A 3D Cell Culture Organ-on-a-Chip Platform With a Breathable Hemoglobin Analogue Augments and Extends Primary Human Hepatocyte Functions in vitro

A 3D Cell Culture Organ-on-a-Chip Platform With a Breathable Hemoglobin Analogue Augments and Extends Primary Human Hepatocyte Functions in vitro

Remarkable advances in three-dimensional (3D) cell cultures and organ-on-a-chip technologies have opened the door to recapitulate complex aspects of human physiology, pathology, and drug responses in vitro. The challenges regarding oxygen delivery, throughput, assay multiplexing, and experimental co...

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Main Authors: James T. Shoemaker, Wanrui Zhang, Selin I. Atlas, Richard A. Bryan, S. Walker Inman, Jelena Vukasinovic
Format: Article
Language:English
Published: Frontiers Media S.A. 2020-10-01
Series:Frontiers in Molecular Biosciences
Subjects:
3D cell culture
organ-on-a-chip
liver model
CYP450
drug metabolism
cell metabolism
Online Access:https://www.frontiersin.org/article/10.3389/fmolb.2020.568777/full
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spelling doaj-9056a615c4ca4da38ca6a102f3be0e152020-11-25T03:53:57ZengFrontiers Media S.A.Frontiers in Molecular Biosciences2296-889X2020-10-01710.3389/fmolb.2020.568777568777A 3D Cell Culture Organ-on-a-Chip Platform With a Breathable Hemoglobin Analogue Augments and Extends Primary Human Hepatocyte Functions in vitroJames T. Shoemaker0Wanrui Zhang1Selin I. Atlas2Richard A. Bryan3S. Walker Inman4Jelena Vukasinovic5Lena Biosciences, Inc., Atlanta, GA, United StatesLena Biosciences, Inc., Atlanta, GA, United StatesLena Biosciences, Inc., Atlanta, GA, United StatesLucid Scientific, Atlanta, GA, United StatesLucid Scientific, Atlanta, GA, United StatesLena Biosciences, Inc., Atlanta, GA, United StatesRemarkable advances in three-dimensional (3D) cell cultures and organ-on-a-chip technologies have opened the door to recapitulate complex aspects of human physiology, pathology, and drug responses in vitro. The challenges regarding oxygen delivery, throughput, assay multiplexing, and experimental complexity are addressed to ensure that perfused 3D cell culture organ-on-a-chip models become a routine research tool adopted by academic and industrial stakeholders. To move the field forward, we present a throughput-scalable organ-on-a-chip insert system that requires a single tube to operate 48 statistically independent 3D cell culture organ models. Then, we introduce in-well perfusion to circumvent the loss of cell signaling and drug metabolites in otherwise one-way flow of perfusate. Further, to augment the relevancy of 3D cell culture models in vitro, we tackle the problem of oxygen transport by blood using, for the first time, a breathable hemoglobin analog to improve delivery of respiratory gases to cells, because in vivo approximately 98% of oxygen delivery to cells takes place via reversible binding to hemoglobin. Next, we show that improved oxygenation shifts cellular metabolic pathways toward oxidative phosphorylation that contributes to the maintenance of differentiated liver phenotypes in vitro. Lastly, we demonstrate that the activity of cytochrome P450 family of drug metabolizing enzymes is increased and prolonged in primary human hepatocytes cultured in 3D compared to two-dimensional (2D) cell culture gold standard with important ramifications for drug metabolism, drug-drug interactions and pharmacokinetic studies in vitro.https://www.frontiersin.org/article/10.3389/fmolb.2020.568777/full3D cell cultureorgan-on-a-chipliver modelCYP450drug metabolismcell metabolism
collection DOAJ
language English
format Article
sources DOAJ
author James T. Shoemaker
Wanrui Zhang
Selin I. Atlas
Richard A. Bryan
S. Walker Inman
Jelena Vukasinovic
spellingShingle James T. Shoemaker
Wanrui Zhang
Selin I. Atlas
Richard A. Bryan
S. Walker Inman
Jelena Vukasinovic
A 3D Cell Culture Organ-on-a-Chip Platform With a Breathable Hemoglobin Analogue Augments and Extends Primary Human Hepatocyte Functions in vitro
Frontiers in Molecular Biosciences
3D cell culture
organ-on-a-chip
liver model
CYP450
drug metabolism
cell metabolism
author_facet James T. Shoemaker
Wanrui Zhang
Selin I. Atlas
Richard A. Bryan
S. Walker Inman
Jelena Vukasinovic
author_sort James T. Shoemaker
title A 3D Cell Culture Organ-on-a-Chip Platform With a Breathable Hemoglobin Analogue Augments and Extends Primary Human Hepatocyte Functions in vitro
title_short A 3D Cell Culture Organ-on-a-Chip Platform With a Breathable Hemoglobin Analogue Augments and Extends Primary Human Hepatocyte Functions in vitro
title_full A 3D Cell Culture Organ-on-a-Chip Platform With a Breathable Hemoglobin Analogue Augments and Extends Primary Human Hepatocyte Functions in vitro
title_fullStr A 3D Cell Culture Organ-on-a-Chip Platform With a Breathable Hemoglobin Analogue Augments and Extends Primary Human Hepatocyte Functions in vitro
title_full_unstemmed A 3D Cell Culture Organ-on-a-Chip Platform With a Breathable Hemoglobin Analogue Augments and Extends Primary Human Hepatocyte Functions in vitro
title_sort 3d cell culture organ-on-a-chip platform with a breathable hemoglobin analogue augments and extends primary human hepatocyte functions in vitro
publisher Frontiers Media S.A.
series Frontiers in Molecular Biosciences
issn 2296-889X
publishDate 2020-10-01
description Remarkable advances in three-dimensional (3D) cell cultures and organ-on-a-chip technologies have opened the door to recapitulate complex aspects of human physiology, pathology, and drug responses in vitro. The challenges regarding oxygen delivery, throughput, assay multiplexing, and experimental complexity are addressed to ensure that perfused 3D cell culture organ-on-a-chip models become a routine research tool adopted by academic and industrial stakeholders. To move the field forward, we present a throughput-scalable organ-on-a-chip insert system that requires a single tube to operate 48 statistically independent 3D cell culture organ models. Then, we introduce in-well perfusion to circumvent the loss of cell signaling and drug metabolites in otherwise one-way flow of perfusate. Further, to augment the relevancy of 3D cell culture models in vitro, we tackle the problem of oxygen transport by blood using, for the first time, a breathable hemoglobin analog to improve delivery of respiratory gases to cells, because in vivo approximately 98% of oxygen delivery to cells takes place via reversible binding to hemoglobin. Next, we show that improved oxygenation shifts cellular metabolic pathways toward oxidative phosphorylation that contributes to the maintenance of differentiated liver phenotypes in vitro. Lastly, we demonstrate that the activity of cytochrome P450 family of drug metabolizing enzymes is increased and prolonged in primary human hepatocytes cultured in 3D compared to two-dimensional (2D) cell culture gold standard with important ramifications for drug metabolism, drug-drug interactions and pharmacokinetic studies in vitro.
topic 3D cell culture
organ-on-a-chip
liver model
CYP450
drug metabolism
cell metabolism
url https://www.frontiersin.org/article/10.3389/fmolb.2020.568777/full
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