Oxygen Gradient Induced in Microfluidic Chips Can Be Used as a Model for Liver Zonation

Availability of oxygen plays an important role in tissue organization and cell-type specific metabolism. It is, however, difficult to analyze hypoxia-related adaptations in vitro because of inherent limitations of experimental model systems. In this study, we establish a microfluidic tissue culture...

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Autores principales: Ghafoory, Shahrouz, Stengl, Christina, Kopany, Stefan, Mayadag, Mert, Mechtel, Nils, Murphy, Brennah, Schattschneider, Sebastian, Wilhelmi, Niklas, Wölfl, Stefan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9738923/
https://www.ncbi.nlm.nih.gov/pubmed/36496994
http://dx.doi.org/10.3390/cells11233734
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author Ghafoory, Shahrouz
Stengl, Christina
Kopany, Stefan
Mayadag, Mert
Mechtel, Nils
Murphy, Brennah
Schattschneider, Sebastian
Wilhelmi, Niklas
Wölfl, Stefan
author_facet Ghafoory, Shahrouz
Stengl, Christina
Kopany, Stefan
Mayadag, Mert
Mechtel, Nils
Murphy, Brennah
Schattschneider, Sebastian
Wilhelmi, Niklas
Wölfl, Stefan
author_sort Ghafoory, Shahrouz
collection PubMed
description Availability of oxygen plays an important role in tissue organization and cell-type specific metabolism. It is, however, difficult to analyze hypoxia-related adaptations in vitro because of inherent limitations of experimental model systems. In this study, we establish a microfluidic tissue culture protocol to generate hypoxic gradients in vitro, mimicking the conditions found in the liver acinus. To accomplish this, four microfluidic chips, each containing two chambers, were serially connected to obtain eight interconnected chambers. HepG2 hepatocytes were uniformly seeded in each chamber and cultivated under a constant media flow of 50 µL/h for 72 h. HepG2 oxygen consumption under flowing media conditions established a normoxia to hypoxia gradient within the chambers, which was confirmed by oxygen sensors located at the inlet and outlet of the connected microfluidic chips. Expression of Hif1α mRNA and protein was used to indicate hypoxic conditions in the cells and albumin mRNA and protein expression served as a marker for liver acinus-like zonation. Oxygen measurements performed over 72 h showed a change from 17.5% to 15.9% of atmospheric oxygen, which corresponded with a 9.2% oxygen reduction in the medium between chamber1 (inlet) and 8 (outlet) in the connected microfluidic chips after 72 h. Analysis of Hif1α expression and nuclear translocation in HepG2 cells additionally confirmed the hypoxic gradient from chamber1 to chamber8. Moreover, albumin mRNA and protein levels were significantly reduced from chamber1 to chamber8, indicating liver acinus zonation along the oxygen gradient. Taken together, microfluidic cultivation in interconnected chambers provides a new model for analyzing cells in a normoxic to hypoxic gradient in vitro. By using a well-characterized cancer cell line as a homogenous hepatocyte population, we also demonstrate that an approximate 10% reduction in oxygen triggers translocation of Hif1α to the nucleus and reduces albumin production.
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spelling pubmed-97389232022-12-11 Oxygen Gradient Induced in Microfluidic Chips Can Be Used as a Model for Liver Zonation Ghafoory, Shahrouz Stengl, Christina Kopany, Stefan Mayadag, Mert Mechtel, Nils Murphy, Brennah Schattschneider, Sebastian Wilhelmi, Niklas Wölfl, Stefan Cells Article Availability of oxygen plays an important role in tissue organization and cell-type specific metabolism. It is, however, difficult to analyze hypoxia-related adaptations in vitro because of inherent limitations of experimental model systems. In this study, we establish a microfluidic tissue culture protocol to generate hypoxic gradients in vitro, mimicking the conditions found in the liver acinus. To accomplish this, four microfluidic chips, each containing two chambers, were serially connected to obtain eight interconnected chambers. HepG2 hepatocytes were uniformly seeded in each chamber and cultivated under a constant media flow of 50 µL/h for 72 h. HepG2 oxygen consumption under flowing media conditions established a normoxia to hypoxia gradient within the chambers, which was confirmed by oxygen sensors located at the inlet and outlet of the connected microfluidic chips. Expression of Hif1α mRNA and protein was used to indicate hypoxic conditions in the cells and albumin mRNA and protein expression served as a marker for liver acinus-like zonation. Oxygen measurements performed over 72 h showed a change from 17.5% to 15.9% of atmospheric oxygen, which corresponded with a 9.2% oxygen reduction in the medium between chamber1 (inlet) and 8 (outlet) in the connected microfluidic chips after 72 h. Analysis of Hif1α expression and nuclear translocation in HepG2 cells additionally confirmed the hypoxic gradient from chamber1 to chamber8. Moreover, albumin mRNA and protein levels were significantly reduced from chamber1 to chamber8, indicating liver acinus zonation along the oxygen gradient. Taken together, microfluidic cultivation in interconnected chambers provides a new model for analyzing cells in a normoxic to hypoxic gradient in vitro. By using a well-characterized cancer cell line as a homogenous hepatocyte population, we also demonstrate that an approximate 10% reduction in oxygen triggers translocation of Hif1α to the nucleus and reduces albumin production. MDPI 2022-11-23 /pmc/articles/PMC9738923/ /pubmed/36496994 http://dx.doi.org/10.3390/cells11233734 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Ghafoory, Shahrouz
Stengl, Christina
Kopany, Stefan
Mayadag, Mert
Mechtel, Nils
Murphy, Brennah
Schattschneider, Sebastian
Wilhelmi, Niklas
Wölfl, Stefan
Oxygen Gradient Induced in Microfluidic Chips Can Be Used as a Model for Liver Zonation
title Oxygen Gradient Induced in Microfluidic Chips Can Be Used as a Model for Liver Zonation
title_full Oxygen Gradient Induced in Microfluidic Chips Can Be Used as a Model for Liver Zonation
title_fullStr Oxygen Gradient Induced in Microfluidic Chips Can Be Used as a Model for Liver Zonation
title_full_unstemmed Oxygen Gradient Induced in Microfluidic Chips Can Be Used as a Model for Liver Zonation
title_short Oxygen Gradient Induced in Microfluidic Chips Can Be Used as a Model for Liver Zonation
title_sort oxygen gradient induced in microfluidic chips can be used as a model for liver zonation
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9738923/
https://www.ncbi.nlm.nih.gov/pubmed/36496994
http://dx.doi.org/10.3390/cells11233734
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