris S.
Heslop, James A.
Metcalfe, Pete
Kitteringham, Neil R.
Baxter, Melissa
Harrison, Sean
Hanley, Neil A.
Burke, Zoë D.
Storm, Mike P.
Welham, Melanie J.
Tosh, David
Küppers-Munther, Barbara
Edsbagge, Josefina
Starkey Lewis, Philip J.
Bonner, Frank
Harpur, Ernie
Sidaway, James
Bowes, Joanne
Fenwick, Stephen W.
Malik, Hassan
Goldring, Chris E. P.
Park, B. Kevin
author_sort Kia, Richard
collection PubMed
description Emerging hepatic models for the study of drug-induced toxicity include pluripotent stem cell-derived hepatocyte-like cells (HLCs) and complex hepatocyte-non-parenchymal cellular coculture to mimic the complex multicellular interactions that recapitulate the niche environment in the human liver. However, a specific marker of hepatocyte perturbation, required to discriminate hepatocyte damage from non-specific cellular toxicity contributed by non-hepatocyte cell types or immature differentiated cells is currently lacking, as the cytotoxicity assays routinely used in in vitro toxicology research depend on intracellular molecules which are ubiquitously present in all eukaryotic cell types. In this study, we demonstrate that microRNA-122 (miR-122) detection in cell culture media can be used as a hepatocyte-enriched in vitro marker of drug-induced toxicity in homogeneous cultures of hepatic cells, and a cell-specific marker of toxicity of hepatic cells in heterogeneous cultures such as HLCs generated from various differentiation protocols and pluripotent stem cell lines, where conventional cytotoxicity assays using generic cellular markers may not be appropriate. We show that the sensitivity of the miR-122 cytotoxicity assay is similar to conventional assays that measure lactate dehydrogenase activity and intracellular adenosine triphosphate when applied in hepatic models with high levels of intracellular miR-122, and can be multiplexed with other assays. MiR-122 as a biomarker also has the potential to bridge results in in vitro experiments to in vivo animal models and human samples using the same assay, and to link findings from clinical studies in determining the relevance of in vitro models being developed for the study of drug-induced liver injury.
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spelling pubmed-43491412016-03-01 MicroRNA-122: A Novel Hepatocyte-Enriched in vitro Marker of Drug-Induced Cellular Toxicity Kia, Richard Kelly, Lorna Sison-Young, Rowena L. C. Zhang, Fang Pridgeon, Chris S. Heslop, James A. Metcalfe, Pete Kitteringham, Neil R. Baxter, Melissa Harrison, Sean Hanley, Neil A. Burke, Zoë D. Storm, Mike P. Welham, Melanie J. Tosh, David Küppers-Munther, Barbara Edsbagge, Josefina Starkey Lewis, Philip J. Bonner, Frank Harpur, Ernie Sidaway, James Bowes, Joanne Fenwick, Stephen W. Malik, Hassan Goldring, Chris E. P. Park, B. Kevin Toxicol Sci MicroRNA-122 as A Biomarker of Liver Injury Emerging hepatic models for the study of drug-induced toxicity include pluripotent stem cell-derived hepatocyte-like cells (HLCs) and complex hepatocyte-non-parenchymal cellular coculture to mimic the complex multicellular interactions that recapitulate the niche environment in the human liver. However, a specific marker of hepatocyte perturbation, required to discriminate hepatocyte damage from non-specific cellular toxicity contributed by non-hepatocyte cell types or immature differentiated cells is currently lacking, as the cytotoxicity assays routinely used in in vitro toxicology research depend on intracellular molecules which are ubiquitously present in all eukaryotic cell types. In this study, we demonstrate that microRNA-122 (miR-122) detection in cell culture media can be used as a hepatocyte-enriched in vitro marker of drug-induced toxicity in homogeneous cultures of hepatic cells, and a cell-specific marker of toxicity of hepatic cells in heterogeneous cultures such as HLCs generated from various differentiation protocols and pluripotent stem cell lines, where conventional cytotoxicity assays using generic cellular markers may not be appropriate. We show that the sensitivity of the miR-122 cytotoxicity assay is similar to conventional assays that measure lactate dehydrogenase activity and intracellular adenosine triphosphate when applied in hepatic models with high levels of intracellular miR-122, and can be multiplexed with other assays. MiR-122 as a biomarker also has the potential to bridge results in in vitro experiments to in vivo animal models and human samples using the same assay, and to link findings from clinical studies in determining the relevance of in vitro models being developed for the study of drug-induced liver injury. Oxford University Press 2015-03 2014-12-18 /pmc/articles/PMC4349141/ /pubmed/25527335 http://dx.doi.org/10.1093/toxsci/kfu269 Text en © The Author 2014. Published by Oxford University Press on behalf of the Society of Toxicology. http://creativecommons.org/licenses/by/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle MicroRNA-122 as A Biomarker of Liver Injury
Kia, Richard
Kelly, Lorna
Sison-Young, Rowena L. C.
Zhang, Fang
Pridgeon, Chris S.
Heslop, James A.
Metcalfe, Pete
Kitteringham, Neil R.
Baxter, Melissa
Harrison, Sean
Hanley, Neil A.
Burke, Zoë D.
Storm, Mike P.
Welham, Melanie J.
Tosh, David
Küppers-Munther, Barbara
Edsbagge, Josefina
Starkey Lewis, Philip J.
Bonner, Frank
Harpur, Ernie
Sidaway, James
Bowes, Joanne
Fenwick, Stephen W.
Malik, Hassan
Goldring, Chris E. P.
Park, B. Kevin
MicroRNA-122: A Novel Hepatocyte-Enriched in vitro Marker of Drug-Induced Cellular Toxicity
title MicroRNA-122: A Novel Hepatocyte-Enriched in vitro Marker of Drug-Induced Cellular Toxicity
title_full MicroRNA-122: A Novel Hepatocyte-Enriched in vitro Marker of Drug-Induced Cellular Toxicity
title_fullStr MicroRNA-122: A Novel Hepatocyte-Enriched in vitro Marker of Drug-Induced Cellular Toxicity
title_full_unstemmed MicroRNA-122: A Novel Hepatocyte-Enriched in vitro Marker of Drug-Induced Cellular Toxicity
title_short MicroRNA-122: A Novel Hepatocyte-Enriched in vitro Marker of Drug-Induced Cellular Toxicity
title_sort microrna-122: a novel hepatocyte-enriched in vitro marker of drug-induced cellular toxicity
topic MicroRNA-122 as A Biomarker of Liver Injury
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4349141/
https://www.ncbi.nlm.nih.gov/pubmed/25527335
http://dx.doi.org/10.1093/toxsci/kfu269
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